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GS8General and Thoracic Surgery Toronto Notes 2023
Drains
. NG tube
• indications: gastric decompression, analysis of gastric contents, irrigation /dilution of gastric
contents, feeding, and/or administration of medications, if necessary
2 types: NG tube (for drainage or feeding) and Dobhoff (for feeding only)
insertion should be done in stages with x-ray protocol to avoid injury
• contraindications:suspected basalskull fracture, obstruction of nasal passages,esophageal
stricture, esophageal varices
• Foley catheter with urometer
indications: to accurately monitor urine output, decompression of bladder, relieve obstruction,
rapidly expanding suprapubic mass
contraindications:suspected urethral injury and difficult insertion of catheter
Drain Sire
Measured by the unit French:
French ~ diameter (mm) x 3
Surgical Complications
• general principles in preventing complications during the postoperative p
• frequent examination of the patient (daily or more) and their wound
• removal of surgical tubes assoon as possible (e.g. Foley catheters and surgical drains)
early mobilization
monitor fluid balance and electrolytes
• analgesia - enough to adequately address pain (minimize opioids through routine use of antiinflammatories and acetaminophen)
eriod Include:
Postoperative Fever
• postoperative fever is considered a temperature higher than 38C on two consecutive postoperative
days or higher than 39C on any postoperative day
• fever does not necessarily imply infection, particularly in the first 24-48 h postoperative!)'
• fever may not be present or may be blunted if patient is receiving chemotherapy, glucocorticoids, or
other immunosuppressive agents
• timing of fever may help identify cause
• hours aftersurgery - POD #1
inflammatory reaction in response to physiological stressfrom surgery; most common cause
of fever on POD #1-3and unlikely to be infectious(unless necrotizing fasciitis or another
severe infection)
reaction to blood products received during surgery
malignant hyperthermia
• POD #1-2 (acute)
atelectasis
early necrotizing fasciitis wound infection (especiallyClostridium perfringens, (5-hemolytic
Group A Streptococcus)
-,feel for crepitus and look for “dishwater"
drainage
• aspiration pneumonitis
• other: acute adrenal insufficiency, thyroid storm, and transfusion reaction
POD #3-7: likely infectious
UT1,surgicalsite infection, IV site/line infection (commonly with Staphylococcus),septic
thrombophlebitis, and leakage at bowel anastomosis (tachycardia, hypotension,oliguria, and
abdominal pain)
POD #8+
intra-abdominal abscess, DVT/PE (can be anytime postoperative, most commonly POD #8-
10, may occur earlier but recognition is often delayed), and drug fever
other: URT’
I, infected scroma/hiloma/hcmatoma,C difficile colitis, and endocarditis
Treatment
• resuscitation then treat primary cause
Wound/Incisional Complications
WOUND CARE (see Plastic Surgery, PL8)
• can shower POD #2-3 after epithelialization of wound (or earlier depending on dressing)
• most dressings can be removed POD #2 and left uncovered if dry
• Steristrips or dermabond glue should be left on for up to 2 wk
• examine wound for wet dressing,signs of infection (fever, tachycardia, and pain)
• skin sutures and staples can be removed POD # 7-10
exceptions:incision crosses crease (groin), closed under tension, in extremities (hand) or patient
factors(elderly, corticosteroid use, or immunosuppressed) removed POD #14 or earlier if there are
signs of infection
• negative pressure dressings consist of foam and suction, promote granulation
ideal for large (grafted sites) or non-healing wounds (irradiated skin or ulcer)
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GS9 General and Thoracic Surgery Toronto Notes 2023
DRAINS
• drains may be placed selectively at the time ofsurgery to prevent fluid accumulation (blood, pus,
serum, bile,and urine)
can be used to assess quantity of third space fluid accumulation postoperativelv
• potential route of infection; to decrease risk of wound infection bring out through separate incision
(vs. operative wound) and remove as soon as possible
• types of drains
• open (e.g. Penrose), higher risk of infection
closed: 1) gravity drainage (e.g. Foley catheter); 2) underwater-seal drainage system (e.g. chest
tube);3) suction drainage (e.g.lackson-Pratt)
sump (e.g. NG tube)
• monitor drain outputs daily
• drainsshould be removed once drainage is minimal (usually <30-50 cc/24 h)
• drains do not guarantee that the patient will not form a collection of fluid
• ridged drains can erode through internal structures, and excessive suction can cause necrosis
• evidence does notsupport routine postoperative drainage of abdominal cavity
Complication laboratory/lmaging Tests
Wound Wound cultutc. CBC. Cl scan
Complication
Fever CSC. eteebotytes. glucose,
creatinine. BUN.U/A.CXR,
urine/blood sputum and
wound cultureif applicable
EKG,echo,CXR,ABG,CTangiography of the chest
AKI/Oliguria Electrolytes,glucose.
creatinine. 8UH. U ’A
with microscopy,urine
electrolytes. EKG. renal U/S
Hypotension CSC. electrolytes,glucose,
creatinine. 8UH. lactate.
ABG.ACTHstimutation
testing,cortisol level,and
coagulation studies
Electrolytes,glucose,
creatinine,8UH. AXR
Stress Ulcer CBC. upper endoscopy
Respiratory
Distress
SURGICAL SITE INFECTION
Etiology
• most surgical wounds are contaminated by bacteria often consisting of normal endogenous flora from
skin, respiratory, GU, or GI tracts(depending on surgery)
• e.g. skin flora (Gram positive cocci: S. aureus. Streptococcus spp.) and GI flora (Gram positive
microbes: Enterococcus spp., Clostridium spp.; Gram negative rods: E. coli; anaerobic species)
Risk Factors
Ileus
PreoperativeSkin Antisepticsfor Preventing
Surgical Wound Infections after CleanSurgery
Cochrane DB Syst Rev 2015;4:CD003949
Purpose:lo determine whether preoperalive skin
antisepsis prior to dean surgery prerentssurgicalsite infection (SSI) and to compare the effectiveness
of other antiseptics.
Methods:Systematic renew of RCIs part ol the
Cothiane Wounds Group Specialised Register and
the Cochrane Central Register of Coufroled Trials
(CENTRAL). Main outcome wasSSI.Secondary
outcomes included quality of bfe.mortaldy. and
resource use.
Resnlts:13RCTs ( n-2S23 patients)were included
that made11 total comparisons between skin
antiseptics.A single stu dy foun d that0.5%
chtorhendine solution in methylated spirits was
significantly superior m preventing SSIs after dean
surgery compared toalcobol-trased povidone lor) ne
solution. No ocher statistically vgiificant differences
weielound.
Conclusions:Further research is warranted to
determine tlreellectireness o< one antiseptic over the
others at preventing SSI post dean surgery.
Table 5. Classification of Surgical Wound Contamination
Classification Clean Clean-Contaminated Contaminated Dirty/Infected
Definition Established infection present
before wound is made in skin;
contamination of wound during traumalic wound with delayed
procedure (i.e.gross spillage Ireatment
of stool, inlection in biliary, Traumatic wound with delayed
respiratory,oi GU systems) treatment
Incision under
sterile conditions;
nontraumatic;no
entrance of hollow
organ
Incision under sterile
conditions;ENTRANCE of hollow conditions:MAJOR
viseus with no spillage: no
evidence of active infection:
minimal conlamrnalion with
no spillage
Incision under sterile
Roulme cholecystectomy; colon Bowel obstruction with
resection
Appendiceal abscess: traumatic
wound with contaminated
devitalized tissue;perforated
viscus
Example Hernia repair
enterotomy and spillage ol
contents;necrotic bowel
resection:fresh traumatic
wounds
Infection Rate "
2%
Wound Closure Primary closure
3-4%
Primary closure
7-10%
Often secondary closure
30- 40%
Secondary closure
•patient characteristics
• age, DM,steroids, immunosuppression,smoking, obesity, burn, malnutrition, patient with other
infections, traumatic wound, radiation, and chemotherapy
•other factors
» prolonged preoperative hospitalization,skin preparation, multiple antibiotics, reduced blood
flow, break in sterile technique,foreign bodies (drains,sutures, grafts), excessive tension,
hematoma,serorna, hypoxemia, and hypothermia
Prophylaxis
•preoperative antibiotics for most surgeries (ccfazolin ± metronidazole or if p-lactam allergy,
clindamycin ± gentamicin or vancomycin)
• within 1 h pre-incision; can re-dose at 1-2 half-lives (~q4-8 h ) in the OR
• not required for low-risk or clean surgery, e.g. elective thyroidectomy, cholecystectomy,
hemorrhoidectomy, fistulotomy, and sphincterotomy for fissure
• important to review patient factors and clinical context; immunosuppression (transplant,
Cushing’s, malignancy, etc.) would likely warrant preoperative antibiotics
some evidence suggests role in breast surgery
• important that redosing antibiotics is performed if surgery is longer than the half-life of
antibiotics
•reserve postoperative antibiotics for treatment of suspected or documented intra-abdominal infection
• normothermia (maintain patient temperature 36-38*C in the OR)
•hyperoxygenation (consider EiO:of 80% in OR)
•chlorhexidine-alcohol wash ofsurgical site
•hair removal should not be performed unless necessary;if so, clipping superior to shaving done at the
time of surgery
•consider delayed primary closure of incision for contaminated wounds
•use sterile closing tray for laparotomy
Primary vs. Delayed Primary Incision Closure
in Contaminated Abdominal Surgery:AMeta - Anilysis
JSurg Res 2019:239:22 30
Purpose: lo determine il delayed pnnaiy inns or
closure (DPC) haslower rates of surgicalsite
rrrfections(SSI|and length of stay (LOS) compared
tp primary incision closure (PC) in contaminated
abdominalsurgery.
Methods:Systematic renew and meta-analysis of
RCIs in Medline. Embase, and Cochrane data base
between 1980-2017.
Results: 12 RCIs were included andanalyzed.Using
a tried effect model. OPC showed Significantly
reduced SSI with nsk ratio of 0.64 (9S\Cl 0.51-0.79;
P> 0.0001) and reduced 10S with amean difference
oi lessthan one day compared with PC.However,
usng a random-effect model, there was no significant
rtfference in SSI or LOS.
Conclusions: DPC may be the preferential option
in contaminated abdominal incisions, however
higher quality research is required to proride a more
comprehensive evidence base.
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GS10 General and Thoracic Surgery Toronto Notes 2023
Clinical Features
• typically fever POD #5-8 (
.Streptococcus and Clostridium can present in 24 h)
• localized pain, blanchablc erythema, induration, purulent discharge, and warmth
• complications:fistula,sinus tracts,sepsis, abscess,suppressed wound healing,superinfection,
spreading infection to myonecrosis or fascial necrosis (necrotizing fasciitis), wound dehiscence,
evisceration, and hernia
Treatment
• examination of the wound:inspect, compress adjacent areas,swab drainage for C&S and Gram stain
• reopen affected part of incision, drain, pack, heal by secondary intention in most cases
• for deeper or necrotizing infections, debride necrotic and non-viable tissue
• antibiotics and demarcation of erythema only if cellulitis or immunodeficiency
WOUND HEMORRHAGE/HEMATOMA
Risk Factors
• anticoagulant therapy, coagulopathies, thrombocytopenia, DIC,severe liver disease,
myeloproliferative disorders,severe arterial HT'
N, and severe cough
• more common with transverse incisions through muscle due to vascularity of muscle
• more clinically relevant in small working spacessuch as breast or thyroid surgery (airway edema/
compression)
Clinical Features
• pain,swelling, discolouration of wound edges, and leakage
• rapidly expanding neck hematoma can compromise airway and is a surgical emergency: consider
having a suture kit at bedside in all neck surgery in the event of having to open the wound emergently
(most important treatment in this case isto protect the airway with intubation)
Treatment
• pressure dressing
• open drainage ± wound packing (large hematoma only)
• ifsignificant bleeding, may need to re-operate to find source (often do not find a discrete source)
SEROMA
• fluid collection related to serous lymph drainage
• secondary to transection of lymph vessels
• increased infection risk if drained
Treatment
• observation
• consider pressure dressing ± needle drainage (this may increase infection risk)
WOUND DEHISCENCE
• disruption of a wound that was primarily closed, causing loss of barrier of skin or fascia
Risk Factors
• local: technical failure of closure, excessive tension on the wound, increased intra-abdominal pressure
(c.g.CQPD, ileus, bowel obstruction), hematoma, infection, poor blood supply,radiation, and
transverse incision
• systemic:male,smoking, malnutrition (hypoalbuminemia, vitamin C deficiency), connective tissue
diseases, immunosuppression, pulmonary disease, ascites, poor nutrition,steroids, chemotherapy,
obesity, and other (e.g. age,sepsis, and uremia)
• DM alone is not a risk factor
Clinical Features
• typically POD #1-3 or «7-10; most common presentation sign is serosanguinous(salmon-coloured)
drainage from wound;erythema or leakage of enteric material
• + evisceration
• palpation of wound edge:should normally feel a “healing ridge” from abdominal wall closure (raised
area of tissue under incision)
Treatment
• place moist dressing over wound with binder around abdomen and transfer to OK
• may consider conservative management with debridement of fascial and/orskin margins
• evisceration (i.e.‘burst abdomen’) is a surgical emergency:take patient for operative re-closure
INCISIONAL HERNIA
• a late complication of fascial dehiscence and failure of fascial closure;G1 contents are still contained
within sack of peritoneum
• hernia can develop 6-8 wk postoperatively due to poor wound healing and/or increased stress on
abdominal wall
• symptoms aggravated by coughing orstraining
• smaller fascial defectssuch aslaparoscopic port sites have a higher risk of incarceration
• definitive treatment:surgical repair
large hernias that pose little risk of incarceration do not need to be repaired as minimal chance of
bowel obstruction
Small lilts«s.Large B itesIor Closure of
Abdominal Midlint Incisions (Stitch):A Double
Blind.Multkentre.Randomistd Controlltd Trial
Lancet 2015:336:1254-1260
Purpose:To compare the large bitessuture technique
with the small b.testechnique for lascial closure of
midline laparobonrp iochrons.
Methods: PCI conducledat 10 hospitalsln the
Netherlands.Patients undergoing elective abdominal
surgery randomiied (1:1|to small or large bite
technique.Primary outcomewas incisional hernia
occurrence.
Results:At one year follow-up, the large bites
group had a greater incidence olincisional hernia
occurrence than the small bitesgroup (21% us.13V
respectively).Rates ol adveise events did not differ
between the groups.
Conclusion:Small bitessuture technique a
superior to the large bitestechnique for preveotioo
of incisional hernia io m id line incisionsand is not
associated with a higher rate of adverse events.
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GS11 General and Thoracic Surgery Toronto Notes 2023
Urinary and Renal Complications
URINARY RETENTION
• may occur after any operation with general anesthesia or more commonly with spinal anesthesia
• more likely in older males with history of benign prostatic hyperplasia and patients on
anticholinergics but can also happen in young, healthy patients
Clinical Features
• abdominal discomfort, palpable bladder,overflow incontinence, post-void residual urine volume >100 mL
Treatment
• Foley catheter to rest bladder, then trial of voiding
• often accompanied by an a-blocker such as tamsulosin (does notstart working for 48 h)
• if postoperative retention:patients may need to be sent home with foley catheter to follow-up within
the week for trial
-of-void
OLIGURIA/ANURIA
Etiology
• prerenal (e.g. hypovolemia due to transient renal hypoperfusion) vs.renal (e.g.ATN, acute interstitial
nephritis (AIN), acute glomerulonephritis) vs. postrenal (e.g. urinary tract obstruction)
• most common postoperative cause is prerenal ± ischemic ATN
external fluid loss: hemorrhage, dehydration, and diarrhea
internal fluid loss: third-spacing due to bowel obstruction and pancreatitis
Clinical Features
• urine output <0.5 cc/kg/h (e.g. <450 cc in 75 kg patient in 12 h),increasing Cr and BUN
Treatment
• according to underlying cause; fluid deficit is treated with crystalloid ( NS or RL)
Postoperative Dyspnea
•see Respiratory Complications and CardiacComplications, GSI 2
Etiology
• respiratory: atelectasis, pneumonia/pneumonitis, pulmonary embolism ( PE), ARDS, asthma, and
pleural effusion
•cardiac: Ml, arrhythmia, and CHF
•inadequate pain control
Respiratory Complications
ATELECTASIS
• comprises 90% of postoperative pulmonary complications
Risk Factors
• COPD,smoking, obesity,and elderly persons
• upper abdominal/thoracic surgery, oversedation,significant postoperative pain, and poor inspiratory
effort
Clinical Features
• postoperative atelectasis may be asymptomatic or present as low-grade fever on POD #1, tachycardia,
crackles, decreased breath sounds, bronchial breathing, and tachypnea
Treatment
• preoperative prophylaxis
smoking cessation (best if >8 wk preoperative)
• postoperative prophylaxis
incentive spirometry,deep breathing exercise,chest physiotherapy, and intermittent positivepressure breathing
• short-acting neuromuscular blocking agents
minimize use of respiratory depressive drugs, and ensure adequate pain control, and early
ambulation r n
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PNEUMONIA/PNEUMONITIS
• may be secondary to aspiration of gastric contents during anesthetic induction or extubation causing
a chemical pneumonitis
Risk Factors
• aspiration:general anesthetic, decreased LOG,GERD, full stomach, bowel/gastric outlet obstruction +
non-functioning NG tube, pregnancy, and seizure disorder
• non-aspiration: atelectasis, immobility, and pre-existing respiratory disease
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GS12 General and Thoracic Surgery Toronto Notes 2023
Clinical Features
• productive cough and fever
• tachycardia, cyanosis, respiratory failure, and decreased LOG
• CXR: pulmonary infiltrate
Treatment
• prophylaxis:see atelectasis prophylaxis, preoperative NPO/NG tube, and rapid sequence anesthetic
induction
• immediate removal of debris and fiuid from airway
• consider endotracheal intubation and flexible bronchoscopic aspiration
• empiric IV antibiotics to cover oral nosocomial aerobes and anaerobes (e.g. piperacillin- tazobactam,
cefepime + metronidazole)
PULMONARY EMBOLUS
Clinical Features
• unilateral leg swelling and pain (DVT as a sourceof PH),sudden onset dyspnea, pleuritic chest pain,
tachycardia, and fever
• most commonly POD #8-10, but can occur anytime postoperatively, even after discharge
• diagnosis made by chest CT scan usually
Treatment
• initial treatment: IV heparin or subcutaneous LMWH, bridging to therapeutic anticoagulation
is required for a minimum of 3 mo (usually 6 mo);for patients with cancer, or other risk factors
for hypercoagulability, the duration of anticoagulation may be longer;severe cases may require
endovascular thrombectomy and thrombolysis
• Greenfield (1VC) filter if contraindications to anticoagulation helps prevent worsening of PH
• prophylaxis:subcutaneous heparin (5000 units BID) or LMWH, compression stockings (TEDTTM
Hose), and sequential compression devices
PULMONARY EDEMA
Etiology
• cardiogenic vs. noncardiogenic
• circulatory overload: excess fluid overload, left ventricular (LV ) failure, shift of fluid from peripheral to
pulmonary vascular bed, negative airway pressure, and alveolar injury due to toxins (e.g. ARDS)
• more common with pre-existing cardiac disease
• negative pressure pulmonary edema due to inspiratory efforts against a closed glottis upon awakening
from general anesthesia
Clinical Features
• shortness of breath, crackles at lung bases, and CXR abnormal
Treatment (LMNOP)
• Lasix* (furosemide)
• Morphine (decreases symptoms of dyspnea, venodilator, and afterload reduction)
• Nitrates (venodilator)
• Oxygen + non-invasive ventilation
• Position (sit patient up)
New onset 'asthma" and wheezing in
the elderly Is cardiogenic until proven
otherwise
RESPIRATORY FAILURE
Clinical Features
• dyspnea, cyanosis,and evidence of obstructive lung disease
• earliest manifestations- tachypnea and hypoxemia (RR >25, PO’ <60)
• pulmonary edema and unexplained decrease in SaO’
Treatment
• ABCs, O2, ± positive pressure ventilation, and intubation
• bronchodilators and diuretics to treat CHI'
• adequate blood pressure to maintain pulmonary perfusion
• if these measures fail to keep Pa02 >60, consider ARDS (see Respirology. R26)
Cardiac Complications
•abnormal HCGs common in postoperative period (compare to preoperative HCG)
•common arrhythmias: supraventricular tachycardia, atrial fibrillation (secondary to fluid overload,
PH, and Ml)
MYOCARDIAL INFARCTION
•see Cardiology and Cardiac Surgery, C9
•surgery increases risk of Ml
•incidence
0.5% in previously asymptomatic men ages >50
40-fold increase in men ages >50 with previous Ml
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GS13 General andUtoracic Surgery Toronto Notes 2023
Risk Factors
• preoperative H IN,CHI
• previous Ml (highest risk <6 mo, but risk never returns to baseline)
• increased age
• intraoperative hypotension
• operations >3 h
• angina
Clinical Features
• majority of cases on day of operation or POD*3-4 (shifting of third space fluid back into intravascular
compartment)
• often silent without chest pain, may only present with new-onset CHF (dyspnea), arrhythmias, and
hypotension
Intra-Abdominal Abscess
Definition
• collection of pus walled-off from rest of peritoneal cavity by inflammatory adhesions and viscera
Etiology
• usually polymicrobial:Gram-negative bacteria, and anaerobes
• consider Gram-positivesif coexisting cellulitis
Risk Factors
• emergency surgery and contaminated OR
• GI surgery with anastomotic leak
• poor healing risk factors (DM, poor nutrition, etc.)
• may occur POD «3 after laparotomy when third space fluid redistribution occurs
Clinical Features
• manifests at least 5-7 d aftersurgery. Cannot manifest earlier as it takes time to form collection
• persistentspiking fever, dull pain, and weight loss
• peritoneal signs if abscess perforation and secondary peritonitis
• leukocytosis or leukopenia (immunocompromised and elderly)
• coexisting effusion (pleural effusion with subphrenic abscess)
• mass is often difficult to palpate
• common sites:pelvis, Morrisons pouch (space between kidney and liver),subphrenic, paracolic
gutters,lesser sac, peri-appendiceal,post-surgical anastomosis,diverticular, and psoas
Investigations
• CBC, blood cultures x2
• CT ± IV and water-soluble contrast
• DUE (pelvic abscess)
Treatment
• drain placement by interventional radiology (preferred), laparoscopy, and open drainage
• subsequent antibiotic coverage; ceftriaxone metronidazole or piperacillin-tazobactani (Pip-Tazo)
Differential Diagnosis of Upper 61
Symptoms
GI Causes Non Cl Causes
Cholelithiasis
Diverticulitis
Peptic ulcer
Achalasia
Pancreatitis
Ml
Angina Paralytic Pericarditis Ileus
• see Paralytic Ileus,GS3I
GERD
Gastritis Delirium Hiatus hernia
• see Psychiatry, PS23 and Neurology, N21
Horner has a MAPof the Coast
A Pancoast tumour compresses the
cervical sympathetic plexus causing
Horner's syndrome:
Miosis
Anhydrosis
Ptosis
Thoracic and Foregut Surgery
Approach to the Solitary Pulmonary Nodule
•see Medical Imaging. MIS
Definition
•lesion up to 3cm, which may or may not be calcified and is surrounded by normal lung
•can be benign or malignant
r -i
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Differential of an Anterior
Compartment Mass
4 Ts
Thymoma +
Thyroid enlargement (goitre)
Teratoma
Tumours (lymphoma,parathyroid,
esophageal, angiomatous)
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GSM General and Thoracic Surgery Toronto Notes 2023
Table 6. Differential Diagnosis for Benign vs. Malignant Solitary Nodule
Benign (70%) Malignant (30%)
Bronchogenic carcinoma
Adenocarcinoma
Infectious granuloma (histoplasmosis, coccidiomycosis,16.
atypical mycobacteria) •most common
Other infections (bacterial abscess. POP. aspergilloma)
Benign neoplasms( hamartoma, lipoma, fibroma)
Vascular (AVmalformation, pulmonary varix)
Developmental (bronchogeniccyst)
Inflammatory (granulomatosis with polyangiitis, rheumatoid
nodule,sarcoidosis, amyloidosis)
Other (infarct, pseudotumour, rounded atelectasis, lymph nodes,
amyloidoma)
Metastatic lesions
Breast
Head and neck
Melanoma
Colon
Kidney
Sarcoma
Gerin cell tumours
SCC
Large cell carcinoma
Small cell carcinoma
Small cell lung cancer
Investigations
• CXR:always compare with previous CXR
• CT and contrast-enhanced CT of thorax
• biopsy (bronchoscopic or percutaneous) or excision (thoracoscopy):if clinical and radiographic
features do not help distinguish between benign or malignant lesion
if at risk forlung cancer,biopsy may be performed regardless of radiographic features
if a biopsy is non-diagnostic, whether to observe, re-biopsy, or resect will depend on the level of
suspicion
• watchful waiting: repeat CT scan at 3,6, 12 mo depending on nodule characteristics and patient risk
• PET scan can narrow the differential diagnosis
Table 7. CT Characteristics of Benign vs. Malignant Solitary Nodule
Parameters Benign Malignant
Sire Module ("3 cm)
Smooth or lobulaled
Calcified pattern:diffuse, central,laminated,
'‘popcorn"
pattern if hamartoma, usually no cavitation:if cavitating.
wall issmooth and thin, no other lung pathology
Doubles in <20 or >400 d
Mass (»3cm)
Irregular or spiculated
Usually not calcified:if calcified, pattern is eccentric,
stippled,no satellite lesions, cavitation with thick wall,may
have pleuralelfusions. lymphadcnopalhy
Doubles between 20 and 400 d
Borders
Features
Doubling Time
Table 8. Evaluation of a Solitary Pulmonary Nodule
SOLID NODULES
Size <6 mm («100 mm'
) Size 6-8 mm (100-250 mm1
) Size >8 mm (>250 mm1 Nodule Type )
Single
Low-Risk No routine follow-up Cl at 6-12 mo.then consider CT at
18-24 mo
Cl at 6-12 mo. then at 18 24 mo
Consider CT a 3mo.PET/CT or tissue
sampling
Consider CT a 3 mo. PET/CT or tissue
sampling
High-Risk Optional CT at 12 mo
Multiple
Low-Risk CT at 3- 6 mo. then consider CT at
18- 24 mo
CT at 3-6 mo.then at 18-24 mo
CT at 3-6 mo.then consider CT at
18-24 mo
CT at 3-6 mo then at18-24 mo
No routine follow-up
High-Risk Optional CT at12 mo
SUBSOLID NODULES
Size < 6 mm («100 mm1
) Size >6 mm (>100 mm1 Nodule Type )
Single
Ground Glass
Part Solid
CT at 6-12 mo to confirm persistence then CT every 2 yr until 5 yr
Cl at 3-6 mo to confirm persistence
If unchanged and solid component remains <6 mm.annual CT should be
performed for 5yr
CT at 3-6 mo
Subsequent managementbased on the most suspicious nodule(s)
No routine follow- up
No routine follow- up
Multiple CT at 3- 6 mo. II stable consider CT at
2 and 4 yr
Adapted from:MacMahon H.NaidichDP.Goo JM.et al.Guidelines for Management of Incidental Pulmonary Nodules Detected on CT Images. The
Fleischner Society 2017.Radiology Journal. doi:10.1148/radiol.2017161659.Feb 23 2017.
Lung Cancer
Classification
• lung tumours can be classified as:
primary or secondary
• benign or malignant
endobronchial or parenchymal
• bronchogenic carcinoma (epithelial lung tumours) are the most common type of primary lung tumour
(other types make up less than 1%)
small cell lung cancer (SCLC): 10-15%
L J
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GS15 General and Thoracic Surgery Toronto Notes 2023
• non-small
-cell lung cancer (NSCLC):85-90%
SCC:arise from the proximal respiratory epithelium
adenocarcinoma: incidence is increasing; most common subtype in nonsmokers
- mucinous adenocarcinoma: grows along the alveolar wall in the periphery; may
arise at sites of previous lung scarring
large cell carcinoma
• benign epithelial lung tumours can be classified as papillomas or adenomas
Table 9. Characteristics of Lung Cancer
Cell Type Percentage of Correlation Location Histology
Lung Cancer with Smoking
Metastasis 5 Yr Survival Rates Canadian Task Force on Preventive
Health (2016)
Screening with low-dose CT
recommended for high-risk patients
10-15% Strong Central Oat cell,
neuroendocrine
Disseminated at
entation
10-13% limitedstage.
1-2% eUensive stage
SCLC
presi
Origin in
endobronchial cells
3nl'
,:
- 55-74 yr
• >30 pack-yr smoking Hx
• Current smoker or quit within last Adenocarcinoma M:35%
F:40%
70% limitedstage.7%
extensive stage
Moderate Peripheral Papillary,lepidic. Early,distant
acinar,mucinous,
solid
Central Keratin,
intercellular
bridges
Peripheral Anaplastic,
undifferentiated
15 yr
- Annual screening low-dose CT up to
3yr ONLY in centres with expertise
in diagnosis and treatment of lung
cancer
SCC 30% Strong Local invasion and 47%limited stage.6%
distant spread,may extensive stage
cavitate
Early,distant 53%limitedstage.5%
extensive stage
Large Cell
Carcinoma
10-15% Strong
US Mortality Files. National Center tor Health Statistics.CDC
Risk Factors
• cigarette smoking: the relative risk of developing lung cancer is 10-30 times higher for smokers than
for nonsmokers
• risk of lung cancer increases with number of cigarettessmoked per day (linear) and duration of
smoking (exponential)
• other risk factors: cigarsmoking, pipe smoking,second-hand smoke, asbestos withoutsmoking
(relative risk is 5), asbestos with smoking (relative risk is 92), metals (e.g.chromium, arsenic, nickel),
radon gas, ionizing radiation, and genetics
Clinical Features
• may be due to primary lesion, metastasis, or paraneoplastic syndrome
• primary lesion
cough (75%); beware of chronic cough that changes in character
dyspnea (60%)
chest pain (45%)
hemoptysis(35%)
other pain (25%)
clubbing (21%)
constitutional symptoms: anorexia, weight loss,fever, and fatigue
• metastasis
• lung, hilum, mediastinum, pleura:pleural effusion, atelectasis, wheezing, post-obstructive
pneumonia
pericardium: pericardial effusion, pericardial tamponade
esophageal compression: dysphagia
• phrenic nerve: paralyzed diaphragm, dyspnea
• recurrent laryngeal nerve: hoarseness
superior vena cava syndrome
obstruction of SVC causing neck and facialswelling
other symptoms:dyspnea, cough, hoarseness, tongue swelling, epistaxis, and hemoptysis
physical findings:dilated neck veins, increased number of collateral veins covering the
anterior chest wall, cyanosis, edema of the face, arms,and chest, Pemberton'
ssign (facial
flushing, cyanosis, and distension of neck veins upon raising both arms above head)
milder symptoms if obstruction is above the azygos vein
• lung apex ( Pancoast tumour):Horner’ssyndrome, brachial plexus palsy (most commonly C8and
T1 nerve roots)
• rib and vertebrae: erosion, pain
• distant metastasis to brain, bone,liver, and adrenals
• paraneoplastic syndromes
• most often associated with SCLC
Malignant
©
lung tumours are the most
common cause of cancer mortality in
both men and women worldwide
Endobronchial Ultrasound (EBUS)
• Allows visualization of peri-bronchial
structures and lung lesions
• Allowsfor guided biopsies of lymph
nodes and tumours
• Used for diagnosis and staging
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GSI6 General and Thoracic Surgery Toronio Notes 2023
Table 10. Paraneoplastic Syndromes
System Clinical Features Associated Malignancy
2/3 of primary lung cancer is foundin
the upper lung:2/3 of metastases occur
in the lower lung (hematogenous spread
secondary to increased blood flow to the
base of the lung)
Skeletal Clubbing, hypertrophic pulmonary osteoarthropathy (HPOA)
Acanthosis nigricans
Oermatomyosltis
Hypercalcemia (osteolysis or PIHrP)
Hypophosphatemia
Hypoglycemia
Cushing'
ssyndrome (ACIH)
Carcinoid syndrome
SIADH
lambert-Eatonsyndrome
Polymyositis
Subacute cerebellar degeneration
Spinocerebellar degeneration
Peripheral neuropathy
Nonbacterial endocarditis
trousseau'
ssyndrome (migratory thrombophlebitis)
Non -small cell lung cancer (NSCLC)
Dermatologic Lung cancer
Endocrine SCC
SCC
Saicoma
Small cell lung cancer (SCLC)
Bronchial carcinoid
SCLC
Heuromyopathic SCLC
Vascular/Hematologic Lung cancer
NSCLC
QIC
Renal Nephrotic syndiome Lung carcinoma
Investigations
• initial diagnosis
imaging: CXR, CT chest + abdomen, PET scan
biopsy: bronchoscopy, EBUS,CT-guided percutaneous needle biopsy
• staging workup
TNM staging system:T- primary tumour (size); N -regional lymph nodes;M - distant
metastasis
blood work: electrolytes, Ll'
Ts, calcium, ALP
• imaging: CXR, CT thorax and abdomen, PET'
scan, bone scan (
-in confirmed stage I cancer),
neuroimaging (MRI Brain)
• invasive: bronchoscopy (EBUS), mediastinoscopy, VATS
Prevention
• Smoking cessation
• Avoidance of exposures
• Early detection
Terminology
• "Nodule" <3 cm
• "Mass" >3 cm
Table 11. SCLC vs. NSCLC
Stage Definition Treatment Median Survival Mutations in endothelial growth factor
receptor are more common in nonsmoking patients with adenocarcinoma Limited stage Confined lo single radiation port (one Radiation t chemotherapy
hemithorax and regional lymph nodes) i prophylactic to brain
Extensive stage Extension beyond a single radiation port Chemotherapy
SCLC 1-2 yr (12 vvk without
treatment)
6 mo (5 wk without
treatment)
Stage TNM Treatment 5 Yr Survival (%)•
Corona Radiata Sign on Chest CT
• Fine striations that extend linearly
from a nodule in a spicutated fashion
• Highly associated with malignancy
HSCLC 0 TisNOMO
TtaNOMO
TlbNOMO
TkNOMO
T2aN0M 0
T2bH0M0
1st line iscomplete surgical resection
(VAIS or open thoracotomy) with possible 90-92
83-85
77-80
68-73
60-65
IA1
IA2 postoperative adjuvant chemotherapy
with stage IB and stage It:radiotherapy
for non-surgical candidates
IA3
IB
IIA
IIB T3N0M 0 or T1H1M 0 or T 2N1M 0 53 56
Carcinoids
• Early onset (40-60 yr)
• Most are central and can produce
symptoms and signs of bronchial
obstruction
• Hemoptysis is present in-50% of
cases
• Assuming adequate pulmonary
function,surgicalresection (i.e.
segmentedomy. wedge resections,
and lobectomy) is the preferred
treatment approach
T 4N0M0 or T 4H1M0 or I3M1N 0 or T1N 2M0 Combined modality appioach (chemo 36- 41
or T 2N 2M0
IMA
t radiation, and sometimessurgical
resection)
IIIB T3N 2 M0 or I4M2 N0 or T1N3M 0 or I 2 N 3M0 24 26
IIC f 3N 3M0 or I4N 3M0
T1-4N 0-3M1a-1b
1213
IVA Systemic therapy or molecularly targeted 10
therapy orsymptom-based palliative
management (radiation):isolated
metastasis may be resected
IVB T1-4H 0 -3M1C 0
'Depends on clinical vs. pathologic stage Reler to AJCC Cancel Staging Manual.8th ed. 2017 lor complete TNM classification
Treatment
• options include surgery, radiotherapy, ablation, chemotherapy, and palliative care lor end-stage
disease
• surgery not usually performed for SCLC since it is generally non-curable
• contraindications for surgery
spread to contralateral mediastinal lymph nodes or distant sites
patients with potentially resectable disease must undergo mediastinal node sampling since
CT thorax is not accurate in 20-40% of cases
poor pulmonary status (e.g. unable to tolerate resection of lung)
postoperative estimated l-
'HVi and DLCO must be at least 40% of predicted to tolerate surgery
• chemotherapy (used in combination with other treatments)
• common agents: cisplatin-vinorelbine (standard of care), etoposide, ifosfamide, vincristine,
anthracyclines, paclitaxel. irinotecan, gefitinib (an endothelial growth factor receptor inhibitor)
• pembrolizumab, a HD-1 monoclonal antibody is used in those with tumour PD-l.l levels >50%;
for those with PD-L1 levels <50%, combination of doublet chemotherapy and pembrolizumab is
initiated
r -l
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GS17 General and Thoracic Surgery Toronto Notes 2023
targeted therapiessuch as EGFR tyrosine kinase inhibitors and ALK tyrosine kinase inhibitors
are used if tumourtests positive for these mutations
complications
acute:tumourlysissyndrome,infection,bleeding,myelosuppression, hemorrhagic cystitis
(qxlophosphamide),cardiotoxicitv (doxorubicin),renal toxicity (dsplatin), peripheral
neuropathy (vincristine)
chronic:neurologicdamage,leukemia,additional primary neoplasms
Pleura, Lung, and Mediastinum
• see Respirologv.R23
Hamartomas
• 10% of benign lung lesions
. Composed of tissues normally
present in lung (fat epithelium,
fibrous tissue, and cartilage), but
they exhibit disorganized growth
• Peak incidence is age 60. more
common in men
• Usually peripheral and clinically silent
• CXR shows clustered "popcorn"
pattern of calcification
(pathognomonic for hamartoma)
• Peripheral small hamartomas
can generally be observed with
occasional follow-up to monitor
growth:symptomatic endobronchial
hamartomas are removed via rigid
transbronchial resection
Complicated Parapneumonic Effusion
Definition
• persistent bacteria in the pleural space but fluid is non-purulent
• neutrophils, pleural fluid acidosis ( pH<7.20),low glucose (<40mg/dL)
• often no bacteria grown since rapidly cleared from pleural space
Clinical Features
• fever, pleuritic chest pain,dyspnea, and sputum production
Treatment
• antibiotics depending on Gram stain and culture
• chest tube drainage
Empyema
Definition
• bacteria in pleural space or an effusion with organismsseen on a Gram stain or culture (e.g. pleural
fluid is grossly purulent in advanced stage empyema)
• positive culture is not required for diagnosis
Etiology
• contiguousspread from lung infection (most commonly anaerobes) or infection through chest wall
(e.g.trauma,surgery)
Clinical Features
• fever, pleuritic chest pain,dyspnea,and sputum production
Investigations
• CT chest
• thoracentesis
PMNs (lymphocytesin TB) ± visible organisms on Gram stain
Treatment
• antibiotic therapy for at least -1-6 wk (rarely effective alone)
• complete pleural drainage with chest tube
• if loculated, more difficult to drain - may require surgical drainage with VATS, or fibrinolysis
(surgical or tPA/DNAse) to allow lung re-expansion (decortication)
Pneumothorax
Definition
• presence of air in the pleural space
• can be classified as:
primary orsecondary
open or closed
simple or tension or occult (only visible on CTscan)
Pathophysiology
• entry of air into pleuralspace raisesintrapleural pressure causing partial or complete lung deflation
Etiology
• traumatic:penetrating or non-penetrating chest injuries
• iatrogenic:central venous catheter,thoracentesis,mechanical ventilation with barotrauma,surgery +
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GS18 General and Thoracic Surgery Toronto Notes 2023
•spontaneous: no history of trauma or other underlying cause
• primary (no underlying lung disease)
spontaneous rupture of apical subplcural bleb (pockets of air) of lung into pleural space
smoker, male, family history, Marfan'
ssyndrome
secondary (underlying lung disease)
rupture of subpleural bleb in the pleural space which can migrate along bronchioalveolar
bronchoalveolarsheath to the mediastinum then to the intrapleuralspace
necrosis of lung tissue adjacent to pleuralsurface
pneumonia, abscess, PCP,lung cancer,COPD,CP,TB,lymphangioleiomyomatosis(LAM),
pulmonary Langerhans cell histiocytosis (PLCH),lung metastasis (e.g.sarcoma)
Clinical Features
•can be asymptomatic
•acute-onset pleuritic chest pain, dyspnea
•tachypnea, tachycardia
•tracheal deviation (contralateral deviation in tension pneumothorax)
•shock (in tension pneumothorax)
•ipsilateral diminished chest expansion
•decreased tactile/vocal fremitus
•hyperresonance
•ipsilateral diminished breath sounds
Investigations
•CXR
small:separation of visceral and parietal pleura seen as fine crescentic line parallel to chest wall
at apex
large:decreased density and decreased volume oflung on side of pneumothorax
see Medical Imaging. M14 and M19
Treatment
•primary spontaneous pneumothorax
• stable,small (<3 cm), minimal symptoms:observation + ().
’
• symptomatic or large (>3 cm): aspiration or chest tube
• unstable/tension pneumothorax: needle decompression then chest tube, VATS bullectomy, and
pleurodesis if unsuccessful (25-50%)
•secondary spontaneous pneumothorax
• stable,small (<3 cm),minimal symptoms:observation + 02
symptomatic,large, or unstable: chest tube and VATS pleurodesis with or without bullectomy if
unsuccessful
Tube thoracostomy can be completed
under U/S guidance
Orientation
.fit UIM
Tube Thoracostomy
Indications
• to drain abnormal air or fluid collections in the pleural space
hemothorax, pleural effusion, chylothorax, and empyema
pneumothorax, if:
large or progressive
patient is on mechanical ventilation
bronchopleural fistula
« tension pneumothorax
• to treat symptomatic and/or recurrent pleural effusion
• see Respirology. R23
for long-term drainage of malignant effusions use: 1.Tunneled pleural catheter; 2. Pleural
drainage and Talc pleurodesis
via facilitation of pleurodesis- obliteration of the pleural space by instilling talc or betadine (less
common) to cause fusion of parietal and visceral pleura
Dissection from
inferior ribto
superior rib
Intercostal vessels
and nerves - -
Kelly clamp
riser: or
Complications
• overall complications are rare (1-3%)
• malposition (most common complication), especially by inexperienced operators
tubes may dissect along the external chest wall, or may be placed below the diaphragm
• bleeding (anticoagulation is a relative contraindication)
• local infection, empyema
• perforation of lung parenchyma or vasculature
• risk of re-expansion pulmonary edema when large volumes of air or fluid are drawn off quickly ( >I.O1.5 L)
at superior
pole ol lung
1J
+
Figure 6.Tube thoracostomy
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GS19 General and Thoracic Surgery Toronto Notes 2023
Lung Transplantation
Conditions Leading to Transplantation
• obstructive: chronic acquired lung disease (e.g.COPD),CF,and emphysema due to a-l antitrypsin
deficiency
• restrictive interstitial lung disease: IPF, hypersensitivity pneumonitis
• vascular:idiopathic pulmonary arterial HT'
N (IPAH),secondary pulmonary HTN, and Eisenmenger’
s
syndrome
• other:sarcoidosis, lymphangioleiomyomatosis, and pulmonary Langerhans cell histiocytosis
Clinical Indications
• transplantation should be considered for patients with advanced lung disease refractory to maximal
medical orsurgical therapy
• patients who are symptomatic during activities of daily living and have risk of death >50% over the
next 2 yr
Criteria for Transplantation
• lung allocation score based on:1) post-transplantsurvival measure, and 2) waiting list urgency
measure
• transplant benefit = post-transplant survival (days) - waitlist survival (days)
Absolute Contraindications
• uncontrolled or untreatable pulmonary or extrapulmonary infection
• active TBinfection
• malignancy in the last 2 yr
• dysfunction of vital organs including glomerular filtration rate of <40 mL/min/1.73 m 3,stroke
within 30 d, acute liver failure or cirrhosis, acute coronary syndrome within 30 d or heart disease not
amenable to revascularization, and untreatable hematologic disorders
• active cigarette smoking
• BM1 S35 kg/m 3
• unresolved psychosocial problems or non-adherence to medical therapy
• smoking
• absence ofsocial support system
Relative Contraindications
• ages >70 years and low physiologic reserve
• BM1 30-34.9 kg/m 1
• limited functionalstatusincluding severe malnutrition or osteoporosis
• HIV infection, HBV infection
• alcohol (required to stay within healthy drinking guidelines)
Postoperative Complications
• primary graft dysfunction
• airway anastomotic complications (bronchial necrosis and dehiscence, tracheobronchomalacia,
stenosis)
• chronic lung allograft dysfunction (bronchiolitis obliteranssyndrome and restrictive allograft
syndrome)
• infectious complications (bacterial, fungal,CMV, community-acquired respiratory viruses, and
mycobacteria)
• malignancy (non-melanoma skin cancer, post-transplant lymphoproliferative disorders, colon, breast,
Kaposi’
ssarcoma, and bladder)
Prognosis
• median survival for all adult recipients: 6.5 yr;bilateral transplant survival higher than single (7.6 vs.
4.7 yr, respectively)
. 1 yr survival:COPD > IFF > IPAH
• 10 yr survival:CE, a-l antitrypsin deficiency > IPAH > COPD,IPF
Chronic Obstructive Pulmonary Disease
• see Kespirologv. R9
r t
Treatment
• indicationsforsurgical management
dyspnea despite maximal medical therapy and pulmonary rehabilitation
GT showing hyperinflation and heterogeneously distributed emphysema predominant in the
upper lung zone
may be used as a bridging procedure to lung transplantation
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GS20 General and Thoracic Surgery Toronto Notes 2023
•contraindications
ages >75, cigarette smoking within the prior 6 mo, higher risk ofsurgical mortality (e.g.severe
CAD or HE)
• homogeneously distributed emphysematous changes without areas of preserved lung tissue
severe cachexia or obesity, chest wall deformity, or pulmonary HTN (PA systolic pressure >45
mmHg)
diffusing capacity of lung for carbon monoxide <20% of predicted, PaCOt >60 mmHg, Pa02 <45
mmHg
•surgical procedures
• lung volume reduction surgery: wedge excision of emphysematous tissue
» bilateral or unilateral, thoracotomy or VAT'
S (preferred)
Complications of Treatment
•arrhythmias, pneumonia (may require reintubation and mechanical ventilation), prolonged air leak
from chest tube
Prognosis
•worse early mortality but belter exercise capacity and quality of life with LVRS
Mediastinal Masses
Definition
• mediastinum: bound by the thoracic inlet, diaphragm,sternum, vertebral bodies, and the pleura
• can be broken down into 3compartments: anterior, middle, and posterior
Etiology and Pathophysiology
• diagnosis is aided by location and patient'
s age
• anterior compartment: more likely to be malignant
• “Pour Ts” (see sidebar),lymphadenopathy, lipoma, pericardial cyst, goitre, and ascending aortic
aneurysm thymic tumours/cysts
• middle compartment
pericardial cyst, bronchogenic cyst/tumour,lymphadenopathy, aortic aneurysm
• posterior compartment
neurogenic tumours, meningocele, enteric cysts, lymphadenopathy, diaphragmatic hernias,
esophageal tumours, aortic aneurysm
Differential of an Anterior
Compartment Mass
4Ts
Thymoma
Thyroid enlargement (goitre)
Teratoma
Tumours(lymphoma, parathyroid,
esophageal, angiomatous)
Mediastinal Components
Anterior sternum to pericardium and
great vessels.Includes:thymus, extrapericardial aorta and branches,great
veins,lymphatic tissues
Middle: pericardium (anteriorly),
posterior pericardial reflection,
diaphragm,thoracic inlet Includes:
heart irrtrapericardial great vessels,
trachea
Posterior:posterior pericardial
reflection,posterior border of vertebral
bodies,first rib to the diaphragm.
Includes:esophagus,vagus nerve,
thoracic duct sympathetic chain,
azygous venoussystem
Clinical Features
• 50% asymptomatic (mainly benign); when symptomatic,50% are malignant
• chest pain, cough, dyspnea, recurrent respiratory infections
• hoarseness, dysphagia,Horner’ssyndrome (see sidebar),facial/upper extremity edema (SVC
compression)
• paraneoplastic syndromes (e.g.myasthenia gravis(thymomas))
Investigations
• CXR (compare to previous)
• CT with contrast (anatomic location,density, relation to mediastinal vascularstructures)
• MRI:specifically indicated in the evaluation of neurogenic tumours
• Echo: best for assessment ofstructuresin close proximity to the heart and pericardium
• radionuclide scanning: 1311 (for thyroid), gallium (for lymphoma), PET/CT
• biochemicalstudies: thyroid function,serum calcium, phosphate, PTH, APP, p-hCG, LDH
• biopsy (mediastinoscopy, bronchoscopy, and EBUS, percutaneous needle aspiration)
Management
• excision -symptomatic benign mass that is enlarging or a mass with concerns for malignancy
• resect bronchogenic cysts and localized neurogenic tumours via VAT'
S or open surgery
• diagnostic biopsy rather than major operation if mass is likely to be a lymphoma, germ cell tumour, or
unresectable invasive malignancy
• no biopsy if AEP, p-hCG, LDH elevated - pathognomonic for germ cell tumour
Masaoka Staging System
Stage I:completely encapsulated
Stage II: invasion beyond capsule
Stage III:into another organ
Stage IVa:pleural/pericardial mets
Stage IVb: hematogenous/lymphatic
IMtl
Thymoma
Definition
• rare neoplasms in thymus, located in anterior mediastinum
Epidemiology
• patients between 40 and 60 yr
. M*F
• no known risk factors,strong association with myasthenia gravis and other paraneoplastic syndromes +
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GS21 General and Thoracic Surgery Toronto Notes 2023
Clinical Features
• frequently asymptomatic: incidental finding on imaging
• symptoms related to tumour size and location (chest pain, SOB, cough, and phrenic nerve palsy)
• DDx includes intrathoracic goitre, lymphoma, and other anterior mediastinal tumours(see
Mediastinal Masses,GS20)
Investigations
• CT chest (and/or MR!): assess resectability
• germ cell tumour markers (
P-hCG,a fetoprotein),thyroid function, acetylcholinesterase antibodies
(to rule out myasthenia gravis), and PR'
s
• Masaoka staging system widely used
Treatment
• for patients with resectable disease
surgical resection of the thymoma and the thymus via median sternotomy or VATS depending on
the size
± postoperative radiation based on Masaoka staging
radiation considered forstage 11/111 disease
• for potentially unresectable disease (i.e.invasion into heart and great vessels) or non-surgical patients
definitive or palliative chemo and radiation therapy
• re-evaluation if debulking procedure feasible in situations where preoperative chemo- and radiation
therapy is offered
• common chemotherapy regimens include: I ) cyclophosphamide, doxorubicin, and dsplatin, or 2)
cisplatin and etoposide
Prognosis
• depends upon stage of disease and resectability
• generally slow-growing tumours and have good prognosis
Esophageal Carcinoma
Epidemiology
• M:E=3:1
• onset 50-60 yr
. upper (20-33%), middle (33%), and lower (33-50%)
• main types
• most common worldwide:SCC in upper 2/3of esophagus
most common in Western countries:adenocarcinoma in lower 1/3of esophagus
Risk Factors
. SCC
underlying esophageal disease such asstrictures,diverticula, and achalasia
smoking, alcohol, and hot liquids
more common in Black and Asian populations
• adenocarcinoma
» Barrett’s esophagus (most important),smoking,obesity (increased reilux), and GERL)
• more common in White populations
Clinical Features
• progressive dysphagia (mechanical):first solids then liquids, then saliva
• odynophagia then constant pain
• constitutional symptoms
• regurgitation and aspiration (aspiration pneumonia)
• hematemesis and anemia
• direct, hematogenous, or lymphatic spread
• trachea (coughing), recurrent laryngeal nerves (hoarseness, vocal paralysis), aortic,liver, lung,
bone, celiac, and mediastinal nodes
Investigations and Staging
• barium swallow:shows narrowing -suggestive but not diagnostic
• endoscopic biopsy to assess location, resectability, and confirm diagnosis
• both SCC and adenocarcinoma use TNM staging system but have separate stage groupings according
to histology'
. endoscopic U/S (EUS)
visualize local disease
regional nodal involvement (number of nodes may be more important than location)
• bronchoscopy and laryngoscopy
• rule out airway invasion in tumours of the upper and middle esophagus
• full metastatic workup (CXR, bone scan,CT head,CT chest/abdomen /pelvlx, and Ll’Ts, etc.)
• PET scan more sensitive than CT in detecting metastatic disease
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