2338 PART 9 Disorders of the Kidney and Urinary Tract
leukocyte infiltration, activation of procoagulant factors, and release of
various cytokines. In situ immune complex formation also plays a role
in renal injury. These immune deposits may occur in the mesangial,
subendothelial, and/or subepithelial spaces.
The clinical manifestations, course of disease, and treatment of
lupus nephritis are closely linked to renal pathology. The most common clinical sign of renal disease is proteinuria, but hematuria, hypertension, varying degrees of renal failure, and active urine sediment
with red blood cell casts can all be present. Anti-dsDNA antibodies
that fix complement correlate best with the presence of renal disease. Hypocomplementemia is common in patients with acute lupus
nephritis (70–90%), and declining complement levels may herald a
flare. A kidney biopsy should be performed in most patients with renal
involvement to establish the histologic subtype, which guides therapy.
The World Health Organization (WHO) workshop in 1974 first outlined several distinct patterns of lupus-related glomerular injury, and
this classification was modified in 2004. This latest version of lesions
seen on biopsy (Table 314-3) forms the basis for modern treatment
recommendations. Class I nephritis describes normal glomerular histology by normal light microscopy with minimal mesangial deposits
on immunofluorescent or electron microscopy. Class II designates
mesangial immune complexes with mesangial proliferation. Both class I
and II lesions are typically associated with minimal renal manifestation
and normal renal function; nephrotic syndrome is rare. Patients with
lesions limited to the renal mesangium have an excellent prognosis and
generally do not need therapy for their lupus nephritis.
The subject of lupus nephritis is presented under acute nephritic
syndromes because of the aggressive and important proliferative
lesions seen in class III–V renal diseases. Class III describes focal
lesions involving <50% of the glomeruli with proliferation or scarring,
often involving only a segment of the glomerulus (see Fig. A4-12).
Class III lesions have the most varied course. Hematuria and proteinuria are present, and some patients also have an active urinary
sediment, nephrotic syndrome, hypertension, and a decreased GFR.
Patients with mild proliferation involving a small percentage of glomeruli respond well to therapy with steroids alone, and <5% progress
to renal failure over 5 years. Patients with more severe proliferation
involving a greater percentage of glomeruli have a far worse prognosis
and lower remission rates. Treatment of those patients is the same as
that for class IV lesions. Class IV describes diffuse lesions with >50%
of the glomeruli involved and proliferative endocapillary lesions with or
without extracapillary lesions that may be segmental (IV-S), involving
<50% of the glomerular tuft, or global (IV-G), involving >50%. Patients
with class IV lesions commonly have high anti-DNA antibody titers,
low serum complement, hematuria, red blood cell casts, proteinuria,
hypertension, and decreased renal function; 50% of patients have
nephrotic-range proteinuria. Patients with crescents on biopsy often
have a rapidly progressive decline in renal function (see Fig. A4-12).
TABLE 314-3 Classification for Lupus Nephritis
Class I Minimal mesangial Normal histology with mesangial deposits
Class II Mesangial
proliferation
Mesangial hypercellularity with expansion of
the mesangial matrix
Class III Focal nephritis Focal endocapillary ± extracapillary
proliferation with focal subendothelial immune
deposits and mild mesangial expansion
Class IV Diffuse nephritis Diffuse endocapillary ± extracapillary
proliferation with diffuse subendothelial
immune deposits and mesangial alterations
Class V Membranous
nephritis
Thickened basement membranes with diffuse
subepithelial immune deposits; may occur
with class III or IV lesions and is sometimes
called mixed membranous and proliferative
nephritis
Class VI Sclerotic nephritis Global sclerosis of nearly all glomerular
capillaries
Note: Revised in 2004 by the International Society of Nephrology-Renal Pathology
Society Study Group.
Without treatment, this aggressive lesion has the worst renal prognosis, with class IV-S worse than class IV-G. However, if a remission—
defined as a return to near-normal renal function and proteinuria
≤330 mg/dL per day—is achieved with treatment, renal outcomes are
excellent. Current evidence suggests that inducing a remission with
administration of high-dose steroids and either cyclophosphamide
or mycophenolate mofetil for 2–6 months, followed by maintenance
therapy with lower doses of steroids and mycophenolate mofetil or
azathioprine, best balances the likelihood of successful remission with
the side effects of therapy. There is no consensus on use of high-dose
intravenous methylprednisolone versus oral prednisone, monthly
intravenous cyclophosphamide versus daily oral cyclophosphamide, or
other immunosuppressants such as cyclosporine, tacrolimus, or rituximab. Nephrologists tend to avoid prolonged use of cyclophosphamide
in patients of childbearing age without first banking eggs or sperm.
The class V lesion describes subepithelial immune deposits producing a membranous pattern; a subcategory of class V lesions is associated
with proliferative lesions and is sometimes called mixed membranous
and proliferative disease (see Fig. A4-11); this category of injury is
treated like class IV glomerulonephritis. Sixty percent of patients present with nephrotic syndrome or lesser amounts of proteinuria. Patients
with lupus nephritis class V, like patients with idiopathic membranous
nephropathy (IMN), are predisposed to renal vein thrombosis and
other thrombotic complications. A minority of patients with class V
will present with hypertension and renal dysfunction. There are conflicting data on the clinical course, prognosis, and appropriate therapy
for patients with class V disease, which may reflect the heterogeneity
of this group of patients. Patients with severe nephrotic syndrome,
elevated serum creatinine, and a progressive course will probably
benefit from therapy with steroids in combination with other immunosuppressive agents. Therapy with inhibitors of the renin-angiotensin
system also may attenuate the proteinuria. Antiphospholipid antibodies present in lupus may result in glomerular microthromboses and
a thrombotic microangiopathy. The renal prognosis is worse despite
anticoagulant therapy.
Patients with any of the above lesions also can transform to another
lesion; hence, patients often require reevaluation, including repeat
renal biopsy. Lupus patients with class VI lesions have >90% sclerotic
glomeruli and ESRD with interstitial fibrosis. Up to 20% of patients
with lupus nephritis will reach end-stage disease, requiring dialysis
or transplantation. Patients with lupus nephritis have a markedly
increased mortality compared with the general population. Renal
transplantation in renal failure from lupus, usually performed after ~6
months of inactive disease, results in allograft survival rates comparable to patients transplanted for other reasons.
■ ANTIGLOMERULAR BASEMENT MEMBRANE
DISEASE
Patients who develop autoantibodies directed against glomerular
basement antigens frequently develop a glomerulonephritis termed
antiglomerular basement membrane (anti-GBM) disease. When they
present with lung hemorrhage and glomerulonephritis, they have a
pulmonary-renal syndrome called Goodpasture’s syndrome. The target
epitopes for this autoimmune disease lie in the quaternary structure
of α3 NC1 domain of collagen IV. Indeed, anti-GBM disease may
be considered an autoimmune “conformeropathy” that involves the
perturbation of quaternary structure of the α 345NC1 hexamer. MHCrestricted T cells initiate the autoantibody response because humans
are not tolerant to the epitopes created by this quaternary structure.
The epitopes are normally sequestered in the collagen IV hexamer and
can be exposed by infection, smoking, oxidants, or solvents. Goodpasture’s syndrome appears in two age groups: in young men in their late
twenties and in men and women in their sixties and seventies. Younger
patients are more likely to present with the full Goodpasture’s syndrome, with hemoptysis, a sudden fall in hemoglobin, fever, dyspnea,
and hematuria, and older patients are more likely to present with isolated glomerulonephritis. Hemoptysis is largely confined to smokers,
and those who present with lung hemorrhage as a group do better than
older populations who have prolonged, asymptomatic renal injury;
2339 Glomerular Diseases CHAPTER 314
presentation with oliguria is often associated with a particularly bad
outcome. The performance of an urgent kidney biopsy is important in
suspected cases of Goodpasture’s syndrome to confirm the diagnosis
and assess prognosis. Renal biopsies typically show focal or segmental
necrosis that later, with aggressive destruction of the capillaries by
cellular proliferation, leads to crescent formation in Bowman’s space
(see Fig. A4-14). As these lesions progress, there is concomitant interstitial nephritis with fibrosis and tubular atrophy.
The presence of anti-GBM antibodies and complement is recognized
on biopsy by linear immunofluorescent staining for IgG (rarely IgA).
In testing serum for anti-GBM antibodies, it is particularly important
that the α3 NC1 domain of collagen IV alone be used as the target.
This is because nonnephritic antibodies against the α1 NC1 domain
are seen in paraneoplastic syndromes and cannot be discerned from
assays that use whole basement membrane fragments as the binding
target. Between 10 and 15% of sera from patients with Goodpasture’s
syndrome also contain ANCA antibodies against myeloperoxidase.
Prognosis at presentation is worse if there are >50% crescents on renal
biopsy with advanced fibrosis, if serum creatinine is >5–6 mg/dL, if
oliguria is present, or if there is a need for acute dialysis. Patients who
present with hemoptysis should be treated for their lung hemorrhage,
as it responds to plasmapheresis. Treated patients with less severe disease typically respond to 8–10 treatments of plasmapheresis accompanied by oral prednisone and cyclophosphamide. Maintenance therapy
with low-dose immunosuppressants should be considered until antibody titers are negative. There are scarce data alternatively using rituximab, azathioprine, or mycophenolate mofetil. Kidney transplantation
should wait for 6 months and until serum antibodies are undetectable.
■ IgA NEPHROPATHY
Berger first described the glomerulonephritis now termed IgA nephropathy. It is classically characterized by episodic hematuria associated
with the deposition of IgA in the mesangium. IgA nephropathy is one
of the most common forms of glomerulonephritis worldwide. There
is a male preponderance, a peak incidence in the second and third
decades of life, and rare familial clustering. There are geographic differences in the prevalence of IgA nephropathy, with 30% prevalence along
the Asian and Pacific Rim and 20% in southern Europe, compared to a
much lower prevalence in northern Europe and North America. This
may reflect variation in detection or a true variation among racial and
ethnic groups.
IgA nephropathy is predominantly a sporadic disease, but susceptibility to it has been shown uncommonly to have a genetic component depending on geography and the existence of “founder effects.”
Familial forms of IgA nephropathy are more common in northern
Italy and eastern Kentucky. No single causal gene has been identified.
Clinical and laboratory evidence suggests close similarities between
Henoch-Schönlein purpura and IgA nephropathy. Henoch-Schönlein
purpura is distinguished clinically from IgA nephropathy by prominent
systemic symptoms, a younger age (<20 years old), preceding infection,
and abdominal complaints. Deposits of IgA are also found in the glomerular mesangium in a variety of systemic diseases, including chronic
liver disease, Crohn’s disease, celiac disease, chronic bronchiectasis,
idiopathic interstitial pneumonia, dermatitis herpetiformis, mycosis
fungoides, ankylosing spondylitis, HIV infection, and Sjögren’s syndrome. IgA deposition in these entities is not usually associated with
clinically significant renal disease. IgG A-dominant Staphylococcusassociated postinfectious glomerulonephritis is associated with clinically significant renal disease.
The pathognomonic finding on kidney biopsy is dominant or
codominant mesangial IgA deposits, either alone or with IgG, IgM, or
C3
. (See Glomerular Schematic 2.) IgA deposits are typically J-chain
containing polymeric IgA. Abnormalities have been described in
IgA production by plasma cells, in IgA clearance by the liver, and in
mesangial IgA clearance and receptors for IgA. Currently, however,
abnormalities in the O-glycosylation of the hinge region of primarily
polymeric IgA1 seem to best account for the pathogenesis of sporadic
IgA nephropathy. Synthesis of poorly galactosylated IgA1 results in
exposure of N-acetyl-galactosamine in truncated IgA1 hinge regions,
which is recognized by IgG or IgA1 antibodies leading to formation
of immune complexes in the circulation or in situ after glomerular
deposition of galactose-deficient IgA1. A second hit, such as a viral or
other antigen exposure, or hereditary defects in alternative complement pathway proteins may affect the manifestation of disease. Despite
the presence of elevated serum IgA levels in 20–50% of patients and
IgA deposition in skin biopsies in 15–55% of patients, a renal biopsy is
necessary to confirm the diagnosis. Although the immunofluorescent
pattern of IgA on renal biopsy defines IgA nephropathy in the proper
clinical context, a variety of histologic lesions may be seen on light
microscopy (see Fig. A4-8), including DPGN; segmental sclerosis; and,
rarely, segmental necrosis with cellular crescent formation, which typically presents as RPGN.
The two most common presentations of IgA nephropathy are
recurrent episodes of macroscopic hematuria during or immediately
following an upper respiratory infection often accompanied by proteinuria and persistent asymptomatic microscopic hematuria. Nephrotic syndrome is uncommon. Proteinuria can also first appear late
in the course of the disease. Rarely, patients present with acute renal
failure and a rapidly progressive clinical picture. IgA nephropathy is
a benign disease for the majority of patients, and 5–30% of patients
may go into a complete remission, with others having hematuria but
well-preserved renal function. In the minority of patients who have
progressive disease, progression is slow, with renal failure seen in only
25–30% of patients with IgA nephropathy over 20–25 years. This risk
varies considerably among populations. Cumulatively, risk factors for
the loss of renal function identified thus far account for <50% of the
variation in observed outcome but include the presence of hypertension or proteinuria, the absence of episodes of macroscopic hematuria,
male sex, and older age of onset. Mesangial hypercellularity (M),
endocapillary hypercellularity (E), segmental glomerulosclerosis (S),
tubular interstitial fibrosis (T), and crescents (C) have predictive value
as established by the Oxford Classification and the MEST-C score.
Several analyses in large populations of patients found persistent proteinuria for 6 months or longer to have the greatest predictive power
for adverse renal outcomes.
There is no agreement on optimal treatment. Both large studies that
include patients with multiple glomerular diseases and small studies
of patients with IgA nephropathy support the use of angiotensinconverting enzyme (ACE) inhibitors in patients with proteinuria or
declining renal function. In patients with persistent proteinuria after
Glomerular schematic 2
IgA
NEPHROPATHY
Mesangial deposits
plus more
mesangial cells
2340 PART 9 Disorders of the Kidney and Urinary Tract
ACE inhibitor therapy, steroid treatment or other immunosuppressives
have demonstrated conflicting results. Tonsillectomy and fish oil have
also been suggested in small studies to benefit select patients. When
presenting as RPGN, patients typically receive steroids, cytotoxic
agents, and plasmapheresis.
■ ANCA SMALL-VESSEL VASCULITIS
A group of patients with small-vessel vasculitis (arterioles, capillaries, and venules; rarely small arteries) and glomerulonephritis have
serum ANCA; the antibodies are of two types, anti-proteinase 3 (PR3)
or anti-myeloperoxidase (MPO) (Chap. 363). ANCA are produced
with the help of T cells and activate leukocytes and monocytes, which
together damage the walls of small vessels. Endothelial injury also
attracts more leukocytes and extends the inflammation. Granulomatosis with polyangiitis, microscopic polyangiitis, Churg-Strauss syndrome, and renal-limited vasculitis belong to this group because they
are ANCA-positive and have a pauci-immune glomerulonephritis with
few immune complexes in small vessels and glomerular capillaries.
Patients with any of these diseases can have any combination of the
above serum antibodies, but anti-PR3 antibodies are more common in
granulomatosis with polyangiitis, and anti-MPO antibodies are more
common in microscopic polyangiitis or Churg-Strauss. Although each
of these diseases has some unique clinical features, most features do not
predict relapse or progression, and as a group, they are generally treated
in the same way. Once diagnosed, ANCA monitoring has limited value,
but targeted determination of ANCA levels may be useful if a relapse
is clinically suspected. Since mortality is high without treatment, virtually all patients receive urgent treatment. Induction therapy usually
includes glucocorticoids and either cyclophosphamide or rituximab.
Plasmapheresis is recommended in rapidly progressive renal failure or
pulmonary hemorrhage. Remission is induced in 85–90% of patients,
but relapse is common. Steroids are tapered soon after acute inflammation subsides. Maintenance therapy includes low-dose steroids and
cyclophosphamide or less toxic agents such as azathioprine, methotrexate, or rituximab for up to a year to minimize the risk of relapse.
Granulomatosis with Polyangiitis Patients with this disease
classically present with fever, purulent rhinorrhea, nasal ulcers, sinus
pain, polyarthralgias/arthritis, cough, hemoptysis, shortness of breath,
hematuria, and subnephrotic proteinuria; occasionally, there may be
cutaneous purpura and mononeuritis multiplex. Patients may present
without renal involvement, although most of these patients develop
renal injury later. Chest x-ray often reveals nodules and persistent
infiltrates, sometimes with cavities. Biopsy of involved tissue will
show a small-vessel vasculitis and adjacent noncaseating granulomas.
Renal biopsies during active disease demonstrate segmental necrotizing
glomerulonephritis without immune deposits and have been classified
as focal, mixed, crescentic, or sclerotic (see Fig. A4-13). The disease
is more common in patients exposed to silica dust and those with
α1
-antitrypsin deficiency, which is an inhibitor of PR3. Relapse after
achieving remission is common and is more common in patients with
granulomatosis with polyangiitis than the other ANCA-associated vasculitis, necessitating diligent follow-up care. Although associated with
an unacceptable high mortality rate without treatment, the greatest
threat to patients, especially elderly patients in the first year of therapy,
is from adverse events, which are often secondary to treatment, rather
than active vasculitis. Patients should also be monitored long term for
malignancy after immunosuppressive therapy.
Microscopic Polyangiitis Clinically, these patients look somewhat similar to those with granulomatosis with polyangiitis, except
they rarely have significant lung disease or destructive sinusitis. The
distinction is made on biopsy, where the vasculitis in microscopic
polyangiitis is without granulomas. Some patients will also have injury
limited to the capillaries and venules.
Churg-Strauss Syndrome When small-vessel vasculitis is associated with peripheral eosinophilia, cutaneous purpura, mononeuritis,
asthma, and allergic rhinitis, a diagnosis of Churg-Strauss syndrome
(eosinophilic granulomatosis with polyangiitis [EGPA]) is considered.
Hypergammaglobulinemia, elevated levels of serum IgE, or the presence of rheumatoid factor sometimes accompanies the allergic state.
Lung inflammation, including fleeting cough and pulmonary infiltrates, often precedes the systemic manifestations of disease by years;
lung manifestations are rarely absent. A third of patients may have
exudative pleural effusions associated with eosinophils. Small-vessel
vasculitis and focal segmental necrotizing glomerulonephritis without
immune deposits can be seen on renal biopsy, usually absent eosinophils or granulomas. The cause of Churg-Strauss syndrome is autoimmune, but the inciting factors are unknown.
■ C3
GLOMERULOPATHIES
C3
glomerulopathy is a recent disease classification that is defined by
the glomerular accumulation of C3
with little or no immunoglobulin
and encompasses dense deposit disease (DDD), formerly MPGN type
II (see below), and C3
glomerulonephritis (C3
GN) (Table 314-4). DDD
is defined morphologically by dense deposits forming ribbons in the
GBM. In the absence of this specific morphology, the entity is categorized as C3
GN. Both are associated with the presence of a complement
mutation believed to cause the renal pathology, including mutations in
the complement factor H regulatory (CFHR) protein genes. DDD is
primarily a disease of children and young adults, whereas the other C3
glomerulopathies are reported to present in an older age group (mean
age 30). By definition, kidneys with C3
glomerulopathy show sole or
dominant staining for C3
but can have variable light microscopy, with
mesangial proliferative or membranoproliferative patterns seen most
commonly. Morphologically, many cases are not distinguishable from
recovering postinfectious glomerulonephritis. Patients with DDD present with proteinuria, which may be nephrotic range, and/or hematuria,
which may be macroscopic or microscopic. Partial lipodystrophy and
Drusen bodies in the retina may also be present. Prognosis is poor,
with 50% of patients progressing to ESRD. C3
GN patients are clinically
less well defined, but approximately two-thirds have hematuria and
one-third have proteinuria. C3
levels are low with normal C4
, and C3
nephritic factor is present in most patients with DDD and less commonly in C3
GN. Abnormalities in factor H, soluble C5b-9, paraprotein
detection, and specific CFHR genetic mutations should be assessed as
well. Screening family members may be indicated. The optimal therapies remain undefined but include inhibition of the renin-angiotensin
TABLE 314-4 Membranoproliferative Glomerulonephritis:
Immunoglobulin-Mediated
Type I Disease—Most Common
Idiopathic
Infection: Subacute bacterial endocarditis, hepatitis B and C, fungal and
parasitic infections
Autoimmune diseases: Systemic lupus erythematosus, cryoglobulinemia,
Sjögren’s
Monoclonal gammopathies: Monoclonal gammopathy of undetermined
significance, myeloma, monoclonal gammopathy of renal significance
Cancer: Lung, breast, and ovary (germinal)
Type II Disease
Idiopathic
Dense deposit disease (immunoglobulin-mediated)
Type III Disease
Idiopathic
C3
Glomerulopathy: C3
Dominant, Non-Immunoglobulin-Mediated
Dense Deposit Disease (C3
dominant)
Idiopathic
Specific genetic mutations and/or autoantibodies to alternate complement
pathway factors or regulatory factors of alternate complement pathway
C3
Glomerulonephritis
Specific genetic mutations and/or autoantibodies to alternate complement
pathway factors or regulatory factors of alternate complement pathway
2341 Glomerular Diseases CHAPTER 314
system, lipid lowering, steroids, and other immunosuppressants. Evidence suggests a benefit of therapy with eculizumab, a monoclonal
antibody directed at C5
, which is activated by C3.
■ MEMBRANOPROLIFERATIVE
GLOMERULONEPHRITIS
MPGN is characterized by thickening of the GBM with mesangioproliferative changes often leading to a lobular appearance of the
glomerular tuft; 70% of patients have hypocomplementemia. MPGN
is rare in African Americans, and idiopathic disease usually presents
in childhood or young adulthood. MPGN has been subdivided based
on histology into type I, type II, and type III disease. Type I MPGN is
immune complex–mediated and commonly associated with persistent
hepatitis B and C, fungal and parasitic infections, SBE, autoimmune
diseases such as lupus or cryoglobulinemia, or monoclonal gammopathies, including monoclonal gammopathy of renal significance
(MGRS), where the only clinically apparent manifestations are in
the kidney (Table 314-4). Types II and III MPGN can be idiopathic
and immunoglobulin-mediated disease (driven by the classical complement pathway), but the vast majority of cases formerly defined as
MPGN type II or III are non-immunoglobulin-mediated and driven
by the alternate complement pathway.
Type I MPGN, the most proliferative of the three types, shows
mesangial proliferation with lobular segmentation on renal biopsy and
mesangial interposition between the capillary basement membrane
and endothelial cells, producing a double contour sometimes called
tram-tracking (see Fig. A4-9). (See Glomerular Schematic 3.) Subendothelial deposits with low serum levels of C3
are typical, although
50% of patients have normal levels of C3
and occasional intramesangial
deposits. Low serum C3
and a dense thickening of the GBM containing
ribbons of dense deposits and C3
characterize type II MPGN, dense
deposit disease (see Fig. A4-10). Classically, the glomerular tuft has
a lobular appearance; intramesangial deposits are rarely present, and
subendothelial deposits are generally absent. Proliferation in type III
MPGN is less common than the other two types and is often focal;
mesangial interposition is rare, and subepithelial deposits as well as
subendothelial deposits can occur along widened segments of the
GBM that appear laminated and disrupted.
Classic type I MPGN is secondary to glomerular deposition of
circulating immune complexes or their in situ formation. Patients
with MPGN present with proteinuria, hematuria, and pyuria (30%);
systemic symptoms of fatigue and malaise that are most common in
children with type I disease; or an acute nephritic picture with RPGN
and a speedy deterioration in renal function in up to 25% of patients.
Low serum C3
levels are common. Fifty percent of patients with MPGN
develop ESRD 10 years after diagnosis, and 90% have renal insufficiency after 20 years. Nephrotic syndrome, hypertension, and renal
insufficiency all predict poor outcome. In the presence of proteinuria,
treatment with inhibitors of the renin-angiotensin system is prudent.
Evidence supports the efficacy of treatment of primary MPGN with steroids, particularly in children. There are reports of efficacy with other
immunosuppressive drugs. If defects in the complement pathway are
found, treatment with eculizumab is of benefit. In secondary MPGN,
treating the associated infection, autoimmune disease, or neoplasms is
of demonstrated benefit. Patients with primary MPGN are well known
to be at risk for not only a histologic recurrence in the transplanted
kidney but also a clinically significant recurrence with loss of graft
function.
■ MESANGIOPROLIFERATIVE
GLOMERULONEPHRITIS
Mesangioproliferative glomerulonephritis is characterized by expansion of the mesangium, sometimes associated with mesangial hypercellularity; thin, single contoured capillary walls; and mesangial
immune deposits. Mesangioproliferative pathology may be seen in IgA
nephropathy, Plasmodium falciparum malaria, resolving postinfectious
glomerulonephritis, and class II nephritis from lupus, all of which can
have a similar histologic appearance. With these secondary entities
excluded, the diagnosis of primary mesangioproliferative glomerulonephritis is made in <15% of renal biopsies.
NEPHROTIC SYNDROME
Nephrotic syndrome classically presents with heavy proteinuria, minimal hematuria, hypoalbuminemia, hypercholesterolemia, edema,
and hypertension. If left undiagnosed or untreated, some of these
syndromes will progressively damage enough glomeruli to cause a fall
in GFR, producing renal failure. Multiple studies have noted that the
higher the 24-h urine protein excretion, the more rapid is the decline
in GFR.
Therapies for various causes of nephrotic syndrome are noted
under individual disease headings below. In general, all patients with
hypercholesterolemia secondary to nephrotic syndrome should be
treated with lipid-lowering agents because they are at increased risk
for cardiovascular disease. Edema secondary to salt and water retention can be controlled with the use of diuretics, avoiding intravascular
volume depletion. Venous complications secondary to the hypercoagulable state associated with nephrotic syndrome can be treated with
anticoagulants. The losses of various serum binding proteins, such as
thyroid-binding globulin, lead to alterations in functional tests. Lastly,
proteinuria itself is hypothesized to be nephrotoxic, and treatment of
proteinuria with inhibitors of the renin-angiotensin system can lower
urinary protein excretion.
■ MINIMAL CHANGE DISEASE
MCD, sometimes known as nil lesion, causes 70–90% of nephrotic syndrome in childhood but only 10–15% of nephrotic syndrome in adults.
MCD usually presents as a primary renal disease but can be associated
with several conditions, including Hodgkin’s disease, allergies, use
of nonsteroidal anti-inflammatory agents or lithium, infections, and
other glomerular diseases. MCD on renal biopsy shows no glomerular
lesion by light microscopy and is negative for deposits by immunofluorescent microscopy or occasionally shows small amounts of IgM in the
mesangium (see Fig. A4-1). (See Glomerular Schematic 4.) Electron
microscopy, however, consistently demonstrates an effacement of the
foot processes supporting the epithelial podocytes with weakening of
slit-pore membranes. The pathogenesis of this lesion is unclear. Most
agree there is a disturbance related to T-cell responses, or expression of
CD80 or CD40/40L may alter capillary charge and podocyte integrity;
interestingly, the use of checkpoint inhibitors as chemotherapy is associated with MCD. There also is some circumstantial evidence for the
presence of preceding allergies, altered cell-mediated immunity during
viral infections, and a high frequency of remissions with steroids.
MCD presents clinically with the abrupt onset of edema and nephrotic syndrome accompanied by acellular urinary sediment. Average
urine protein excretion reported in 24 h is 10 g with severe hypoalbuminemia. Less common clinical features include hypertension (30%
in children, 50% in adults), microscopic hematuria (20% in children,
MEMBRANOPROLIFERATIVE
GLOMERULONEPHRITIS TYPE I
Subendothelial
Widened deposits mesangial
Macrophage and
mesangial cells
Mesangial
interposition
Glomerular schematic 3
2342 PART 9 Disorders of the Kidney and Urinary Tract
33% in adults), atopy or allergic symptoms (40% in children, 30% in
adults), and decreased renal function (25–40%), which often returns to
normal after remission of the nephrotic syndrome. The appearance of
acute renal failure in adults is often seen more commonly in patients
with low serum albumin and intrarenal edema (nephrosarca) that is
responsive to diuretics. This presentation must be distinguished from
acute renal failure secondary to hypovolemia. Acute tubular necrosis and interstitial inflammation are also reported. In children, the
abnormal urine principally contains albumin with minimal amounts
of higher-molecular-weight proteins and is sometimes called selective
proteinuria. Although up to 30% of children have a spontaneous
remission, most children today are treated with steroids; only children
who are nonresponders are biopsied. Primary responders are patients
who have a complete remission (<0.2 mg/24 h of proteinuria), often
abruptly after a single course of prednisone; steroid-dependent patients
relapse as their steroid dose is tapered. Frequent relapsers have two or
more relapses in the 6 months following taper, and steroid-resistant
patients fail to respond to steroid therapy. Adults are not considered
steroid-resistant until after 4 months of therapy. Ninety to 95% of children will develop a complete remission after 8 weeks of steroid therapy,
and 80–85% of adults will achieve complete remission, but only after a
longer course of 20–24 weeks. Patients with steroid resistance may have
FSGS on repeat biopsy. If the first renal biopsy does not have a sample
of deeper corticomedullary glomeruli, then the correct diagnosis of
FSGS may be missed.
Relapses occur in 70–75% of children after the first remission, and
early relapse predicts multiple subsequent relapses, as do high levels of
basal proteinuria. The frequency of relapses decreases after puberty.
There is an increased risk of relapse following the rapid tapering of
steroids in all groups. Relapses are less common in adults but are more
resistant to subsequent therapy. Prednisone is first-line therapy, either
given daily or on alternate days. Other immunosuppressive drugs, such
as cyclophosphamide, chlorambucil, and mycophenolate mofetil, are
saved for frequent relapsers, steroid-dependent patients, or steroidresistant patients. Cyclosporine can induce remission, but relapse is
also common when cyclosporine is withdrawn. The long-term prognosis in adults is less favorable when acute renal failure or steroid
resistance occurs.
■ FOCAL SEGMENTAL GLOMERULOSCLEROSIS
FSGS refers to a pattern of renal injury characterized by segmental
glomerular scars that involve some but not all glomeruli (focal); the
clinical findings of FSGS largely manifest as proteinuria. When the
secondary and genetic causes of FSGS are eliminated (Table 314-5),
the remaining patients are considered to have primary FSGS. The
incidence of this disease is increasing, and it now represents up to onethird of cases of nephrotic syndrome in adults and one-half of cases of
nephrotic syndrome in African Americans. The pathogenesis of FSGS
has multiple possible mechanisms including a circulating permeability
factor, an adaptive response to glomerular hypertrophy or hyperfiltration, and podocyte abnormalities associated with direct toxic injury or
genetic mutations. Risk polymorphisms at the APOL1 locus expressed
in podocytes substantially explain the increased burden of FSGS
among African Americans.
The pathologic changes of FSGS are most prominent in glomeruli
located at the corticomedullary junction (see Fig. A4-2), so if the renal
biopsy specimen is from superficial tissue, the lesions can be missed,
which sometimes leads to a misdiagnosis of MCD. In addition to focal
and segmental scarring, other variants have been described, including
cellular lesions with endocapillary hypercellularity and heavy proteinuria; collapsing glomerulopathy (see Fig. A4-3) with segmental or
global glomerular collapse and a rapid decline in renal function; a hilar
stalk lesion (see Fig. A4-4); or the glomerular tip lesion (see Fig. A4-5),
which may have a better prognosis. (See Glomerular Schematic 5.)
FSGS can present with hematuria, hypertension, any level of
proteinuria, and renal insufficiency. Nephrotic-range proteinuria,
African-American race, and renal insufficiency are associated with a
poor outcome, with 50% of patients reaching renal failure in 6–8 years.
FSGS rarely remits spontaneously, but treatment-induced remission
of proteinuria significantly improves prognosis. Treatment of patients
with FSGS should include inhibitors of the renin-angiotensin system.
Patients with primary FSGS with nephrotic-range proteinuria can be
treated with steroids but respond far less often and after a longer course
of therapy than patients with MCD. Proteinuria remits in only 20–45%
of patients receiving a course of steroids over 6–12 months. Limited
evidence suggests the use of cyclosporine in steroid-responsive patients
helps ensure remissions. Relapse frequently occurs after cessation of
cyclosporine therapy, and cyclosporine itself can lead to a deterioration
of renal function due to its nephrotoxic effects. A role for other agents
that suppress the immune system such as rituximab or mycophenolate
mofetil has not been established. Immunosuppressive therapy is not
indicated in secondary or genetic FSGS. FSGS recurs in 30% of renal
transplants, more commonly in primary FSGS, less commonly in secondary FSGS, and rarely in genetic FSGS. In recurrent posttransplant
FSGS, many patients will achieve a full or partial remission with plasmapheresis. The treatment of secondary FSGS typically involves treating the underlying cause and controlling proteinuria. There is no role
for steroids or other immunosuppressive agents in secondary FSGS.
MINIMAL
CHANGE DISEASE
Glomerular schematic 4 TABLE 314-5 Focal Segmental Glomerulosclerosis
Primary focal segmental glomerulosclerosis
Secondary focal segmental glomerulosclerosis
Adaptive response to hyperfiltration/reduced renal mass, obesity
Viruses: HIV/hepatitis B/parvovirus
Hypertensive nephropathy
Reflux nephropathy
Cholesterol emboli
Drugs: Heroin/analgesics/bisphosphonates/ecstasy
Oligomeganephronia
Sickle cell disease
Radiation nephritis
Familial podocytopathies
NPHS1 mutation/nephrin
NPHS2 mutation/podocin
PLCE1 mutation/phospholipase Cε1
INF2 mutation/inverted formin 2
WT1 mutation/Wilms tumor
TRPC6 mutation/cation channel
ACTN4 mutation/actinin
α-Galactosidase A deficiency/Fabry’s disease
N-Acetylneuraminic acid hydrolase deficiency/nephrosialidosis
2343 Glomerular Diseases CHAPTER 314
■ MEMBRANOUS GLOMERULONEPHRITIS
MGN, or membranous nephropathy as it is sometimes called, accounts
for ~25% of cases of nephrotic syndrome in adults, with a peak incidence between the ages of 30 and 50 years and a male-to-female ratio of
2:1. IMN is rare in childhood and the most common cause of nephrotic
syndrome in the elderly. In 20–30% of cases, MGN is secondary and is
associated with a malignancy (solid tumors of the breast, lung, colon),
infection (hepatitis B, syphilis, malaria, schistosomiasis), rheumatologic disorders such as lupus or rheumatoid arthritis, IgG4 diseases, or
drug exposure (Table 314-6).
Uniform thickening of the basement membrane along the peripheral capillary loops is seen by light microscopy on renal biopsy (see
Fig. A4-7); this thickening needs to be distinguished from that seen
in diabetes and amyloidosis. (See Glomerular Schematic 6.) Immunofluorescence demonstrates diffuse granular deposits of IgG and C3
,
Afferent
arteriole
Efferent
arteriole
Collapsed
capillary
and scar
Detachment
of cell from
GBM
FOCAL
SCLEROSING
GLOMERULONEPHRITIS
Proliferation of
subepithelial cells
Glomerular schematic 5
and electron microscopy typically reveals electron-dense subepithelial
deposits. While different stages (I–V) of progressive membranous
lesions have been described, some published analyses indicate the
degree of tubular atrophy or interstitial fibrosis is more predictive
of progression than is the stage of glomerular disease. The presence
of subendothelial deposits or the presence of tubuloreticular inclusions strongly points to a diagnosis of membranous lupus nephritis,
which may precede the extrarenal manifestations of lupus. In 70% of
cases of IMN, autoantibodies against the M-type phospholipase A2
TABLE 314-6 Membranous Glomerulonephritis
Primary/idiopathic membranous glomerulonephritis
Secondary membranous glomerulonephritis
Infection: Hepatitis B and C, syphilis, malaria, schistosomiasis, leprosy, filariasis
Cancer: Breast, colon, lung, stomach, kidney, esophagus, neuroblastoma
Drugs: Gold, mercury, penicillamine, nonsteroidal anti-inflammatory agents,
probenecid, antitumor necrosis factor agents
Autoimmune diseases: Systemic lupus erythematosus, rheumatoid arthritis,
primary biliary cirrhosis, dermatitis herpetiformis, bullous pemphigoid,
myasthenia gravis, Sjögren’s syndrome, Hashimoto’s thyroiditis
Other systemic diseases: Fanconi’s syndrome, sickle cell anemia, diabetes,
Crohn’s disease, sarcoidosis, Guillain-Barré syndrome, Weber-Christian disease,
angiofollicular lymph node hyperplasia, IgG4 disease
MEMBRANOUS
GLOMERULONEPHRITIS
Foot process
fusion
Subepithelial
deposits
Glomerular schematic 6
2344 PART 9 Disorders of the Kidney and Urinary Tract
receptor circulate and bind to a conformational epitope present in the
PLA2R on human podocytes, producing characteristic in situ deposits. Three to 10% of IMN patients alternatively have autoantibodies
to thrombospondin type-1 domain containing 7A (THSD7A). Both
antigens co-localize within glomerular subepithelial deposits with IgG4
(PLA2R). Other renal diseases do not involve these autoantibodies.
In most cases of secondary membranous nephropathy, these autoantibodies are absent, with rare reports of autoantibodies to PLA2R
in membranous glomerulopathy associated with hepatitis B, cancer,
and sarcoidosis. Circulating deposits and glomerular deposits of these
autoantibodies have correlated with the likelihood of a spontaneous
remission, severity of IMN, and the response to therapy. Eighty percent
of patients with MGN present with nephrotic syndrome and nonselective proteinuria. Microscopic hematuria is seen but less commonly
than in IgA nephropathy or FSGS. Spontaneous remissions occur in
20–33% of patients and often occur late in the course, which makes
treatment decisions difficult. One-third of patients continue to have
relapsing nephrotic syndrome but maintain normal renal function,
and approximately another third of patients develop renal failure or die
from the complications of nephrotic syndrome. Male gender, older age,
hypertension, and the persistence of nephrotic-range proteinuria are
associated with worse prognosis. Although thrombotic complications
are a feature of all nephrotic syndromes, MGN has the highest reported
incidences of renal vein thrombosis, pulmonary embolism, and deepvein thrombosis. Prophylactic anticoagulation is controversial but has
been recommended for patients with hypoalbuminemia.
In addition to the treatment of edema, dyslipidemia, and hypertension, inhibition of the renin-angiotensin system is recommended.
Therapy with immunosuppressive drugs is also recommended for
patients with primary MGN and persistent proteinuria (>3.0 g/24 h).
The choice of immunosuppressive drugs for therapy is controversial,
but current recommendations are to treat with steroids and cyclophosphamide, chlorambucil, mycophenolate mofetil, or cyclosporine or rituximab, an anti-CD20 antibody directed at B cells. Attaining remission
is associated with a good long-term prognosis.
■ DIABETIC NEPHROPATHY
Diabetic nephropathy is the single most common cause of chronic
renal failure in the United States and worldwide. The dramatic increase
in the number of patients with diabetic nephropathy reflects the epidemic increase in obesity and type 2 diabetes mellitus. Approximately
40% of patients with diabetes develop nephropathy, but due to the
higher prevalence of type 2 diabetes (90%) compared to type 1 (10%),
the majority of patients with diabetic nephropathy have type 2 disease.
Renal lesions are more common in African-American, Native-American,
Polynesian, and Maori populations. Risk factors for the development
of diabetic nephropathy include hyperglycemia, hypertension, dyslipidemia, smoking, a family history of diabetic nephropathy, and gene
polymorphisms.
Within 1–2 years after the onset of clinical diabetes, morphologic
changes appear in the kidney. Thickening of the GBM is a sensitive
indicator for the presence of diabetes but correlates poorly with the
presence or absence of nephropathy. The composition of the GBM is
altered notably with a loss of heparan sulfate moieties that form the
negatively charged filtration barrier resulting in increased filtration of
serum proteins into the urine. The expansion of the mesangium due
to the accumulation of extracellular matrix correlates with the clinical
manifestations of diabetic nephropathy (see stages in Fig. A4-20).
This expansion in mesangial matrix is associated with the development
of mesangial sclerosis. Some patients also develop eosinophilic, PAS+
nodules called nodular glomerulosclerosis or Kimmelstiel-Wilson nodules.
Immunofluorescence microscopy often reveals the nonspecific deposition of IgG (at times in a linear pattern) or complement staining
without immune deposits on electron microscopy. Prominent vascular
changes are frequently seen with hyaline and hypertensive arteriosclerosis. This is associated with varying degrees of chronic glomerulosclerosis and tubulointerstitial changes. Renal biopsies from patients
with types 1 and 2 diabetic nephropathies with albuminuria are largely
indistinguishable. Patients with type 2 diabetes without albuminuria
are classified as having diabetic kidney disease as opposed to diabetic
nephropathy and may have myriad pathologic findings.
Multiple lines of evidence support an important role for changes in
glomerular hemodynamics including increases in glomerular capillary
pressure and glomerular hyperfiltration in these pathologic changes.
Hyperglycemia activates the renin-angiotensin-aldosterone system
and also alters insulin-like growth factor, reactive oxygen species, and
endothelin 1. Diabetes upregulates the sodium-glucose cotransporters
(SGLT1 and SGLT2) in the proximal tubule, resulting in decreased
distal delivery of sodium to the macula densa and further glomerular
hyperfiltration. Sustained glomerular hypertension increases matrix
production and alterations in the GBM with disruption in the filtration
barrier. Other factors that alter matrix production include the accumulation of advanced glycosylation end products, circulating factors
including growth hormone, connective tissue growth factor, TGF-β,
and dyslipidemia.
The natural history of diabetic nephropathy has been historically
well characterized in the ~40% of diabetics who develop it as a progression from glomerular hyperfiltration and renal hypertrophy to
increasing albuminuria followed by declining GFR and ESRD. However, since the onset of type 1 diabetes is readily identifiable and the
onset of type 2 diabetes is not, a patient newly diagnosed with type 2
diabetes may present with advanced diabetic nephropathy. Albuminuria
and decreased GFR are potent risk factors for cardiovascular disease,
with some patients dying before they reach ESRD. Furthermore, contemporary studies reveal that up to 24% of patients with type 1 diabetes
and 50% with type 2 diabetes and chronic kidney disease may be normoalbuminuric. It is unknown whether this alteration in the natural
history reflects contemporary effective interventions or perhaps
other kidney diseases that happen to occur in patients with diabetes.
The degree of early glomerular hyperfiltration does correlate with the
development of albuminuria and declining GFR. Albuminuria in the
range of 30–300 mg/24 h is called microalbuminuria (Table 314-1).
Microalbuminuria appears 5–10 years after the onset of diabetes. It is
currently recommended to test patients with type 1 disease for microalbuminuria 5 years after diagnosis of diabetes and yearly thereafter and,
because the time of onset of type 2 diabetes is often unknown, to test
type 2 patients at the time of diagnosis of diabetes and yearly thereafter.
Microalbuminuria classically progresses over 5–10 years to proteinuria
and declining GFR, but in contemporary studies, greater heterogeneity is reported with regression to normoalbuminuria; however,
albuminuria remains the single most important predictor of a faster
decline in GFR. Regression of albuminuria with a treatment intervention is a good prognostic sign. Proteinuria in diabetic nephropathy
can be variable, ranging from 500 mg to 25 g/24 h. More than 90% of
patients with type 1 diabetes and nephropathy have diabetic retinopathy, so the absence of retinopathy in type 1 patients with proteinuria
should prompt consideration of a diagnosis other than diabetic nephropathy; only 60% of patients with type 2 diabetes with nephropathy
have diabetic retinopathy. There is a significant correlation between
the presence of retinopathy and the presence of Kimmelstiel-Wilson
nodules (see Fig. A4-20). Even with advanced chronic kidney disease,
patients with diabetic nephropathy will have enlarged kidneys. Using
the above data, and in the absence of other clinical or serologic data
suggesting another disease, diabetic nephropathy is usually diagnosed
without a renal biopsy. The risk of progression to ESRD is influenced
by treatment and other risk factors, and reports vary from a decline of
1.8–14 mL/min per year. Survival on dialysis is worse for patients with
diabetes. Renal transplantation results in better survival than dialysis.
Good evidence supports the benefits of blood sugar and blood pressure control, inhibitors of the renin-angiotensin-aldosterone system
(RAAS), and inhibitors of SGLT2 in retarding the progression of diabetic nephropathy. In patients with type 1 diabetes, intensive control of
blood sugar clearly prevents the development or progression of diabetic
nephropathy. The evidence for benefit of intensive blood glucose control in patients with type 2 diabetes is less certain, with current studies
reporting conflicting results.
Controlling systemic blood pressure decreases renal and cardiovascular adverse events in this high-risk population. The vast majority of
2345 Glomerular Diseases CHAPTER 314
patients with diabetic nephropathy require three or more antihypertensive drugs to achieve this goal. Drugs that inhibit the RAAS (ACE
inhibitors, angiotensin receptor blockers [ARBs]), independent of their
effects on systemic blood pressure, have been shown in large clinical
trials to slow the progression of diabetic nephropathy at early (microalbuminuria) and late (proteinuria with reduced glomerular filtration)
stages. Evidence suggests increased risk for cardiovascular adverse
events without increased efficacy in patients with a combination of
two drugs (ACE inhibitors, ARBs, or renin inhibitors) that suppress
several components of the RAAS. In patients with type 2 diabetes and
kidney disease with albuminuria, the risk of kidney failure and cardiovascular events was lower in those receiving SGLT2 in addition to
inhibitors of the RAAS. Ongoing trials are examining the hypotheses
that other agents may be of benefit, including endothelin antagonists
and aldosterone antagonists.
■ GLOMERULAR DEPOSITION DISEASES
Plasma cell dyscrasias producing excess light chain immunoglobulin
sometimes lead to the formation of glomerular and tubular deposits
that cause heavy proteinuria and renal failure; the same is true for the
accumulation of serum amyloid A protein fragments seen in several
inflammatory diseases. This broad group of proteinuric patients has
glomerular deposition disease.
Light Chain Deposition Disease The biochemical characteristics of nephrotoxic light chains produced in patients with light
chain malignancies confer renal injury; that of either cast nephropathy (see Fig. A4-17), which causes renal failure but not heavy proteinuria or amyloidosis, or light chain deposition disease (LCDD)
(see Fig. A4-16), which produces proteinuria with renal failure.
These latter patients produce kappa light chains that do not have the
biochemical features necessary to form amyloid fibrils. Instead, they
self-aggregate and form granular deposits along the glomerular capillary and mesangium or, more prominently, in the tubular basement
membrane and Bowman’s capsule. Light chain deposits are not fibrillar
and do not stain with Congo red, but they are easily detected with anti–
light chain antibody. A combination of the light chain rearrangement,
self-aggregating properties at neutral pH, and abnormal metabolism
probably contributes to the deposition.
Monoclonal Plasma Cell Disorders Multiple myeloma, Waldenström’s macroglobulinemia, or lymphoma may be present, as well
as heart, liver, and pulmonary involvement. The monoclonal protein
may be found with serum electrophoresis or with serum free light
chain analysis. Nephrotic syndrome may develop, and ~70% of patients
progress to dialysis. Treatment for LCDD is treatment of the primary
disease and, if possible, autologous stem cell transplantation. Rarely,
truncated heavy chains similarly cause nonamyloid deposits.
Renal Amyloidosis Most renal amyloidosis is either the result of
primary fibrillar deposits of immunoglobulin light chains known as
amyloid L (AL) or secondary to fibrillar deposits of serum amyloid A
(AA) protein fragments (Chap. 112). Even though both occur for different reasons, their clinicopathophysiology is quite similar. Amyloid
infiltrates the liver, heart, peripheral nerves, carpal tunnel, upper pharynx, and kidney, producing restrictive cardiomyopathy, hepatomegaly,
macroglossia, and heavy proteinuria sometimes associated with renal
vein thrombosis. In contrast to LCDD, amyloid renal deposits are
fibrillar, stain with Congo red, and contain predominantly the variable
region of lambda chains (see Fig. A4-15). In systemic AL amyloidosis,
also called primary amyloidosis, light chains produced in excess by
clonal plasma cell dyscrasias are made into fragments by macrophages
so they can self-aggregate at acid pH. Approximately 10% of patients
have overt myeloma as defined by CRAB (hypercalcemia, renal insufficiency, anemia, or lytic bone lesions). Nephrotic syndrome is common,
and ~20% of patients progress to dialysis. AA amyloidosis is sometimes
called secondary amyloidosis and also presents as nephrotic syndrome.
It is due to deposition of β-pleated sheets of serum amyloid A protein,
an acute phase reactant. Patients with AA amyloid have associated
inflammatory diseases including rheumatoid arthritis, ankylosing
spondylitis, psoriatic arthritis, juvenile inflammatory arthritis, and
familial Mediterranean fever. An increasing proportion of patients
have unidentified chronic inflammation; this may reflect better treatments for the previously associated diseases or a rise in chronic inflammation due to obesity. Fragments of serum amyloid A protein increase
and self-aggregate by attaching to receptors for advanced glycation end
products in the extracellular environment; nephrotic syndrome is common, and ~40–60% of patient’s progress to dialysis. Serum-free light
chain analysis is useful in the early diagnosis and follow-up of disease
progression. Biopsy of involved liver or kidney is diagnostic 90% of the
time when the pretest probability is high; abdominal fat pad aspirates
are positive ~70% of the time, but apparently less so when looking
for AA amyloid. Amyloid deposits are distributed along blood vessels
and in the mesangial regions of the kidney. The treatment for primary
amyloidosis, melphalan, and autologous hematopoietic stem cell transplantation (HCT) can delay the course of disease. Patients who are not
candidates for HCT often receive bortezomib-based regimens. Secondary amyloidosis is also relentless unless the primary disease can be
controlled. Some new drugs in development that disrupt the formation
of fibrils may be available in the future.
Fibrillary and Immunotactoid Glomerulopathies Fibrillary
and immunotactoid glomerulopathies are rare (<1.0% of renal biopsies), morphologically defined diseases characterized by glomerular
accumulation of nonbranching randomly arranged fibrils that are
Congo red negative. Fibrillary glomerulopathy accounts for 85–90%
of cases and is identified by the presence of the protein DnaJ heat
shock protein family B9 (DNAJB9) in the glomeruli, which is absent
in the rarer immunotactoid glomerulopathy. In both, glomerular and
mesangial deposits contain oligoclonal or oligotypic immunoglobulins
and complement, with 12- to 24-nm fibrils in fibrillary glomerulopathy
and >30-nm fibrils organized into microtubules in immunotactoid
glomerulopathy. The cause of this “nonamyloid” glomerulopathy is
mostly idiopathic; reports of fibrillary glomerulonephritis describe
associations with malignancy, autoimmune disease, and monoclonal
gammopathy, and immunotactoid glomerulopathy has been associated with lymphoma or plasma cell disorders. Both disorders appear
in adults aged 40–80 years old, with moderate to heavy proteinuria
(100%), hematuria (70%), renal insufficiency (50%), and a wide variety
of histologic lesions, including DPGN, MPGN, MGN, or mesangioproliferative glomerulonephritis. Most patients have disease limited to the
kidney. Patients should be screened for associated disorders. Half of
patients develop renal failure over a few years. There is no consensus
on treatment of this uncommon disorder, although rituximab has been
reported to remit proteinuria. These diseases can recur in the renal
transplant.
■ FABRY’S DISEASE
Fabry’s disease is an X-linked inborn error of globotriaosylceramide metabolism secondary to deficient lysosomal α-galactosidase A
(alpha-Gal A) activity, resulting in excessive intracellular storage of
globotriaosylceramide. Affected organs include the vascular endothelium, heart, brain, and kidneys. Classically, Fabry’s disease presents in
childhood in males with acroparesthesias, angiokeratoma, cornea verticillate, and hypohidrosis. Over time, male patients develop cardiomyopathy, cerebrovascular disease, and renal injury, with an average age
of death around 50 years of age. Hemizygotes with hypomorphic mutations sometimes present in the fourth to sixth decade with single-organ
involvement. Rarely, dominant-negative alpha-Gal A mutations or
female heterozygotes with unfavorable X inactivation present with
mild single-organ involvement. Rare females develop severe manifestations including renal failure but do so later in life than males. Renal
biopsy reveals enlarged glomerular visceral epithelial cells packed with
small clear vacuoles containing globotriaosylceramide; vacuoles may
also be found in parietal and tubular epithelia (see Fig. A4-18).
These vacuoles of electron-dense materials in parallel arrays (zebra
bodies) are easily seen on electron microscopy. Ultimately, renal
biopsies reveal FSGS. The nephropathy of Fabry’s disease typically
presents in the third decade as mild to moderate proteinuria, sometimes with microscopic hematuria or nephrotic syndrome. Urinalysis
may reveal oval fat bodies and birefringent glycolipid globules under
2346 PART 9 Disorders of the Kidney and Urinary Tract
polarized light (Maltese cross). Measurement of alpha-Gal A activity
and mutational analysis of the gene is diagnostic, with renal biopsies
sometimes helpful. Progression to renal failure occurs by the fourth
or fifth decade. Treatment with inhibitors of the renin-angiotensin
system is recommended. Treatment with recombinant alpha-Gal A or
migalastat, a chaperone that facilitates trafficking of alpha-Gal A, clears
microvascular endothelial deposits of globotriaosylceramide from the
kidneys, heart, and skin. In patients with advanced organ involvement
including chronic kidney disease, progression of disease occurs despite
enzyme replacement therapy. Variable responses to enzyme therapy
may be due to the occurrence of neutralizing antibodies or differences
in uptake of the enzyme. Graft and patient survival following renal
transplantation in patients with Fabry’s disease are similar to those of
other causes of ESRD.
PULMONARY-RENAL SYNDROMES
Several diseases can present with catastrophic hemoptysis and glomerulonephritis associated with varying degrees of renal failure. The
usual causes include Goodpasture’s syndrome, granulomatosis with
polyangiitis, microscopic polyangiitis, Churg-Strauss vasculitis, and,
rarely, Henoch-Schönlein purpura or cryoglobulinemia. Each of these
diseases can also present without hemoptysis and are discussed in detail
earlier in “Acute Nephritic Syndromes.” (See Glomerular Schematic 7.)
Pulmonary bleeding in this setting is life-threatening and often results in
airway intubation, and acute renal failure requires dialysis. Diagnosis is
difficult initially because biopsies and serologic testing take time. Treatment with plasmapheresis and methylprednisolone is often empirical
and temporizing until results of testing are available.
BASEMENT MEMBRANE SYNDROMES
All kidney epithelia, including podocytes, rest on basement membranes assembled into a planar surface through the interweaving of collagen IV with laminins, nidogen, and sulfated proteoglycans. Structural
abnormalities in GBM associated with hematuria are characteristic
of several familial disorders related to the expression of collagen IV
genes. The extended family of collagen IV contains six chains, which
are expressed in different tissues at different stages of embryonic
development. All epithelial basement membranes early in human
development are composed of interconnected triple-helical protomers rich in α1.α1.α2(IV) collagen. Some specialized tissues undergo a
developmental switch replacing α1.α1.α2(IV) protomers with an α3.α4.
α5(IV) collagen network; this switch occurs in the kidney (glomerular
and tubular basement membrane), lung, testis, cochlea, and eye, while
an α5.α5.α6(IV) network appears in skin, smooth muscle, and esophagus and along Bowman’s capsule in the kidney. This switch probably
occurs because the α3.α4.α5(IV) network is more resistant to proteases
and ensures the structural longevity of critical tissues. When basement
membranes are the target of glomerular disease, they produce moderate proteinuria, some hematuria, and progressive renal failure.
■ ANTI-GBM DISEASE
Autoimmune disease where antibodies are directed against the α3 NC1
domain of collagen IV produces an anti-GBM disease often associated
with RPGN and/or a pulmonary-renal syndrome called Goodpasture’s syndrome. Discussion of this disease is covered earlier in “Acute
Nephritic Syndromes.”
■ ALPORT’S SYNDROME
Classically, patients with Alport’s syndrome develop hematuria, thinning and splitting of the GBMs, and mild proteinuria (<1–2 g/24 h),
which appears late in the course, followed by chronic glomerulosclerosis leading to renal failure in association with sensorineural deafness.
Some patients develop lenticonus of the anterior lens capsule, “dot and
fleck” retinopathy, and rarely, leiomyomatosis. Approximately 85% of
patients with Alport’s syndrome have an X-linked inheritance of mutations in the α5(IV) collagen chain on chromosome Xq22–24. Female
RAPIDLY
PROGRESSIVE
GLOMERULONEPHRITIS
Glomerular schematic 7
2347 Glomerular Diseases CHAPTER 314
carriers have variable penetrance depending on the type of mutation
or the degree of mosaicism created by X inactivation. Fifteen percent
of patients have autosomal recessive disease of the α3(IV) or α4(IV)
chains on chromosome 2q35–37. Rarely, some kindred have an autosomal dominant inheritance of dominant-negative mutations in α3(IV)
or α4(IV) chains.
Pedigrees with the X-linked syndrome are quite variable in their
rate and frequency of tissue damage leading to organ failure. Seventy
percent of patients have the juvenile form with nonsense or missense
mutations, reading frame shifts, or large deletions and generally
develop renal failure and sensorineural deafness by age 30. Patients
with splice variants, exon skipping, or missense mutations of α-helical
glycines generally deteriorate after the age of 30 (adult form) with
mild or late deafness. Early severe deafness, lenticonus, or proteinuria
suggests a poorer prognosis. Usually females from X-linked pedigrees
have only microhematuria, but up to 25% of carrier females have been
reported to have more severe renal manifestations. Pedigrees with the
autosomal recessive form of the disease have severe early disease in
both females and males with asymptomatic parents.
Clinical evaluation should include a careful eye examination and
hearing tests. However, the absence of extrarenal symptoms does not
rule out the diagnosis. Since α5(IV) collagen is expressed in the skin,
some X-linked Alport’s patients can be diagnosed with a skin biopsy
revealing the lack of the α5(IV) collagen chain on immunofluorescent analysis. Patients with mutations in α3(IV) or α4(IV) require a
renal biopsy. Genetic testing can be used for the diagnosis of Alport’s
syndrome and the demonstration of the mode of inheritance. Early
in their disease, Alport’s patients typically have thin basement membranes on renal biopsy (see Fig. A4-19), which thicken over time into
multilamellations surrounding lucent areas that often contain granules
of varying density—the so-called split basement membrane. In any
Alport’s kidney, there are areas of thinning mixed with splitting of the
GBM. Tubules drop out, glomeruli scar, and the kidney eventually
succumbs to interstitial fibrosis. All affected members of a family with
X-linked Alport’s syndrome should be identified and followed, including mothers of affected males. Primary treatment is control of systemic
hypertension and use of ACE inhibitors to slow renal progression.
Although patients who receive renal allografts usually develop antiGBM antibodies directed toward the collagen epitopes absent in their
native kidney, overt Goodpasture’s syndrome is rare and graft survival
is good.
■ THIN BASEMENT MEMBRANE DISEASE
Thin basement membrane disease (TBMD), a relatively common
disorder characterized by persistent or intermittent, asymptomatic,
usually microscopic hematuria and rarely macroscopic hematuria
with flank pain, is not typically associated with proteinuria, hypertension, or loss of renal function or extrarenal disease. TBMD is often
familial, with pedigrees exhibiting an autosomal dominant pattern. It
usually presents in childhood in multiple family members and is also
called benign familial hematuria. Many cases of TBMD have genetic
defects in type IV collagen, but in contrast to Alport’s syndrome, the
disease behaves as an autosomal dominant disorder that in ~40% of
families segregates with the COL(IV) α3/COL(IV) α4 loci. Mutations
in these loci can result in a spectrum of disease, ranging from TBMD
to autosomal dominant or recessive Alport’s. The GBM shows diffuse
thinning compared to normal values for the patient’s age in otherwise
normal biopsies (see Fig. A4-19). The vast majority of patients have a
benign course.
■ NAIL-PATELLA SYNDROME
Patients with nail-patella syndrome develop iliac horns on the pelvis
and dysplasia of the dorsal limbs involving the patella, elbows, and
nails, variably associated with neural-sensory hearing impairment,
glaucoma, and abnormalities of the GBM and podocytes, leading to
hematuria, proteinuria, and FSGS. The syndrome is autosomal dominant, with haploinsufficiency for the LIM homeodomain transcription
factor LMX1B; pedigrees are extremely variable in the penetrance for
all features of the disease. LMX1B regulates the expression of genes
encoding α3 and α4 chains of collagen IV, interstitial type III collagen,
podocin, and CD2AP that help form the slit-pore membranes connecting podocytes. Mutations in the LIM domain region of LMX1B associate with glomerulopathy in 30–40% of patients and rarely progress to
renal failure. Proteinuria or isolated hematuria is discovered throughout life but usually by the third decade. On renal biopsy, pathognomic
rarefications containing clusters of collagen fibrils within the lamina
densa of the GBM are found, and FSGS may be present. Treatment is
nonspecific, but renin-angiotensin system inhibition is recommended.
Patients with renal failure do well with transplantation.
■ GLOMERULAR-VASCULAR SYNDROMES
A variety of diseases result in classic vascular injury to the glomerular
capillaries. Most of these processes also damage blood vessels elsewhere in the body. The group of diseases discussed here lead to vasculitis, renal endothelial injury, thrombosis, ischemia, and/or lipid-based
occlusions.
ATHEROSCLEROTIC NEPHROPATHY
Aging in the developed world is commonly associated with the occlusion of coronary and systemic blood vessels. The reasons for this
include obesity, insulin resistance, smoking, hypertension, and diets
rich in lipids that deposit in the arterial and arteriolar circulation, producing local inflammation and fibrosis of small blood vessels. When
the renal arterial circulation is involved, the glomerular microcirculation is damaged, leading to chronic nephrosclerosis. Patients with GFRs
<60 mL/min have more cardiovascular events and hospitalizations than
those with higher filtration rates. Several aggressive lipid disorders can
accelerate this process, but most of the time, atherosclerotic progression to chronic nephrosclerosis is associated with poorly controlled
hypertension. Approximately 10% of glomeruli are normally sclerotic
by age 40, rising to 20% by age 60 and 30% by age 80. Serum lipid
profiles in humans are greatly affected by apolipoprotein E polymorphisms; the E4 allele is accompanied by increases in serum cholesterol
and is more closely associated with atherogenic profiles in patients with
renal failure. Mutations in E2 alleles, particularly in Japanese patients,
produce a specific renal abnormality called lipoprotein glomerulopathy
associated with glomerular lipoprotein thrombi and capillary dilation.
■ HYPERTENSIVE NEPHROSCLEROSIS
Systemic hypertension causes permanent damage to the kidneys in
~6% of patients with elevated blood pressure. As many as 27% of
patients with end-stage kidney disease have hypertension as a primary cause, and it is the second most common cause of ESRD after
diabetic nephropathy. Hypertensive nephrosclerosis is fivefold more
frequent in African Americans than whites. Risk alleles associated
with APOL1, a functional gene for apolipoprotein L1 expressed in
podocytes, substantially explain the increased burden of ESRD among
African Americans. Associated risk factors for progression to end-stage
kidney disease include increased age, male gender, race, smoking,
hypercholesterolemia, duration of hypertension, low birth weight, and
preexisting renal injury. Kidney biopsies in patients with hypertension,
microhematuria, and moderate proteinuria demonstrate arteriolosclerosis, chronic nephrosclerosis, and interstitial fibrosis in the absence of
immune deposits (see Fig. A4-21). Based on a careful history, physical
examination, urinalysis, and some serologic testing, the diagnosis of
chronic nephrosclerosis is usually inferred without a biopsy. Recent
studies suggest, in the absence of diabetes, adults with hypertension
and cardiovascular risk factors benefit from achieving a systolic blood
pressure <120 mmHg, compared to <140 mmHg. In the presence of
kidney disease, most patients begin antihypertensive therapy with two
drugs, classically a thiazide diuretic and an ACE inhibitor; most will
require three drugs. There is strong evidence in African Americans
with hypertensive nephrosclerosis that therapy initiated with an ACE
inhibitor can slow the rate of decline in renal function independent of
effects on systemic blood pressure. Malignant acceleration of hypertension complicates the course of chronic nephrosclerosis, particularly in
the setting of scleroderma or cocaine use (see Fig. A4-24). The hemodynamic stress of malignant hypertension leads to fibrinoid necrosis of
2348 PART 9 Disorders of the Kidney and Urinary Tract
small blood vessels, thrombotic microangiography, a nephritic urinalysis, and acute renal failure. In the setting of renal failure, chest pain,
or papilledema, the condition is treated as a hypertensive emergency.
■ CHOLESTEROL EMBOLI
Aging patients with clinical complications from atherosclerosis sometimes shower cholesterol crystals into the circulation, either spontaneously or, more commonly, following an endovascular procedure with
manipulation of the aorta or with use of systemic anticoagulation.
Spontaneous emboli may shower acutely or shower subacutely and
somewhat more silently. Irregular emboli trapped in the microcirculation produce ischemic damage that induces an inflammatory reaction.
Depending on the location of the atherosclerotic plaques releasing
these cholesterol fragments, one may see cerebral transient ischemic
attacks; livedo reticularis in the lower extremities; Hollenhorst plaques
in the retina with visual field cuts; necrosis of the toes; and acute glomerular capillary injury leading to FSGS sometimes associated with
hematuria, mild proteinuria, and loss of renal function, which typically
progresses over a few years. Occasional patients have fever, eosinophilia, or eosinophiluria. A skin biopsy of an involved area may be
diagnostic. Since tissue fixation dissolves the cholesterol, one typically
sees only residual, biconvex clefts in involved vessels (see Fig. A4-22).
There is no therapy to reverse embolic occlusions, and steroids do not
help. Controlling blood pressure and lipids and cessation of smoking
are usually recommended for prevention.
■ SICKLE CELL DISEASE
Although individuals with SA-hemoglobin are usually asymptomatic,
most will gradually develop hyposthenuria due to subclinical infarction
of the renal medulla, thus predisposing them to volume depletion.
There is an unexpectedly high prevalence of sickle trait among dialysis patients who are African American. Patients with homozygous
SS-sickle cell disease and less commonly SC-sickle cell disease develop
chronic vaso-occlusive disease in many organs. Polymers of deoxygenated SS-hemoglobin distort the shape of red blood cells. These
cells attach to endothelia and obstruct small blood vessels, producing
frequent and painful sickle cell crises over time. Early changes in the
kidney include glomerular hyperfiltration, hyposthenuria, micro- or
macroscopic hematuria, and microalbuminuria. Later changes can
include papillary necrosis, renal infarction and proteinuria, and most
commonly, FSGS on renal biopsy and rarely MPGN. Vessel occlusions
in the kidney produce glomerular hypertension, FSGS, interstitial
nephritis, and renal infarction associated with hyposthenuria, microscopic hematuria, and even gross hematuria; some patients also present
with MPGN. Renal function can be overestimated due to the increased
tubular secretion of creatinine seen in many patients with SS-sickle cell.
By the second or third decade of life, persistent vaso-occlusive disease
in the kidney leads to varying degrees of renal failure. Their prognosis
on dialysis is poor, and anemia management with erythropoiesisstimulating agents is complicated. Treatment is directed to reducing
the frequency of painful crises and administering ACE inhibitors and
hydroxyurea in the hope of delaying a progressive decline in renal
function. In sickle cell patients undergoing renal transplantation, renal
graft survival is comparable to African Americans in the general transplant population.
■ THROMBOTIC MICROANGIOPATHIES
Thrombotic thrombocytopenic purpura (TTP), Shiga toxin–mediated
hemolytic-uremic syndrome (HUS), and complement-mediated HUS
represent a spectrum of thrombotic microangiopathies (TMAs). TTP
and HUS share the general features of idiopathic thrombocytopenic
purpura, hemolytic anemia, fever, renal failure, and neurologic disturbances. Clinically, when patients, particularly children, have evidence
of renal injury, HUS is suspected, and in adults with neurologic disease,
TTP is suspected. On examination of kidney tissue, there is evidence
of glomerular capillary endotheliosis associated with platelet thrombi,
damage to the capillary wall, and formation of fibrin material in and
around glomeruli (see Fig. A4-23). These tissue findings are similar
to what is seen in preeclampsia/HELLP (hemolysis, elevated liver
enzymes, and low platelet count syndrome), malignant hypertension,
and the antiphospholipid syndrome. TMA is also seen postpartum
(and may be complement mediated); with the use of oral contraceptives or quinine; in renal transplant patients given OKT3 for rejection; in patients taking the calcineurin inhibitors cyclosporine and
tacrolimus; in patients taking the antiplatelet agents ticlopidine and
clopidogrel; and following HIV infection. The implicated drug should
be discontinued.
Shiga toxin–mediated HUS is caused by a toxin released by Escherichia coli 0157:H7 and occasionally by Shigella dysenteriae. This Shiga
toxin (verotoxin) directly injures endothelia, enterocytes, and renal
cells, causing apoptosis, platelet clumping, and intravascular hemolysis
by binding to the glycolipid receptors (Gb3). These receptors are more
abundant along endothelia in children compared to adults. Shiga toxin
also inhibits the endothelial production of ADAMTS13. In familial
cases of adult TTP, there is a genetic deficiency of the ADAMTS13
metalloprotease that cleaves large multimers of von Willebrand’s
factor. Absent ADAMTS13, these large multimers cause platelet
clumping and intravascular hemolysis. An antibody to ADAMTS13
is found in many sporadic cases of adult TTP. Patients can be tested
for ADAMTS13 activity, and if low, the presence of antibodies to
ADAMTS13 distinguishes the deficiency from the immune-mediated
disease. Complement-mediated TMA/HUS is a rare hereditary deficiency of one of the regulatory proteins that restrict the activation
of the alternate complement pathway and can present in children or
adults often preceded by an infection. The treatment of adult TTP with
ADAMTS13 antibodies is daily plasmapheresis, which can be lifesaving. Plasmapheresis with fresh frozen plasma is given until the platelet
count rises, but in relapsing patients, it normally is continued well after
the platelet count improves. There is an anecdotal role in relapsing
patients for using splenectomy, steroids, immunosuppressive drugs,
bortezomib, or rituximab. Patients without antibodies and a genetic
deficiency of ADAMTS13 production can be treated with fresh frozen
plasma alone. Patients with Shiga toxin–mediated HUS are not given
antibiotics and are treated with supportive care because antibiotics are
thought to accelerate the release of the toxin and the diarrhea is usually self-limited. Patients with complement-mediated TMA/HUS are
treated with eculizumab, an anticomplement therapy.
■ ANTIPHOSPHOLIPID ANTIBODY SYNDROME
(SEE CHAP. 357)
GLOBAL CONSIDERATIONS
■ INFECTIOUS DISEASE–ASSOCIATED SYNDROMES
A number of infectious diseases will injure the glomerular capillaries
as part of a systemic reaction producing an immune response or from
direct infection of renal tissue. Evidence of this immune response is
collected by glomeruli in the form of immune deposits that damage
the kidney, producing moderate proteinuria and hematuria. A high
prevalence of many of these infectious diseases in developing countries
results in infection-associated renal disease being the most common
cause of glomerulonephritis in many parts of the world.
Poststreptococcal Glomerulonephritis This form of glomerulonephritis is one of the classic complications of streptococcal infection. The discussion of this disease can be found earlier, in the section
“Acute Nephritic Syndromes.”
Subacute Bacterial Endocarditis Renal injury from persistent
bacteremia absent the continued presence of a foreign body, regardless
of cause, is treated presumptively as if the patient has endocarditis. The
discussion of this disease can be found earlier, in the section “Acute
Nephritic Syndromes.”
Human Immunodeficiency Virus Renal disease is an important complication of HIV disease. The risk of development of ESRD
is much higher in HIV-infected African Americans than in HIVinfected whites. About 50% of HIV-infected patients with kidney disease have HIV-associated nephropathy (HIVAN) on biopsy. The lesion
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