L J

+

Rustgi AK.Hereditary gastrointestinal polyposis and nonpolyposissyndromes. NEJM 1994:331:1694-1702.

Sakorafas GH, Blanchard K,Sarr MG. etal.Paget'sdisease of the breast.Cancer Treatment Reviews 2001;27:9-18.

Sailin en V. Akl EA.You JJ. et al.Meta -analysis of antibiotics versus appendicectomy lor non - perforated acute appendicitis.Br J Surg.2016 May:103(6):656-667.

Safieddine N.Liu G.Cuningham K, et al. Prognostic factorsfor cure,recurrence and long-term survival altersurgical resection of thymoma.J Thorac Oncol 2014;9:1018-1022.

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Safwan M,Penny SM.Emphysematous Cholecystitis:A Deadly Twist to a Common Disease.JDiagn Med Sonogr 2016:32(3):131-137.

Sandlin L,Sandroussi C.Guba M. elal.Living donorliver transplantation vs.deceased donor liver transplantation for hepatocellular carcinoma:comparable survival and recurrence.Liver Transplant 2012:18:315-

322

Sauerland S,JaschinskiI.Neugebauer EA.Laparoscopicvs.open surgery for suspected appendicitis.Cochrane DB Syst Rev 2010:10:CD001546.

Shabanradeh DM.Sorensen LI. Jorgensen T.A prediction rule for risk stratification ofincidentally discovered gallstones:results froma large cohort study.Gastroenterology 2016:150:156.

Sbcth SG,LaMont JT.Toxic megacolon.lancet 1998:351:509-513.

Shojaiefard A,Esmaeilradeh M.Ghafouri A.ctal.Various techniques for the surgicaltreatment olcommon bile duct stones:A meta review.Gaslroenterol Res Pract 2009:840208.

Short MW.layton MC.leer BN,cl al.Colorectal cancer screening and surveillance. Am fam Physician. 2015:91|2):93-100.

Sigalet 0L. Short bowel syndrome ininfants and children:an overview.Semin Pcdiatr Sutg. 2001May;10(2):49 55.

Simeone DM.Hassan A,Scheiman JM.Giant peptic ulcer:asurgical or medical disease? Surgery 1999:126:4 /4 478.

Silari R,Skierucha M,Mielko J,el al.Gastric cancer:epidemiology,prevention,classification,and treatment. Cancer Manag Res 2018;10:239-248.

Soares KC.et al.Choledochal cysts:presentation,clinical differentiation,and management J Am CollSurg 2014:219:1167-1180.

Soreide K.ThorsenK.Soreide JA.Strategies toimprove the outcome of emergency surgery for perforated peptic ulcer.8r J Surg.2014 Jan;101|1):e51-64.

Styblo TM,Wood WC.The management of ductal andlobular breast cancer.Surg Oncol1999:8:67-75.

The CanadianTask Force onPreventive Health Care.Recommendations on screening for breast cancer inaverage-risk women aged 40-74 years.CMAJ 2011:183:1991-2001.

Tsai CJ.leiUmann ME.Willett WC. et al. The effect of long-term intake of cis unsalurated fats on the risk for gallstone disease in men:a prospective cohort study.Ann Intern Med.2004;141|7|:514.

Tsai JF.Chuang LY. Jeng JE,et al.Betel quid chevring as a risk factor for hepatocellular carcinoma:a case-control study.Br J Cancer.2001;84(5):709.

Tseng JF. Tamm EP.Lee JE,et al.Venous resectionin pancreatic cancer surgery.Best Pract RcsClinGaslroenterol 2006:20:349-364.

Van Agtercn JE.Carson KV. Tiong IU. cl al.lung volume reduction surgery lor diffuse emphysema.Cochrane Database Syst Rev 2016:10:CD001001.

Van Beers BE.Diagnosis of cholanglocarcinoma. HP8 (Oxford) 2008;10:87-93.

Hagen P. Hulshof MC.van lanschol JJ.el al.Preoperative chcmoradiotheiupy for esophageal or junctional cancer. NEJM 2012 May 31:366|22):2074- 2084.

Vasei N.Shishegar A.Ghalkham F,clal.Fat necrosis in the Breast:A systematic review ol clinical trials. LipidsHealth Ois 2019:18:139.

Verlcden GM,Raghu G.Meyer KC.et al.Anew classification system for chronic lung allograft dyslunction.J Heart lung Transplant 2014:33:127-133.

Wadsworth CA.Oixon PH.Wong JH,et al.Genetic factors in the pathogenesis of cholangiocatcinoma.Dig Dis 2011:29:93-97.

Waki K.UN0S Liver Registry:ten yearsurvivals.Clin Transplant 2006:29-39.

Way LW.Current surgical diagnosis and treatment.11lhed.2003.

Weill 0.Lung Transplantation:indications and contraindications.J Thorac Dis 2018:10:4574-4587.

WilkinsT.Wheeler B.Carpenter M. Upper Gastrointestinal Bleeding in Adults:Evaluation and Management.Am Fam Physician.2020 Mar1;101(5):294-300.

Willems SM. van Deurien CH. van Oiesl PJ.Diagnosis of breast lesions:fine-needle aspiration cytology or core needle biopsy? A review.J Clin Pathol 2012:65:287-292.

William BM.Corana GR.Hyposplenism:a comprehensive review.Part I:basic concepts andcauses. Hematology. 2007Feb;12(1):1-13.

Wilms IM. de Hoog DE.dc Vasei DC. et al. Appendectomy vs.antibiotic treatment for acule appendicitis Cochrane Oatabasc Syst Rev 2011;|11):CD008359.

WinstonI. Livingston R. Johnson D. et al. Vinorclbmo plus Cisplatin vs. Observation inResected Non-Sinall-Cell lung Cancer.NEJM 2005:352:2589 2597.

World Health Organitation. Cancer.Sept 28.Available from:hllps;//www.who.inl/news- room/lact-sheels/detail/cancer.

Yadav 0.Agarwal N.Pitchumonl CS. A critical evaluation of laboratory tests in acute pancreatitis. Am JGaslroenterol 2002:97:1309-1318.

YamamotoI.WalanabeI.Surgery lor luminal Crohn's disease.World J Gaslroenterol.2014 Jan ?:20|1|:78-90.

Yang XY.Chen CX.Zhang BL.et al.Diagnostic effect of capsule endoscopy in 31cases of subacute small bowel obstruction.WorldJGastroenterol.2009 May 21:15|19):2401-5.

Yeo HL,Lee SW.Colorectal emergencies:review andconlroversies in the management of large bowel obstruction.J Gastrointest Surg.2013 Nov;17(11):2007-12.

Zhang H.YangI.Wu M.et al.Intrahepatic cholangiocarcinoma:Epidemiology,risk factors,diagnosis and surgical management.Cancer Lett 2016;379:198-205.

Zittel TT,Jehle EC.Becker HD.Surgical management of peptic ulcer disease today - indication,technique and outcome.Langenbecks Archives of Surgery 2000:385:84-96.

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Geriatric Medicine

lmaan Zcra Khcrani aiul Saba Manzoor, chapter editors

Karolina Gacbe and Alyssa Li, associate editors

Wei hang Dai and Camilla Giovino, E8M editors

Dr. Jillian Alston, Dr. Vicky Chau, and Dr.Thiru Yogaparan,stall'

editors

Acronyms

Physiology and Pathology of Aging

Framework for the Approach to the Older Adult

Presentations in Older Adults

Constipation

Delirium

Elder Abuse

Falls

Frailty

Immobility

Incontinence

Malnutrition

Presbycusis

Presbyopia

Pressure Injuries

Driving Competency

Reporting Requirements

Conditions That May Impair Driving

Hazards of Hospitalization

Healthcare Institutions

Geriatric Pharmacology.

Pharmacokinetics

Pharmacodynamics

Polypharmacy

Inappropriate Prescribing inOlder Adults

Common Medications

Landmark Geriatric Medicine Trials

References

GM2

GM2

GM3

GM4

GM13

GM14

GM15

GM15

GM17

GM18

GM19

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GMl Geriatric Medicine Toronto Notes 2023

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Acronyms

ACEl angiotensin converting enzyme ESAS

inhibitor

activities of daily living

adverse drug reaction

benign prostatic hypertrophy GCA

blood urea nitrogen

cognitive behavioural therapy GFR

comprehensive geriatric

assessment

chronic kidney disease

central nervous system

cardiac output

creatinine clearance

Edmonton Symptom Assessment MMSE Mini Mental Status Examination PPS

MS multiple sclerosis

musculoskeletal

NE norepinephrine

Palliative Performance Scale

per rectal

parathyroid hormone

personal support worker

peptic ulcer disease

peripheral vascular disease

rheumatoid arthritis

serotonin-norepinephrine

reuptake inhibitor

selective serotonin reuptake

inhibitor

transient ischemic attack

tricyclic antidepressant

urinary incontinence

Scale PR

ADL ESR erythrocyte sedimentation rate MSK

gamma-aminobutryic acid

giant cell arteritis

PTH

ADR GABA PSW

BPH NP nurse practitioner

gastroesophageal reflux disease NPIAP National Pressure Injury

Advisory Panel

NSTEMI non SI elevation myocardial

infarction

PUD

BUN GtIJU PVD

CBT glomerular filtration rate

instrumental activities of daily

living

inflammatory bowel disease NYD

irritable bov/el syndrome

international normalized ratio PCI

RA

CGA IAUL SNRI

CKD IBD not yet diagnosed SSRI

over the counter

percutaneous coronary

intervention

power of attorney

CNS IBS OTC

CO INR TIA

CrCI LOC level of consciousness

left ventricle

TCA

LV POA Ul

Physiology and Pathology of Aging

Holistic Considerations for Aging

• aging is a loss of homeostasis relating to a breakdown in maintenance of specific molecular and

cellular structures and pathways

• some of these changes are specific to the tissues of certain organs, whereas others occur over a number

of organ systems

• normal age-related changes represent biologic processes common to everyone asthey age; however,

the rate and extent is extremely heterogeneous; thus, for the same chronological age, individuals may

present with a different biological age or frailty level

• major categories of impairment develop with old age and affect the physical, mental, and social

domains of older adults, usually due to many predisposing and precipitating factors rather than a

single cause

The table below outlines the physiological changes that occur with aging and their organ specific

impacts. In addition, it outlines pathological conditions occurring in greater frequency in older adults.

Physiological changes may predispose older adults to pathological conditions; however, unlike normal

changes of aging, not all older adults will develop pathological changes associated with aging

Functional Assessment

(ADLs and lADLs)

ADls: ABODE TT lADls:SHAFT TT

Ambulating

Bathing

Continence

Shopping

H ousework

Accounting.'Managing

finances

Foodpiepaiation

Tianspwtation

Telephone

Taking medications

Diessmg

Eating

Tansfenmg

Toileting

Can use lorrn.ilassessment took such as

the Lavrton-Brody Instrumental Activities ot

Daily Living Scale to assess functioning

Table 1. A Systems-Based Analysis of Potential Changes That Can Occur with Aging

System Physiological Changes Impact of Physiologic Changes Pathological Changes

Occurring Frequently with

Older Adults

Comprehensive Geriatric Assessment foi Older

Adults Admitted toHospital

Cochrane OB Syst Rev 2017;CD0062t1

Purpose fo deteimire whether CGA uo improve cue

provided toolder adults admittedlo hospital.

Results Conclusions Inpatient CGA increases

kkefihood that patientswill be alive in then own

homes at 3-12 mo follow-up frisk ratio (KB)1.06.95%

Cl1.01-1.10|.decreases the likelihood that patients

willbe admitted to a nursing home at 3-12 mo (BB

0.80.95% Cl 0.72-0.89),and resultsisktlle oino

difference in dependence (BB 0.97.95% Cl0.89101),

Evidence lor cost reflectiveness of performing a CGA in

older adults admitted to hospitalIs inconclusive due

to imprecision and inconsistency among studies.

Neurologic Mild Impact on woiking memory and

processing speed

Deduced sleep lime

Reduced fine-motor control

Reducedreflex response

Eyes:thickened lenses,reduced pupil Eyes:reduced visual acuity,dark

diameter.Increased lipidinfillrates, adaptation

decreased lacrimal gland secretion ENI:teduced sense of smell and lasle.

ENT:reduced saliva,atrophied hair

cells,reduced cochlear and inner

ear neurons,reduced ossicular

articulation

Increased left ventricular thickness

and stiffness

Increased vascular resistance

Reduced pacemaker cells

Decreased barorcllex and autonomic

reflexes

Decreased vessel elasticity,

cardiac myocyte size and number,

8-adrenergic responsiveness

Increased tracheal cartilage

calcification,mucous gland

hypertrophy

Decreased elastic recoil,increased

residual volume,reduced vital

capacity,forced expiratory volume

Reduced chest wall compliance

Increased Intestinal villous atrophy

Decreased esophageal peristalsis,

gastric acid secretion, liver mass,

hepatic blood flow,calcium, and iron

absorption

Decreased brain mass and cerebral

blood flow

Increased white mailer changes

Reduced number of neuions

Reduced action potential speed

Increased insomnia,

neurodegcneiative disease (e.g.

Vascular dementia.Alzheimer's

disease),stroke

Increased glaucoma,cataracts,

macular degeneration,presbycusis,

presbyopia, tinnitus, vertigo, oral

dryness

Senses

reduced detection olhigher frequency

sounds, reduced vestibular function

Cardiovascular Increased sBP,decreased dBP.HR,CO,

wide pulse pressure

Heart and blood vessels less responsive

to physiological stress

Increased atherosclerosis.CAD. Ml,

CHT.HTN,arrhythmias,orthostatic

hypotension

Comprehensive Geriatric Assessment loi

Community-Dwelling,High-Risk.And frail Older

People

Cochrane D8 Syst Rev 2022:000012705

Purpose: Appraisal of the effectiveness olusing

the CGA for community-dwelling,high-risk, and frail

older adults.

Results Conclusions CGA resultednnodiflerenre

m mortality duringmedian follow -upat 12 months

(BB 0.88 95% Cl 0.76-1.02),and concurrently no

difference innursing home admission|RB 0.93,

95% Cl 0.76to1.14|.CGA may decrease therisk of

unplanned hospital admission overUmonths of

Mow-up (Rfi 0.83 95% Cl 0.70 to 0.99).

Increased COPD.pneumonia,

pulmonary embolism

Respiratory Decreased arterial partial pressure ol

oxygen,decreased exercise tolerance,

decreased pulmonary reserve

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Gastrointestinal Reduced Bl2, calcium andiron absorption Increased dysphagia,cancer.

diverticulitis,constipation, fecal

incontinence,hemorrhoids,intestinal

obstruction,malnutrition,weigh!loss +

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Table 1. A Systems-Based Analysis of Potential Changes That Can Occur with Aging

System Physiological Changes Impact of Physiologic Changes Pathological Changes

Occurring Frequently with

Older Adults

Renal and Urologic Decreased renal mass and number of Decreased cGFR and concentration ability Increased urinary incontinence

renal tubules andglomcruli, reduced ol kidney

renal blood flow

and urgency, nocturia , BPH.

proslate cancel, pyelonephritis,

nephrolithiasis. Utl. testicular atrophy,

proslate enlargement

Increased urine pH

Reduce nerve density and diminished Reduced hydroiylation ol vitamin D

detrusor function in bladder Proteinuria

Reduced diurnal anlidiurelic hormone Urinary frequency and urgency

Hocturia

Reproductive Decreased androgen,estrogen,

sperm count,vaginal secretion

Decreased ovary, uterus, vagina, and

breast sire

Increased Nt. PIN. insulin,

vasopressin

Decreased thyroid and adrenal

corticosteroid secretion

Increased breast and endometrial

cancer, cystocele, rectocele.atrophic

vaginitis

Endocrine Impaired stress response Increased DM. hypothyroidism

MSK Increased calcium lossfrom bone Decreased strength (note:reduced motor Increased arthritis, bursitis.

Decreased muscle massisaicopenia, strength on neurological examination is osteoporosis,muscle weakness with

cartilage,synovial fluid lubrication not expected) gait abnormalities, polymyalgia

Jointstiffness and reduced joint capsule rheumatica

flexibility

Atrophy of sebaceous and sweat

glands

Decreased epidermal and dermal

thickness, dermal vascularity,

melanocytes, collagen synthesis,

elaslin synthesis

Increased skin laxity,wrinkles, and

skin stiffness

Integumentary Increased skin laxity,wrinkles, and skin Increased lentigo, cherry

stiffness, and easy bruising hemangiomas, pruritus,seborrheic

keratosis, herpes roster, decubitus

ulcers,skin cancer, easy bruising,

onychomycosis.senile purpura.

xerosis cutis

Decreased antigen-antibody affinity, Reduced response to new pathogens. Increased susceptibility to

decreased efficacy of neutrophils and reduced response to immunizations and malignancies, infections, and

macrophages,decreased numbers need for boosters autoimmune conditions

of B and T cells (excluding memory B Blunted fever response and atypical

presentation of infections which may

lead to delayed care

Immunologic

and memory I cells)

Psychiatric Decreased processing speed,

cognitive flexibility.visuospalial

perception , working memory.and

divided attention

loss of synaptic plasticity

Increased depression,dementia,

delirium,suicidahty, anxiety,sleep

disruption

Framework for the Approach to the Older Adult

History: A Brief Geriatric Screen Using “The 5 M’s Framework”

• mind: consider mentation, dementia, delirium, and depression

• consider more validated screening when concerns are raised from family members

• consider asking if patients suffer from chronic pain

• mobility: observe for impaired gait and balance and consider fall injury prevention strategies

consider evidenced-based ways to reduce injuries: exercise, vision evaluation and treatment,

home safety assessment, occupational therapy support, calcium and vitamin D supplementation

• medications: monitor for polypharmacy, consider de-prescribing where possible, check adherence,

check medication understanding from patient perspective, be cautious of adverse medication effects

• multimorbidity: use a bio-psycho-social approach to assess a patient’

s comorbidities

• matters most: explore values and priorities (maintaining independence, preventing adverse events,

optimizing comfort, prioritizing prolonged life)

Focused Geriatric Physical Exam

• general and vital signs: weight (signs of cachexia, unintentional weight loss), height (reduction may

indicate vertebral compression fractures or osteoporosis), blood pressure, and orthostatic vitals

• head and neck: test visual acuity, in-office hearing screen (whisper test), dentition, denture fit,

lymphadenopathv, and neck masses

• cardiac: auscultate for arrhythmias, murmurs, extra heart sounds

• respiratory: auscultate, observe for SOB

• peripheral vascular exam: assess for arterial or venous insufficiency, inspect for edema and ulcers,

palpate for diminished peripheral pulses

• dermatologic: look for premalignant/malignant lesions especially on sun-exposed areas, examine for

pressure sores in patients with diabetes, especially those who are immobile, examine for unexplained

bruises or signs of elder abuse

• MSK:determine range of motion of all joints, based on history and focused joint exam for arthritic

features

• gait: check footwear and fit of gait aids, assess gait, Romberg for balance, and 30 ssit-to-stand test

• neurologic: examine cranial nerves, examine tone, reflexes, sensation, upper motor signs, and power

in upper and lower extremities

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Presentations in Older Adults

Constipation

•see Gastroenterology, G27

Definition

•Rome IV Diagnostic Criteria (£2 must be present in 1/4 of bowel movements for S3 mo with

symptom onset 6 mo prior):

straining

« hard stools

sensation of incomplete evacuation

use of manual maneuvers to facilitate defecation

sensation of anorectal obstruction/blockage

<3 bowel movements per wk

• patients must meet both of the following criteria:

loose stool rarely present without the use of laxatives

does not meet Rome IV criteria for IBS

Epidemiology

•chronic constipation increases with age (up to 1/3of patients >65 yr experience constipation and 1/2

of patients >80 yr)

•in the elderly, chronic constipation may present as fecal impaction and overflow diarrhea

Etiology

•neurological:dementia

•metabolic: hypercalcemia, hypothyroidism, hypokalemia

•nutritional:low dietary fibre, dehydration

•drugs association with constipation:

• OiC

opioids

psychotropics (e.g.antipsychotics,TCAs)

anticholinergics (e.g.dimenhydrinate, diphenhydramine,TCAs, antimuscarinicsfor urinary

incontinence)

calcium channel blockers

diuretics

supplements(e.g. iron, calcium)

Pathophysiology

•impaired rectal sensation (increased rectal distention required to stimulate the urge to defecate)

•colorectal dysmotility

Alarm Symptoms

•fever

•blood in stool

•severe nausea/vomiting,severe abdominal pain

•abdominal/rectal mass

•unintentional weight loss

•obstipation

•new changes in bowel habits when age >50 yr

•unexplained anemia or iron deficiency on blood work

Treatment

•non-pharmacological

bowel training

» increase fibre intake (note:bulking agents, e.g. psyllium,Metamucil*, may worsen constipation in

some)

• ensure adequate fluid intake

• increase physical activity

•pharmacological

• see figure I

• discourage chronic laxative use

review medication regime, reduce dosages orsubstitute

•see Common Medications,GM17

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Chronic Constipation j

A Double-Blind. Placebo-Controlled Study of

Prucaloprido inildorlyPatientswithChronic

Constipation

Neurogastioenteiol Hotil 2010:22(91991 98

Purpose:loassess the efficacy, safety,and

tolerability of prucalopride in chronically constipated

elder ty patients.

lesults/Conclusions Ireprucalopnde dose range

tested(1-4 mg duly)is effective at promoting bowel

movements,nunmiiiingconstipation- associated

symptoms,and nptonng quality of life.It Is safe

and well-tolerated in elderly patients wtb chronic

constipation.

NO { Fecal Impaction YES

4

Remove constipating medications (if possible)

Increase fluid intake

Increase activity or exercise

Increase fibre intake (20-30 gfd)

Start Urned toilet training

Perform manual disimpaction

Use enemas and/or suppositories

Start bowel regimen to prevent

recurrence

4

Milk of magnesia

Lactulose

Peg-Lyte

Senna compounds

Bisacodyl

YES Effective NO theEffect of Probiotics as a Treatment for

Constipation in the Elderly:ASystematic Review

Arch GerontolGeriatr 2017:71:142 49

Purpose:Evaluate the effectiveness of probiotxs

m treating elderly constipation,as an alternative to

traditional dug based tieatments.

Results Conclusions Analysis of placebo controlled

RCIs suggested that administration ol probiotics

significantly impioved constipation in the elderly

by 10 AO1icompared toplacebo,further trialsare

requited to elucidate optimalprotocols of probiotic

treatment regimens.

i i

Continue regimen polyethylene glycol (PEG3350 high dose)

j

YES Effective NO

4

^

Continue regimen j

n

’

I

Lubiprotone Biofeedback therapy

Idyssynergic defecation)

Alvimopan

Methylnaltrexone

opioid-induced constipahon)

Figure 1.Treatment algorithm for the management of chronic constipation in older adults

Adapted from:ClinInterv Aging 2010:5:163-171

Delirium

•see Psychiatry. PS23 and Neurology. N21

Definition

•acute and potentially reversible disturbance in cognition, attention, or level of consciousness

Epidemiology

•delirium is especially common among patients in the 1CU setting, postsurgical setting, and general

medicalsetting

• up to 25% of patients after elective surgery

50% of patients after high-risk procedures(e.g. cardiac surgery, hip-fracture repair)

up to 75% of mechanically ventilated patients in the 1CU

•can affect all ages but is especially common in hospitalized older adults

one-third of general medical patients >70 yr have delirium

Screening/Diagnostic Tools

•screened using the Confusion Assessment Method: delirium likely if 1 + 2 and either 3 or 4 are present

1. acute onset and fluctuating course

2. inattention

3. disorganized thinking

4. altered level of consciousness

•classified as: hyperactive,hvpoactive, or mixed

Differential Diagnosis

•3Ds (dementia, delirium, depression) can present with overlapping cognitive changes

An Approach to Delirium: “DIMS-R”

•D: drugs (consider prescribed,over the counter, overdose, intoxication, and withdrawal)

•I:infection (consider urinary tract, lungs, skin, bacteremia)

•M: metabolic disturbances (consider fluid imbalances, electrolyte abnormalities, nutritional

deficiencies)

•S: structural insults (cardiovascular, CNS,pulmonary, Gl)

•R: retention (urinary retention,constipation)

Work-Up

•work-up is not universal and depends on possible causes based on history and physical exam:

drugs, toxins, withdrawal: medication review, substance use history

• infection, infarction,inflammation: CBC, urinalysis,urine culture,blood culture,CXR,EGG,

troponin, creatinine kinase

Delirium inOlder Persons:Advances inDiagnosis

and treatment

JAMA 2017:318(12):1161-74

Purpose:To provide overview of current state of

diagnosis andtreatment of delirium andidentify

prom sing areas for future research

Methods:Controlled vocabulary and keyword terms

were seaabedin Ovid MEDLINE Embase and the

Cochrane Library with focus cn studies conductedIn

elderly populations.

Results:127articles met inclusion criteria.High

sensitnrity and specificity brief screening tools and

measures of delirium sererity contribute to ability

foifagnose.Heat risk stratify,and prognosticate

patents.Honphatmacologic approaches are

effective for delirium preventionand retommeeded

for dehriumtreatment. Pharmacologic treatment

(antipsycbotics.other sedatives) for agitation

should only be used if the patient is at safety risk

fo thniselns oiothers or isimpeding medical

treatment oltbe underlying cause.

Condusioa:Better screening and diagnosis

of dehrium leads to bettei nsk stratification.

Nonphamucotogic approaches of delirium prevention

are effect.re.whereas pharmacological management

o!delmum is controversial.

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GM6 Geriatric Medicine Toronto Notes 2023

metabolic: basic and extended electrolytes, vitamin Bt ’, TSH, LI T, toxicology screen, glucose,

arterial blood gas/venous blood gas, creatinine

structural: neurologic exam, CT head Antipsychotics for Treating Delirium in

HospitalizedAdults:A Systematic Review

A nn Intern Med 2019:1)1:435-95

Purpose Eviluilewillicurrent literature the

risks and benefits of antipsyctiotics in delirium

management hosp.tal zed adults.

Study Selection: KIs of antipsychoticvs. placebo

01 another antipsychotic,iswellas prospective

observational studies that report barms, ate selected

through searches on PuSMed.Embase,CENlltAl,

CINAHL. and PsytIHFO from inceptron to July 2019.

the review selected 16 RCtsard 10 observat onal

studies ofhospitalired adults.

Data Synthesis: No significant difference m sedation,

delirium,hospital length-of-stay.or mortality

between haloperidol and second-generation

antipsychotics vs.placebo. No difference Inmodality

m direct comparisonsbetween second-generation

antipsychotics.While shortterm use ofantipsychotics

lor delirium managementdoes not appear to pose

neiiiotogicalhatm, it posesa risk of 01protongalion.

Conclusion. Ire current evidence does not suppoit

the routine use ol haloper dot or second-generation

antipsychotics in delirium management for adult

inpatients.

Delirium Prevention in Older Adults

•ensure optimal vision and hearing to support orientation (e.g. appropriate eyewear and hearing aids)

•frequent reorientation techniques

•family visitation

•maintaining a routine in prolonged hospital stays

•ensure adequate dentition

•adequate pain management

•provide adequate nutrition and hydration (up in chair to eat and drink whenever feasible)

•encourage regular mobilization to build and maintain strength, balance, and endurance

•avoid unnecessary medications and monitor for drug interactions

•avoid bladder catheterization

•ensure adequate sleep at night and wakefulness during the day

Table 2. Differentiating the Three Ds of Cognitive Impairment

Dementia Delirium Depression

Gradual or step-wise decline

Months to years

Progressive, usually irreversible

Aculc (hours todays)

Days to weeks

Fluctuating, reversible

High morbidily/morlalityin

very old

Fluctuating

Impaired,difficulty concentrating

Impaired, fluctuating

Severe agitation/retardation

Subacule (weeks to months)

Variable

Recurrent,usually reversible

Onset

Duration

Natural History

Level of Consciousness Normal Normal

Intact initially

Intact initially

Oisinhibition.loss of ADlitADLs.

personality change

Normal

Fragmented sleep at night

Labile,flattened, apathetic

Chronic,gradually progressive

decline in cognilion

Domains impacted depend on

dementia subtype

Short termmemory impairment

is predominate in Alzheimer's

dementia

Attention

Orientation tldcr Abuse Prevalence inCommunity Settings: A

SystematicReview and Meta-Analysis

lancet Glob Health 2017:5:117-56

Purpose: Snce quantitative syntheses of elder abuse

prevalence are raie. the study aimed to quantity

and understand prevalence variation at global and

regional levels.

Methods: A comprehensive search strategy from

M databases was employed to identity elder abuse

prevalence studies in the community, published from

inception toJune 2015.Subgroupanalysis and metaregression were used to eiptore heterogeneity.

Results: 52 of the 38544 in t ally identified studies

were eligble loiinclusion,all of which were

geographically diverse (28 countries). The pooled

prevalence estimates werelt.6% for psychological

abuse. 6.8% for financial abuse. 4.2% lor neglect.

2.6% lor physical abose. and 0.9% lorseiual abuse.

Significant heterogeneity was found in associations

with overall prevalence estimates, including sample

size, income classification,and method of data

collection,but not with gender.

Conclusion tldei abuse isa neglected pubk health

priority,especially compared with other types of

violence.Elcder abuse seems to affect1in 6older

adults worldwide,a figure totaling 141million people.

Intact

Behaviour Importuning,self-harm/suicide

Slowing

Early morning awakening

Depressed. stable

Impdired concentration

Psychomotor

Sleep-Wake Cycle

Mood and Affect

Cognition

Fluctuates between eitremcs

Reversed sleep-wake cycle

Anxious,irritable,fluctuating

Fluctuation precededby mood

changes

Inattention

May have impaired short- term

memory

Possible impairment in episodic

memory

Memory Loss

Evidence on Management of Delirium:

• see “Antipsychotics for Treating Delirium in Hospitalized Adults: A Systematic Review”

• see “Delirium in Older Persons: Advances in Diagnosis and Treatment"

Elder Abuse

Definition

• includes physical abuse,sexual abuse, emotional/psychological abuse, financial exploitation, and

neglect

• elder abuse is a criminal offence under the Criminal Code of Canada and in most EJ .S. states

Elder Abuse Screening tools: A Systematic Review

J Adult Prot 2017:19:368 )9

C ontext andPurpose: Wrth high rates of morbidity

and mortality,along with deleterbos psychological

harms,elder abuse is often difficult to detect,this

study seeks to review currently available elder abuse

screening tools.

Results:11of 34 full text studiesmet inclusion

criteria and weie included «the final analysis.

01these,three studies reported sensitivity and

specificity while the remainder reported validty and

reliability testing.Ultimately,the dinical environment

will dictate the choice ol screening tool,

limitations Ydiiatior.s n tool qualitiesand

characteristics led to challenges in data synthesis.

A further challenge was the lack of a gold standard

screening tool(or elder abuse,for evaluation of

heterogeneity.

Conclusion Research on screening tools remains

hard-pressed in distinguishing those assessing

suspected or actual elder abuseard those assessing

risk lactorsfor abuse. Allhough screening tools cany

inherent Imitations,they can be used to guide luithei

assessments lor an object,-

*

diagnosis.

Epidemiology

• in Canada in 2019, almost 4518 seniors were victims of police-reported family violence

• the perpetrators of family violence against seniors were identified to be their grown child (34% of

cases) and their spouses ( 26% of the cases)

• in older adults >60 yr, elder abuse is estimated to occur in 10% of patients

• insufficient evidence to include/exclude screening in the Periodic Health Exam

Risk Factors

Table 3. Risk Factors for Elder Abuse

Situational Factors

Victim Characteristics

Social

Physical or emotional dependenceon caregiver

lack of close familylies

History olfamily violence

Dementia or recent deterioration in health

Related to victim

Dependency on older adult (e.g. financial dependency)

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Perpetrator Characteristics

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GM7 Geriatric Medicine Toronto Notes 2023

Screening Tools

• Elder Abuse Suspicion Index© (EASI©): a six-item questionnaire to raise a physicians level of

suspicion for elder abuse and promote referral of possible victimsfor further assessment by social

services

EASI

For each of the 6 Items below,indicate

“yes.

"“no.

" or “did not answer.

" A response

of “yes"on1+ of questions 2-6 is concerning

for elder abuse

010.S asked of patient;0.6 answered by

doctor (Within the last 12 months)

Management

• assess patient’s decision-making capacity regarding any proposed intervention

• address imminent safety

• consider referral to local resources ( home care, respite agencies,shelters, legal services, police

services,government-supported elder abuse consultants)

• create emergency safety plan

• offer assistance with reporting abuse

• in Ontario, reporting elder abuse is mandatory when an older adult resides in a Long-term Care Home

or a Retirement Home

1Have you relied on people for any of the

following:bathing, dressing,shopping,

banking, or meals?

2 Has anyone prevented you from getting

food, clothes, medication,glasses,

hearing aids or medical care,or from

being with people you wanted to be with?

3 Have you been upset because someone

talked to you in a way that made you feel

shamed or threatened?

4 Has anyone tried to force you to sign

papers or to use your money against your

will?

6 Has anyone made you afraid, touched

you in ways that you did not

you physically?

6 Doctor;Elder abuse may be associated

with findingssuch as:poor eye contact,

withdrawn nature,malnourishment.

hygiene issues, cuts, bruises,

inappropriate clothing,or medication

compliance issues. Did you notice any of

these today or in the last 12 months?

MkHJ.NlunC.URiwick M.eU.fcwkprent and

nMdioo ola tool toassist ptry*

cats'ajenbliuljon ol elder

abuse TieElder torse Suspicion tnta(EIS! ;

|.J Elder Abuse

«ed»O8:2O(3i

:276 3O0.

Mips '«ww.rricgill.tJiTjmlyir«

'

4re»

*

ch,

projettslelder

Falls

Definition

• an event resulting in a person coming to rest inadvertently on a lower level, other than as a

consequence of sudden paralysis, epileptic seizure,or overwhelming external force

Epidemiology

• approximately 20-30% of older adults >65 yr fall each year in Canada, prevalence increases with age

falls resulting in injury (e.g. broken/fractured bones,sprain/strain, concussion) were more likely

to occur in women than men

25% associated with serious and 1/3 of hospitalizations were associated with hip fractures

more than 1/3 of older adults are admitted to long-term care after hospitalization

Etiology

• intrinsic factors

age-related changes and diseases associated with aging: MSK (arthritis, muscle weakness),

sensory (visual, proprioceptive, vestibular), cognitive (depression, dementia, delirium, anxiety),

cardiovascular (CAD,arrhythmia, Ml,low BP), neurologic (stroke, decreased LOC,gait

disturbances/ataxia), and metabolic (glucose, electrolytes)

orthostatic/syncopal

acute illness, exacerbation of chronic illness

• extrinsic factors

environmental (e.g. home layout,slippery surfaces, overcrowding, new environments)

side effects of medications, polypharmacy (>4 medications), and substance misuse (e.g. alcohol

misuse)

• situational factors

activities (e.g. rushing to the toilet, walking while distracted)

want,or hurt

Additional

o

Canadian Resourcesfor

Management of Suspected Elder Abuse

Older A dultsSafety Line:24/7

confidential phone line providing

Information and referralsfor older adults

experiencing abuse

Advocacy Centre for the Elderly

Canadian Network for Prevention of

Elder Abuse

History and Physical Exam

• falls history:pre-fall symptoms (chest pain,syncope, presyncope, palpitations),infectious symptoms,

mechanisms,loss of consciousness, head trauma, neck/cervicalspine trauma, post-fall (how long were

Key Clinical History Findings in Falls

Evaluation

they on the ground, who helped them up, post-fall confusion or amnesia)

• extended history: previous falls and/or gait instability, intrinsic, extrinsic and situational factors,

associated symptoms, medication and alcohol use, change in medications

• have a witness present, if possible, for interview

• physical exam:orthostatic BP,injury screen,cardiac, visual acuity,examination of feet and footwear,

gait assessment, Timed Up-and-Go Test, MSK,neurologic

SPLATT

Symptoms

Previous falls

Location of falls

Activity at the time of fal I

Time of fall

Trauma

Investigations

• CGA to identify potential causes

• investigations should be tailored based on history and physical examination. Ihey might consist of:

CBC, electrolytes, BUN,creatinine,glucose, Ca 2+, TSH, vitamin B12, urinalysis, cardiac enzymes,

ECG,CT head (as directed by history and physical), coagulation profile

• bone densitometry (dual-energy X-ray absorptiometry) for osteoporosis screening in all women and

men >65 yr

Interventions

• interventions depend on the identified intrinsic and extrinsic risk factors.First address any acute

illness that precipitated the fall and treat any injuries or complications

• muscle strengthening, balance retraining (e.g.Tai Chi) with appropriate assistive devices, and group

exercise programs

• hip protectors

• fitted gait aid

• multidisciplinary, multifactorial, health and environmental risk factor assessment, and intervention

programs in the community

Impact of Medication Classes on Falls

Risk in Geriatrics(Odds Ratios)

• Antidepressants (1.68)

• Neuroleptics/antipsychotics(1.59)

• Benzodiazepines(1.57)

• Sedatives/hypnotics(1.47)

. Antihypertensive agents(1.24)

. NSAIDs (1.21)

. Diuretics(1.07)

. fl-blockers (1.01)

MeManalpkol the impact <49oaSutrai

clamonMltineWerly persons.IntiMemMed

20O9:l69f2t):t952-1960

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GM8 Geriatric Medicine Toronto Notes 2023

• home hazard assessment and modification with potential for collaboration with occupational therapy

(e.g. remove loose rugs and tripping hazards, add shower bars and stair railing, improve lighting)

• prescription of vitamin D 1000 1U daily if vitamin D stores are low

• optimization of calcium in diet with 1200 mg ofsupplemental calcium advised if osteoporosis is a risk

• tapering or gradual discontinuation of psychotropic medication

• postural hypotension, heart rate, and rhythm abnormalities management

• eyesight (cataract surgery) and footwear optimization

• compression socks if venousstasis edema

Will My Patient Fall ?

JAMA 2007;197:77-86

P urpoic Ip identify the prognostic Hint of mk

farlorslor future falls amoirqolder patients.

Study Selection: Meta anaiysisot prnspectnae cohort

studies of list factors lor falls.

Results It studieswere included. Clin calif

identiliable risk factors were identified across 6

domains:oitliostatic hypotenvon, visual impairment,

impairment of gait or balance,medication

use. limitations in DDLsor UDls.and cognitive

impairment.Ihe estimated pretest probebilitr ol

falling at least once in any g.ven yr lor individuals »

6b

yr was 2J% (95% Cl19-36% ).Patients who have fallen

m the past year are more likely to falI aga n (182.3•

2.8). Best predictors of future falls were dislorbances

n gait or balarce|lR 1.7-2.4).while visual

impairment impaired cognition,and medication were

not reliable predittors.

Conclusions Screening for nsk ot fallingdliragthe

cluneal examination begins with determining if the

patient hasfa lien in the past yr.For patentswho

have not previously fallen,screening consists of an

assessment of g ai t and balance. Patients who have

fallen or who have a gaitor balance problem are at

higher risk of future falls.

Frailty

Definition

• frailty:clinicallv-recognizable state of decreased reserve in older adults with increased vulnerability

to acute stressors resulting from functional decline across multiple physiologic systems

• functional decline: progressive limitation in the ability to carry out basic functional activities

• frailty is associated with higher risk of in-hospital death, adverse events, length of stay, hospital readmission, and newly dependent at discharge following critical illness

Dulhousie University Clinical Frailty Scale

Severe Frailty

Completely dependent on others

for personol cine,from whatever

cause Iphysical or cognitive I.

Even so.they seem stable and

not at high risk of dying (within

-6 mol

1 Very Fit

People who are robust, active,

enorgotlc.and inotnrotod.

They tend to exorclso regularly

and are among the fittest for

their ege.

4 Very Mild Fraility

Previously "vulnerable 'Eoily

transition from complete

Independence. While not dependent

on othersfor dally help,often

symptomslimit activities- A common

complaint is being "

slowed up"

onCkor bump bred during the day

i

Very Severe Frailly

Completely dependent for

personal cato and

approaching tho end of fafo.

Typically,they could not

recover even from a minor

Fit 5 Mild Frailty

A More evidentslowing and need

help with high ordoi lADLs

(finances, transportation, heavy

J

/A housework).Mild frailty

4 PfW^

ssivaly impairsshopping,

walking alone outside, moal prop. illness,

medications and bogins 1o restrict

light housework.

People who have no active

disoaso symptoms, but are lessfit

than category 1. Ofton, they

exercise or are very active

occasionally (e g. seasonally).

Moderate Frailty

Need help with all outsido activities

and housekeeping. Ofton have

problems with stairs,need help

bathing, and might need minimal

assistance with dressing (cuing.

Terminally III

Approaching tho end ol life

Poople w ill a life expectancy ol

<6 mo,who are not otherwise

living with severe frailty.(Many

terminally ill people can still

exorcise until very close to death).

(

Managing Well

Poople whoso medical problems

aie well controlled, ovoti if

occasionally symptomatic, but are

not regularly active beyond

routine walking

Scoring Frailty in People with Dementia

Degree of frailty generally correspondsto degree of dementia

Mild Dementia

Common symptoms include forgetting tho

details of a recent event,though still

remembering the event itself. Repeating the

samo question/story and social withdrawal

Severe Dementia

They cannot do personal caro without holp.

Very Severe Dementia

They are often bedfast Many are

virtually muto.

Moderate Dementia

Rocont memory is vary impair od. even

though they seemingly can remember

past life events well. Can do personal

care with prompting.

Figure 2. Rockwood Clinical Frailty Scale

Adapted from and reprinted with permission:Geriatric Medicine Research,Dalhousie University.Halifax,Canada. :2005-2020 Version 2.0.Allrights

reserved.

MODELS OF FRAILTY

Physical Frailty (PF) Phenotype (Fried et al.)

•Frail: >3 criteria; at-risk or pre-frail = 1 or 2 criteria

1. shrinking: unintentional weight loss (baseline:>10 lbs or 5% total body weight lost in prior

yr)

2. weakness: grip strength in lowest 20% (by gender, BMl)

3. poor endurance:as indicated by self-report of exhaustion

4. slowness:walking time/15 feet in slowest 20% (by gender,height)

5. low activity: keals/wk in lowest 20% (males: <383 keals/wk,females: <270 keals/wk)

Cumulative Deficit Approach (Rockwood et al.)

•balance between assets (e.g. health, attitudes, resources, caregiver) and deficits (e.g. illness, disability,

dependence, caregiver burden) that determines whether a person can maintain independence in the

community

•frailty index: number of deficits present/number of deficits possible

Etiology

•multifactorial:dvsregulated immune, endocrine,stress, and energy response systemslead to

development of clinical frailty

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Drugs/toxins

azathioprine, mercaptopurine, furosemide,estrogens, methyldopa, Ht-blockers, valproic acid,

ABx, acetaminophen,salicylates, methanol,organophosphates,steroids(controversial)

(£)

When thinking about the causes of

acute pancreatitis remember: I GET

SMASHED, but vast majority due to

gallstones or ethanol

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G'I9 Gastroenterology Toronto Notes 2023

Pathophysiology

• activation of proteolytic enzymes within pancreatic cells,starting with trypsin,leading to local and

systemic inflammatory response

• in gallstone pancreatitis,thisis due to mechanical obstruction of the pancreatic duct by stones

• in ethanol-related pancreatitis, pathogenesis is unknown

• in rare genetic diseases, mutations prevent the physiological breakdown of trypsin required normally

to stop proteolysis (e.g. mutant trypsin in hereditary pancreatitis or mutation in SPINK1 gene, which

normally inhibits activated trypsin); may be model for ethanol

-related pancreatitis

Pathology

• mild (interstitial)

peri-pancreatic fat necrosis

interstitial edema

• severe (necrotic)

• extensive peri-pancreatic and intra-pancreatic fat necrosis

parenchymal necrosis and hemorrhage -> infection in 60%

• release of toxic factors into systemic circulation and peritoneal space (causes multi-organ failure)

• severity of clinical features may not always correlate with pathology

• 3 phases

• local inflammation + necrosis -> hypovolemia

• systemic inflammation in multiple organs, especially in lungs, usually after IV fluids given ->

pulmonary edema

local complications >2 wk after presentation -> fluid collection (pseudocyst) or tissue collection

(necrosis),sterile or infected

Cullen

o's Sign

• Sensitive, not specific for acute

pancreatitis

Grey-Turner’sSign

. Flank ecchymosis

Signs and Symptoms

• pain:epigastric, noncolicky, constant

• can radiate to hack

• may improve when leaning forward (Ingleflnger'

ssign) • tetany:transient hypocalcemia

• tender rigid abdomen;guarding

. N/V

• abdominal distention from paralytic ileus

• fever:chemical, not due to infection

Investigations

• increased serum pancreatic enzymes: amylase, lipase (more specific)

• ALT >150 specific for biliary cause

• increased WBC, glucose, low calcium

• imaging:CT most useful for diagnosis and prognosis

• x-ray:

"sentinel loop" (dilated proximal jejunum), calcification, and “colon cut-off sign" (colonic

spasm)

• U/S:useful for evaluating biliary tree (67% sensitivity, 100% specificity)

CT scan with IV contrast:most useful when done >1 d after presentation, helpful for diagnosis

and prognosis because contrastseen only in viable pancreatic tissue, non-viable areas can be

biopsied percutaneously to differentiate sterile from infected necrosis

ERCP or MRCP if cause uncertain, assess for duct stone, pancreatic or ampullary tumour,

pancreas divisum

Classification

• interstitial edematous vs. necrotizing

• mild, moderate, severe

• jaundice: compression or obstruction of bile duct

• Cullen's/Grey-Turner’ssigns Increased Amylase

• Sensitive, not specific for acute

• hypovolemic shock: can lead to renal failure pancreatitis

• acute respiratory distresssyndrome

• coma Increased Lipase

• Highersensitivity and specificity

• Stays elevated longer

Prognosis

• usually a benign,self-limiting course,single or recurrent

• occasionally severe leading to:

• shock

• pulmonary edema

multi-organ dysfunction syndrome

• (il ulceration due to stress

• death

numerousscalesto describe severity: probably most useful is proportion of pancreas not

taking up contrast on CT done 48 h after presentation (necrotic pancreas does not take up the

contrast dye)

presence of organ failure, particularly organ failure that persists >48 h, is associated with

worse outcomes

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Table 25. Collections in Pancreatitis (Revised 2012 Atlanta Classification)

Liquid Solid +

Acute

Chronic

All of these collections ate classified asinlecled ot not infected

Acute petlpancrcalic fluid collection |APfC)

Pancreatic pseudocyst

Acute necrolic collection (ANC)

Walled-off necrosis (WON)

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G50 Gastroenterology Toronto Notes 2023

Treatment

• goals (only supportive therapy available)

1. hemodynamic stability

2. analgesia

3. oxygen

4.stop progression of damage (difficult)

5. treat local and systemic complications

• antibiotic use in infection (cephalosporins, imipenem), not indicated to prevent infection, although

without aspiration/biopsy can be difficult to distinguish infection from non-infected inflammation

• aspirate necrotic areas of pancreasto diagnose infection;drain if infected

• IV fluids (crystalloid or colloid)

beware third spacing of fluid, monitor urine output carefully

• NG suction (lets pancreas rest) if vomiting,stomach very dilated

• endoscopic sphincterotomy ifsevere gallstone pancreatitis (i.e. cholangitis or ongoing obstruction)

• nutritional support: N ) feeding tube or TPN if cannot tolerate enteric feeds

recent evidence supports NG enteral (or oral if feasible) feeds

• no benefit:glucagon, atropine, aprotinin, H’

-blockers, peritoneal lavage

• follow clinically and CT or U/S to exclude complications

• chief role of invasive intervention is to drain fluid collection, excise necrotic tissue (necrosectomy),

especially indicated if pseudocyst or walled-off necrosis is infected,

try to delay for >2 wk to allow demarcation between viable and necrotic tissue, better done

endoscopically or radiologically, rather than surgically if technically possible

Late Complications

• pseudocysts:follow if asymptomatic, drain ifsymptomatic or growing

drain preferably:endoscopic, percutaneous under radiological guidance,surgical if less invasive

methodsfail

• infected necrosis/abscesses: ABx + percutaneous drainage, endoscopic preferable to surgical

• bleeding: (1) gastric varices if splenic vein thrombosis, (2) pseudoaneurysm of vessels in areas of

necrosis, especially splenic artery,(3) duodenal ulcer related to compression of duodenum by enlarged

pancreas

• splenic and portal vein thrombosis: no effective therapy described, anticoagulation not proven,

hazardous

• rare:DM, pancreatic duct damage

Gallstones only cause acute pancreatitis

(not chronic pancreatitis)

Symptoms of Chronic Pancreatitis

• Abdominal pain

• Diabetes

• Steatorrhea

Etiology = Almost Ahways Alcohol

Chronic Pancreatitis Treatment

• EtOH abstinence

• Pancreatic enzyme replacement

• Analgesics

• Pancreatic resection if ductular

blockage

Definition

• irreversible damage to pancreas characterized by

1. pancreatic cell loss (from necrosis)

2. inflammation

3. fibrosis

Etiology/Pathophysiology

• Toxic-metabolic

EtOH (most common)

causes a larger proportion (>90%) of chronic pancreatitisthan acute pancreatitis

changes composition of pancreatic juice (e.g. increase viscosity)

decreases pancreatic secretion of pancreatic stone protein (lithostathine), which normally

solubilizes calcium salts

When toCallthe Surgeon In Acute Pancreatitis?

Endoscopic Transgastric vs. Surgical Necrosectomy ter

Infected Necrotizing Pancreatitis:A Random ired Trial

JAMA 2012:307:1053-1061

Once it was recognized thatsevere acute (necrotizing)

pancreatitis had a terrible prognosis because ol

an enubeiant inflammatory response leading to

multkirgai) failure, pancreatectocny was attempted.

However, contrary to the expected favourable

results, clinical eiperieuce hasshown thatsurgical

pancreatectomy is usually nol helpful, perhaps

because oncethe inflammatory coscadestirts. it

persists as a self-perpetuating cycle.Ihe problems

caused byacute pancreatitis can be thought of

as widespread burn initiated by inDarn matron in

the pancreas, hut haring little to do with ongoing

problems within the pancreasitself.Studiessuggest

that the only compellmg indication torsurgery is

infected necrotizing pancreatitis not responding to

ABi.As predicted,without removal ofsudi infected

pancreatic tissue,death is likely from sepsis.

In this recent randomized trial, transgastric

neaosectomy,an endoscopic lech nigue that also

removes infected necrotic pancreatic tissue,reduced

both a composite endpoint of major pancreatitis

complications(especially new onset organ failure)

and the pro-inflammatory response (as measured by

serum IL-S levels) to a greater extent than surgical

necrosectomy.Of course,not all necrotic collections

are in areasamenable to endoscopic intervention,

andthe advice olan eipeiienccd surgeon should

always he welcomed in severe acute pancreatitis,

hut the role olsurgery in this previously considered

surgical disease is rapidly diminishing.

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- precipitation of calcium within pancreatic duct results in duct and gland destruction

toxic effect on acinar and duct cells - directly or via increasing free radicals

« acinar cell injury leads to cytokine release, which stimulates pancreatic stellate cells to form

collagen (leading to fibrosis)

varying degrees of ductular dilatation,strictures, protein plugs, calcification

no satisfactory theory to explain why only a minority of individuals with EtOH use disorder

develop pancreatitis

• smoking

hypercalcemia

hypertriglyceridemia

• medications

• Idiopathic

• Genetic

• Autoimmune pancreatitis/steroid-responsive pancreatitis (e.g.IgG4-related disease)

• Recurrent acute pancreatitis/severe acute pancreatitis

• Obstructive (e.g. pancreas divisum, ampullary stenosis)

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Signs and Symptoms

• early stages

recurrent attacks of severe abdominal pain (upper abdomen and back)

chronic painless pancreatitis: 10%

• late stages: occurs in 15% of patients

steatorrhea (maldigestion) when >90% of function is lost

diabetes,calcification, jaundice, weight loss, pseudocyst,ascites, GI bleed

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G51 Gastroenterology Toronto Notes 2023

Investigations

• laboratory

• increase in serum glucose

increase in serum ALP,less commonly bilirubin (jaundice)

serum amylase and lipase usually normal

• stool elastase is low in steatorrhea

• abdominal x-ray: pancreatic calcifications

• U/S or CT:calcification,dilated pancreatic ducts, pseudocyst

• MRCP or ERCP:abnormalities of pancreatic ducts-narrowing and dilatation

• LUN: abnormalities of pancreatic parenchyma and pancreatic ducts, most sensitive test

• 72 h fecal fat test: measures exocrine function, fecal elastase preferable

• secretin test:gold standard, measures exocrine function but difficult to perform, unpleasant for

patient, expensive

Treatment

• most common problem is pain, difficult to control

• general management

• complete abstinence from EtOH

• enzyme replacement may help pain by resting pancreas via negative feedback

analgesics

celiac ganglion blocks

• time: pain decreases with time as pancreas "burns out"

• endoscopy:sphincterotomy,stent if duct is dilated, remove stones from pancreatic duct

• surgery:drain pancreatic duct (pancreaticojejunostomy) if duct is dilated (more effective than

endoscopy);resect pancreas if duct is contracted

• steatorrhea

pancreatic enzyme replacement

neither endoscopy nor surgery'can improve pancreatic function

Autoimmune Pancreatitis

•most commonly presents as a mimicker of pancreatic cancer (pancreatic mass detected because of

jaundice ± abdominal pain)

Investigations

•histology:lymphocyte and plasma cell infiltration of pancreas

•imaging:focal or diffuse enlargement of pancreas on CT or MRI,sausage-shaped, low density rim

around pancreas

•serology:increased serum lgG4 in type 1

•other organ involvement:sialadenitis, retroperitoneal fibrosis,biliary duct narrowing, nephritis

Treatment

•respondsto prednisone

•for refractory patients, consider immunomodulators (azathioprine, mycophenolate mofetil,

methotrexate) or rituximab

Clinical Nutrition

Determination of Nutritional Status

Challenging to Differentiate Markers of Malnutrition from Markers of Disease

• most important feature in assessing the need for nutritionalsupport is weight loss (expressed as

change in body massindex (kg/m-))

• Subjective Global Assessment divides nutritional statusinto A) adequately nourished, B) mild or

moderate malnutrition, and C) severe malnutrition in order to identify those who will benefit from

nutritionalsupport

• includes weight change in past 6 mo, weight change in past 2 wk,dietary intake change, current

dietary intake, G1 symptoms, functional capacity, effect of disease on nutritional requirements and

physical examination, including loss of subcutaneousfat/musdes wasting/edema/ascites

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Table 26. Small Bowel Nutrient Absorption

Fe»’ Proteins,Lipids Bile Acids

Na'

.HiO

CHO Vitamin Bn

Duodenum

Jejunum

Ileum

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G52 Gastroenterology Toronto Notes 2023

Determining Nutritional Requirements

• calories:total energy expenditure (THE)

= resting energy'expenditure (REE) x stressfactor (e.g. 1.7

for burns) usually works out to be 25-35 keal/kg depending on how disease affects metabolism, with

IV nutrition delivered as about 60% carbohydrate, 40% fat. Current trend is to provide fewer calories

(“permissive underfeeding"), especially in 1CU, to prevent hyperglycemia

• protein: 1-2 g/kg/d, depending on effect of disease on protein metabolism. In disease, a greater

proportion of energy expenditure comes from protein than in health

• electrolytes,minerals, and vitamins also required

Indications for Aggressive Nutritional Support:

• inability to meet nutritional needs;logical,but convincing evidence from literature not available for

1CU and other acute illnesses

• evidence that nutritional support improves outcome available for (I )short bowel syndrome (home

TEN), (2) before major abdominal or thoracic surgery if there is substantial malnutrition, (3) before

therapy for cancer of esophagus, head, and neck, (4) decompensated alcoholic liver disease, (5)

pancreatitis (acute and chronic). May be helpful for other indications also, but insufficient data

• nutritionalsupport at best prevents protein loss but usually no gain

Enteral Nutrition

Definition

• EN (tube feeding) is a way of providing food through a tube placed in the stomach or the small

intestine

• nasogastric (NG),or nasojejunal (N|) if nutritional support required for brief time; percutaneous

endoscopic gastrostomy (“G-tube” or “PEG tube")/percutaneous endoscopic jejunostomy (J-tube)

if nutritionalsupport required for more than 1 mo

• tubes can be placed endoscopically,radiologically,orsurgically

Indications

• oral feeding inadequate nr contraindicated

Feeds

• polymeric feeds contain whole protein, carbohydrates, fat as a liquid, and may or may not have fibre

added

• elemental feeds contain protein (as amino acids), carbohydrates (assimple sugars), and are low in fat

content (are therefore high in osmolarity)

• specific diets:low carbohydrate/high fat solution for ventilated patients(carbohydrate has a high

respiratory quotient so minimizes carbon dioxide production), high energy, low electrolyte solutions

for dialysis patients

Relative Contraindications

• non-functioning gut (e.g. intestinal obstruction, enteroenteral or enterocutaneous fistulae)

• uncontrolled diarrhea

• GI bleeding

Complications

• aspiration

• diarrhea

• refeeding syndrome (rare): carbohydrate can stimulate excessive insulin release, leading to cellular

uptake and low serum levels of phosphate, magnesium, potassium

• overfeeding syndrome (rare): hypertonic dehydration, hyperglycemia, hypercapnia, azotemia (from

excess protein)

Most Common Indications for Artificial

Nutrition Support

• Preexisting nutritional deprivation

• Anticipated or actual inadequate

energy intake by mouth

• Significant multiorgan system

disease

Whenever possible. EN is ALWAYS

preferable over PN

Parenteral Nutrition

Definition

• PN is the practice of feeding a person intravenously, bypassing the usual process of eating and

digestion

Indications

• short-term (<1 mo)

use whenever GI tract not functioning

only situations where PN has been well shown to increase survival are after bone marrow

transplant and in short bowel syndrome,some evidence for benefit in gastric cancer, but often

used in 1CU, perioperatively, and in difficult

-to-control sepsis

• preoperative: only useful in severely malnourished (e.g. loss of >15% ofpre-morbid weight,serum

albumin <28 g/L or <2.8 g/dL), and only if given for >2 wk

renal failure: PN shown to increase rate of recovery; no increase in survival

liver disease:branched chain amino acids may shorten duration of encephalopathy;no increase

in survival

IBD:PN closes fistulae and heals acute exacerbations of mucosal inflammation, but effect is

transient (EN is equally effective)

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G53Gastroenterology Toronto Notes 2023

• some evidence for efficacy, but convincing data not available for:

radiation/chemotherapy-induced enteritis

AIDS with wasting diarrhea

severe acute pancreatitis

•long-term (>1 mo):can be given at home

• severe untreatable small bowel disease (e.g. radiation enteritis, extensive GD, high output (istulae)

• following surgical resection of >70% of small bowel (e.g.small bowel infarction)

severe motility diseases (e.g.scleroderma affecting bowel)

Relative Contraindications

•functional G1 tract available for EN

•active infection; at least until appropriate antibiotic coverage

•inadequate venous access; triple-lumen central venous lines usually prevent this problem

Complications of PN

•sepsis: most serious of the common complications

•mechanical pneumothorax from insertion of central line, catheter migration and thrombosis, air

embolus

•metabolic: congestive heart failure, hyperglycemia, gallstones, cholestasis, electrolyte abnormalities,

micronutrient deficiency

Enteral Nutrition Preferable to Parenteral Nutrition

•fewer serious complications (especially sepsis)

•nutritional requirements better understood

•can supply gut-specific fuels such as glutamine and short chain fatty acids with EN

•nutrientsin the intestinal lumen have a trophic effect (prevent atrophy of the gut and pancreas)

•prevents gallstones by stimulating gallbladder motility

•much less expensive

Hypomagnesemia may be an initial sign

of short bowel syndrome in patients

who have undergone surgical bowel

resection

Enteral »s.Parenteral Nutritionlor Acute Pancreatitis

Cochrane DB Syst Ber 2010:1:C 0002837

Purpose: Compare EN vs. IPN m mortality,

morbidity,andhospital stay inpatientswith

pancreatitis.

Study Selection PCIsoflPNvs. EN in pancreatitis.

Results: E gut trials (n-348) were included. EH

decreases RR of death (0.50), multiple organ failure

(0.55),infection|0.39),and Otter local complications

(0.?0|. It also decreasedhospital stay by 2.3? d.

Conclusion: EN reducesmortality,organfiilure.

infections, and lengthol hospital stay m patients with

pancreatitis.

Common Medications

Table 27. Common Drugs Prescribed in Gastroenterology

Mechanism of

Action

Class Generic Drug Trade Name Dosing Contraindications Side Effects

Name

Indications

Proton Pump omeprazole

Inhibitors

(If /K- ATPasc

inhibitors)

Losec -

/

Prilosec '

20 mg PO once daily Inhibits gastric Duodenal ulcer,gastric

enzymes H'/K'

- ATPase ulcer, HSAIO associated

(proton pump) gastric and duodenal

ulcers,reflux esophagitis,

symptomatic OERO,

dyspepsia.ZollingerEllison syndrome,

eradication ofH. pylori

(combined with ABi)

Same as above

Hypersensitivity lodrug Dizziness,headache,

flatulence,abdominal

pain,nausea.rash,

increased risk of

osteoporotic fracture

(secondary to impaired

calcium absorption)

lansoprazole or Prevacid Same as above Same as above Same as above '

dexlansoprazole Dexilanl

Oral therapy:

lansoprazole

15-30 mg once daily

(before breakfast),

dexlansoprarole 30-60

mg once daily (does not

need to be taken before

breakfast)

40 mg PO once daily for

UGIB:80 mg IV

bolus then 8 mg/h

infusion

40 mg PO once daily

PantolocT

Protonix :

pantoprazole Same as above SameasaboveandUGIB Same as above Same as above

Pariet'

/

Aciphex '

Nexium '

rabeprarolc Same as above Same as above Same as above Same as above

csomepraiolc 20 -40 mgP0 once daily Same as above Same as above Same as above Same as above

Histamine

Hz Receptor

Antagonists

ranitidine*

'ranitidine drugs

recalled in 2019

due to impurity

concerns

Zantac - * 300 mg PO once daily or Inhibits gastric

1S0 mg 8ID

IV therapy:50 mg q3

Duodenal ulcer,gastric Hypersensitivity to drug

histamine H2 receptors ulcer, HSAID-associated

gastric and duodenal

ulcers, ulcer prophylaxis,

reflux esophagitis,

symptomatic GERD;not

useful lor acute Gl bleeds

Same as above

Confusion,dizziness,

headache,arrhythmias,

constipation,nausea,

agranulocytosis,

pancytopenia,

depression

h (but

tachyphylaxis a problem)

Pepcid! Oral therapy: duodenal/ Same as above

gastric

ulcers:40 mg qhs

GERD: 20 mg BIO

IV therapy: 20mg BID

famotidine Same as above Same as above

r -t

StoolSoftener docusate sodium Colace 100 400 mg PO once Promotes

daily,divided in1-4 doses incorporation of water

into stool

Rebel of constipation Presence of abdominal pain, throat irritation.

abdominal cramps,

rashes

lever.N/V

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G54 Gastroenterology Toronto Notes 2023

Table 27. Common Drugs Prescribed in Gastroenterology

Generic Drug Trade Name Dosing

Name

Mechanism of

Action

Class Indications Contraindications Side Effects

Osmotic

Laxatives

Constipation: 15 30 ml

POonce daily to BIO

Encephalopathy:

15-30mlBID to OID

Poorly absorbed in Chronic constipation,

Cl tradand is broken prevention, and treatment

down by colonic

bacteria into lactic

acid in the colon,

increases osmotic

colonic contents,

increases stool volume

Osmotic agent causes Relief of constipation

water retention in Colonoscopy prep

stool and promotes

frequency of stool

Osmotic retention of Relief of constipation

fluid which distends

the colon and

increases peristaltic

activity

lactulose lactulose

Constulose'

Patients who require a low

galactose diet

Flatulence,intestinal

cramps,nausea,

diarrhea if excessive

dosage

of portal-systemic

encephalopathy

PEG3350 lax-a-day 5

RestoralAX -

Golytelyr

Constipation:17 g

powder dissolved in 4-8

or liquidPOonce daily

Hypersensitivity to drug Abdominal distension,

pain,anal pain.thirst,

nausea,rigor,tonicclonic seizures (rare)

Renal impairment

Abdominal pain,

vomiting,diarrhea

Milk of

Magnesia/

Pedia -Lax!

Constipation (adult):

400 mg/5 mL:30-60 mL

POqhs

magnesium

hydroxide

Patients with myasthenia

gravis or other

neuromuscular disease

Stimulant

laxatives

Senokot 5 Tablets:1-4 POqhs

Syrup:10-15 mlPOqhs

Induce peristalsis in Constipation

lower colon

Patients with acute

abdomen

Abdominal cramps,

discolouration of breast

milk,urine,feces,

melanosis coli and atonic

colon from prolonged

use (controversial)

Abdominal colic,

abdominal discomfort,

proctitis (with

suppository use),

diarrhea

senna

bisacodyl Bisacodyl!

5-30 mg PO once daily Enteric nerve

(start at10 mg for bowel stimulation and local

contact-induced

secretory effects

Colonic movements

Constipation

Preparation of bowel for

procedure

G!obstruction

Gastroenteritis

preparation)

Bulk Laxatives psyllium Metamucil 5 Start at one heaping

tablespoon daily

Increases stool bulk Constipation

-•water retention

in stool

Hypersensitivity to drug

Gl obstruction

Gl obstruction,diarrhea,

constipation,abdominal

cramps

Guanylate

Cyclase C

Agonist

Constella1 75-145 pg once daily Opens water channels Chronic constipation

in bowel epithelial IBS-constipation

cells to add water

to stool

linadotide Children Diarrhea

Children «2 yr,known Abdominal pain or

hypersensitivity to discomfort,drowsiness

drug,acute dysentery or dizziness,tiredness,

characterized by blood in dry mouth,N/V,

stools and fever,acute UC or hypersensitivity reaction

pseudomembranous colitis

associated withbroadspectrum ABx

Hypersensitivity to

diphenoxylate or

atropine,jaundice,

pseudomembranous

enterocolitis,diarrhea

caused byenterotoxin

producing bacteria

Pancreatic disease,excess

EtOH, gallstonesor other

biliary disease

Antidiarrheal

Agents

loperamide Imodium® Acute diarrhea:4 mg PO

initially,followed by 2

mg after each unformed

stool

Acts as antidiarrheal

via cholinergic,

noncholingeric,

opiate,and non-opiate associated with IBD and

receptor-medicated

mechanisms;

decreases activity of

myenteric plexus

Inhibits Gl propulsion Adjunctive therapy for

via direct action diarrhea,as above

on smooth muscle,

resulting in a decrease

in peristaltic action

and increase in transit

lime

Bowel opioid

modulator

Adjunctive therapy

for acute non-specific

diarrhea,chronicdiarrhea

for reducing the volume of

discharge for ileostomies,

colostomies,and other

intestinalresections

diphenoxylate/

atropine

Lomotil - 5 mg PO TID to OID Dizziness,drowsiness,

insomnia,headache,

N/V,cramps,allergic

reaction

eluxadoline Viberzil - 75-100 mg BID IBS Pancreaticobiliary pain

including sphincter of

Oddi dysfunction

Diarrhea

Antiemetics dimenhydrinate Gravol - 25-50 mg PO/IV/IM

q4- 6 h PRN

Competitive Hr

receptor antagonist in sickness,postoperative

Gl tract,blood vessels, vomiting, and drugand respiratory tract, induced N/V

Blocks chemoreceptor

trigger zone

Diminishes vestibular

simulation and

disrupts labyrinthine

function through

central anticholinergic

action

01,DLeceptor

antagonist in

chemoreceptor trigger

zone and o-adrenergic

and anticholinergic

effects

Depresses reticular

activating system

(RAS) affecting emesis

Dopamine and 5-HI

receptor antagonist

in chemoreceptor

trigger zone.Enhances chemotherapy induced N/V, pheochromocytoma.

response to ACh migraines,constipation seizures,and EPS

inupper Gl tract,

enhancing motility

and gastric emptying.

Increases IES tone

Motion sickness,radiation Hypersensitivity to drug Xerostomia,sedation

prochlorperazine Stemetil 5 5-10 mg PO/IV/IM BID TID Postoperative N/V,

antipsychotic,anxiety

Hypersensitivity to drug Dystonia,

extrapyramidal

symptoms|EPS),seizure,

NMS (rarely)

PRN

metoclopramide Maxeran - 10 mg IV/TM q2-3 h pm,

10 -15 mg P0 OID (30 min

before meals and qhs)

GERO,diabetic

gastroparesis.

postoperative and

Restlessness,

drowsiness,dizziness,

fatigue, EPS,some

rareseriousside

effects include NMS,

agranulocytosis

Hypersensitivity to

drug.Gl obstruction,

perforation,hemorrhage. ri

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