Activate Windows

Go to Settings to activate Windows.

G55 Gastroenterology Toronto Notes 2023

Table 27. Common Drugs Prescribed in Gastroenterology

Class Generic Drug Trade Name Dosing

Name

Mechanism of

Action

Indications Contraindications Side Effects

Zofran '

Depends on procedure. Selective 5-HT3 AT caused by cancer

generally 8-16 mg PO receptor antagonist in chemotherapy and

central chemoreceptor radiation therapy;multiple

trigger zone and off label uses,including

peripherally on vagus gastroenteritis N/V

nerve

1mg PO BID (for nausea Same as above

from chemotherapy/

radiation)

Morphine,hypersensitivity Constipation,diarrhea.

increased liver enzymes,

headache,latigue.

malaise,cardiac

dysrhythmia

ondanselton

to drug

Kylril - AiV caused by cancer

chemotherapy and

radiation therapy

Same as above Constipation,prolonged

01interval (rarely)

granisetron

Prokinetic

Agents

Motilium Gl motility disorder (e.g. peripherally acting

gastroparesis):10 mg TID D2 receptor blocker.

main effect in the

upper Gl motility disorders hypersensitivity to cardiac arrhythmia

(eg.gastroparesis. domperidone,prolonged (use lowest dose for

subacute gastritis). 0T interval,prolactinoma. shortest duration) and

upper Gl tract (i.e. prevention of nausea electrolyte disturbances. hyperprolactinemia

increased esophageal associated with dopamine- CYP3A4 inhibitors, causing hypogonadism,

peristalsis,gastric agonists mechanical Gl obstruction or breast engorgement,

motility), antiemetic perforation,Gl hemorrhage, and galactorrhea

properties severe hepatic dysfunction.

children <2yr

domperidone

Resotran'

Motegrity:

2 mg POOD high affinity S-HK

agonist,main effect

in the lower Gl

tract(i.e.increased

colonic peristalsis,

ameliorates

gastroparesis)

hypersensitivity to

prucalopride.Gl obstruction dizziness,abdominal

or perforation,severe pain.N/V,diarrhea,

inflammation co-morbidity abdominal distention

(e.g.Crohn's disease.UC.

tome megacolon)

prucalopride chronic idiopathic headache,fatigue.

constipation

Aminosalicylates mesalamme

(5-ASAs)

Pentasa:

Salofalk '

Asacol'

Mesasal7

CD:1g PO TID.'OID

Active UC:1g PO OID

Maintenance UC:1.6 g

PO divided doses daily prostaglandinsand

also as suppositories and leukotrienes

enemas

3-4 g/d PO in divided

doses

5-ASA:Blocks

arachidonic acid

metabolism to

M id tomoderate UC Hypersensitivity to Abdominal pain,

mesalamine salicylates: constipation,arthralgia.

Asacol'

containsphthalate. headache

potential urogenital

teratogenicity for male fetus

sulfasalazine Salazopynn1 Compound composed Mild tomoderate UC

of 5-ASAbound

to sulfapyridine.

hydrolysis by intestinal

bacteria releases

5-ASA.the active

component

Hypersensitivity to

sulfasalazine, sulfa drugs,

salicylates;intestinal

or urinary obstruction,

porphyria

Rash,loss of appetite.

AY.headache,

oligospermia (reversible)

6-mercaptopurine Purinethol:

(6-MP)

CD:1.5 mg/kg/d PO Immunosuppressive IBD:active inflammation

and tomaintain remission

Immunosuppressive

Agents

Hypersensitivity to

mercaptopurine,

priorresistance to

mercaptopurine or

th.oguanine,history of

treatment with alkylating

agents,hypersensitivity to

azathioprine.pregnancy

Same as above

Pancreatitis,bone

marrow suppression,

increased risk of cancer

azathioprine Azasan IBD:2-3 mgfkg > dPO Same as above Same as above Same as above '

Imuran'

prednisone Induction of remission Anti-inflammatory

for acute exacerbations:

20-40 mg P0 once daily:

taper 2.5-5 mg/wk until

discontinued

Symptomatic moderate to

severe CD and UC

Hypersensitivity to Hyperglycemia,

prednisone,systemic fungal insomnia,osteoporosis,

infections weight gain,increased

risk of infections

Biologies Remicade' 5-10 mg/kg IV over 2 h Medically refractory CD Heart failure,moderate to

severe,doses »5 mg/kg

infliximab Monoclonal antibody

toTNFo

Reported cases of

reactivated TB.PCP.

fymphoma, other

infections

Other THFo share similar

serious sideeffects

Headaches,skin rashes,

upper respiratory tract

infection

Humira! CD induction:four 40 mg

SC on day1.then 80 mg 2

wk later (day 15)

CD maintenance: 40 mg

every other wk beginn ing

day 29

RA:2 mg/kgatwkO.

4.and then every 8 wk

thereafter (use with

methotrexate)

UC induction:200 mg

SC at wkO,then100 mg

at wk 2

UC maintenance:50 mg

every 4 wk

CD/UC:300 mg at0.2.6

wkand then every 8 wk

thereafter

Monoclonal antibody

to TNFa

Medically refractory CD or Hypersensitivity to

poor response to infliximab adalimumab

Severe infection

Moderate-to-severe heart

failure

adalimumab

Simponi:

gotimumab Monoclonal antibody

to TNFa

Active ankylosing

spondylitis

Psoriatic arthritis

Moderate-to-severe

active RA (combined with

methotrexate)

UC:medically relractory UC

Hypersensitivity to

gol mumab or latex

Severe infection

Mpderate-to-severe heart

failure

Medically refractory

CD UC.including other

TNFainhibitors and

corticosteroids

Moderate to severe CD

andUC

vedohzumab Entyvio: Monoclonal antibody

to o4fl7 integrin

Hypersensitivity to

vedolizumab

Infections,

liver injury,and

progressive multifocal

leukoencephalopathy

Infections,headaches,

joint pain.fever,H/V

r m

j

Stelara - Induction:single IV

weight- based dose on

day1

Maintenance:90 mg

subcutaneous injection

every 8 wk

Hypersensitivity to

ustekinumab

ustekinumab Monoclonal antibody

to IgGIK.inhibits

signals by 11-12 and

11-23

+

Activate Windows

Go to Settings to activate WTridows.

G56Gastroenterology Toronto Notes 2023

Table 27. Common Drugs Prescribed in Gastroenterology

Class Generic Drug Trade Name Dosing

Name

Mechanism of

Action

Indications Contraindications Side Effects

Small Molecules tofacitinib S 10 mg BID JAK inhibitor UC IB,hepatitis B Infections,macro'

cardiac events,

thrombosis (e g.PE,DVI)

Xeljanc '

Antibiotics rifaximin Zaxine ' SSO mg BIO or TID Nonabsorbable

antibiotic, affects

dysbiosis of

microbiome

Hepatic encephalopathy Nil

Non-constipation IBS

Traveller's diarrhea

Nil

Landmark Gastroenterology Trials

Trial Name Reference Clinical Trial Details

PEPTIC ULCER DISEASE

Lanccl 2009;374:119-25 Title:Famotidine for the Prevention of Peptic Ulcers and Oesophagitis inPatients Taking low- dose Aspirin (FAMOUS): A Phase III.Randomised.

Double-blind. Placebo- controlled Trial

Purpose:Evaluate the efficacy ol famotidine in the prevention of peptic ulcers and erosive esophagitis.Inpatients receiving low- dose aspirin.

Methods:Patients without erosions or ulcers on upper endoscopy,currently on low dose aspirin,were randomited to lamolidine 20 mg 610

or placebo,(he primary endpoint was development of new stomach ulcers.

Results:At 12 wk,gastric ulcers occurred in 3.4% of famotidinepatients and15% of placebo- matched patients (OR 0.20:95% Cl0.09 to 0.47;

P'0.0002).Duodenal ulcers developed in 0.5% of famotidine patients and 8.5% of placebo patients (OR 0.05:95% Cl 0.01to 0.40:P~0.0045).

Conclusions:Famotidineis effective in the prevention of gastric and duodenal ulcers,and erosive esophagitis in patients taking low-dose

aspirin.

FAMOUS

INFLAMMATORY BOWEL DISEASE

SONIC NEJM 2010:362:1383-95 Title:Infliximab.Azathioprine,or Combination Therapy for Crohn’s Disease

Purpose:Compare the efficacy and safety of infliximab and azathioprine therapy alone or in combination,in patients with CD.

Methods:CD patients who had not undergone previous biologic or immunosuppressive therapy were randomized to infliximab 5 mg/kg IY

infusion or2.5 mgoral azathioprine.or combination therapy of both drugs.

Results:Among patients receiving combination therapy.56.8% were in steroid-free remission, compared with 44.4% of patients receiving

infliximab monotherapy,and 30% receiving azathioprine monotherapy (P<0.001for comparison with combination:P'0.06 for comparison

with infliximab).

Conclusions:Patients' CD treated with infliximab monotherapy or influimab-azalhioprine combination had better corticosteroid-free

remission than azathioprine monotherapy recipients.

Title:A Comparison ol Methotrexate with Placebo for the Maintenance of Remission in Crohn's Disease

Purpose:Evaluate the role of methotrexate inmaintaining remission of CD.

Methods:Patients with chronically active CO who entered remission were randomized to metlioliexate15 mg IM or placebo for 15 wk.Ihe

primary endpoint was rales of remission at wk 40.

Results:At ihe follow- up pciiod ol 40 wk.65% of methotrexate patients werein remission compared to 39% of patients inIhe placebo group

(risk reduction 26.1%;95% Cl 4% to 47.8%;P'0.04). None of the methotrexate patients reported serious adverse events.

Conclusions:Patients with CD in remission saw increased remission rales and fewer relapse treatments at 40 wk.

Title:Adalimumab Induction Therapy for Crohn's Disease Previously treatedwith Infliximab

Purpose:Determine the efficacy of adalimumab insymptomatic CD patients despite infliximab treatment.

Methods:325 adults with moderate-severe active CD were randomized to induction doses of adalimumab 160 mg and 80 mg at 0 and 2 wk

respectively,or time-matched placebo.The primary endpoint was induction of remission at 4 wk.

Results:Remission was achieved at 4 wk in 21% of adalimumab patients compared with 7% of placebo patients (95% Cl 6.7% to 21.6%).

Conclusions:Adalimumab induces remission more frequently than placebo inadult patients with symptomatic CD despite infliximab therapy.

Title:Ustekinumab as Induction and Maintenance Therapy for Ulcerative Colitis

Purpose:Determine the effectiveness of ustekinumab as induction and maintenance therapy in patients with UC.

Methods:961patients with moderate-severe UC were randomized to IY induction ustekinumab (130 mg),or placebo. The primary endpoint

was clinicalremission determinedby the Mayo scale.

Results:Ihe primary endpoint occurred in 15.6% of patients in the intervention group compared with 5.3% of placebo patients (P*0.001). The

incidence of serious adverse events was similar between groups.

Conclusions:Ustekinumab was more effective than placebo for inducing and maintaining remission in patients with moderate lo-sevctc UC.

Title:Vedolizumab versus Adalimumab for Modcrale- to-Severe Ulcerative Colitis

Purpose:Compare efficacy of vedolizumab versus adalimumabinpatients with moderate-severe UC.

Methods:Adults with moderate-severe active UC were randomized to IV infusions of vedolizumab 300 ing or subcutaneous adalimumab 40

mg (total weekly dose 160 mg).Ihe primary outcome was clinicalremission at wk 52 as determined by the Mayo scale.

Results:At wk 52.clinicalremission was observed in 31.3% of vedolizumab patients compared to 22.5% of adalimumab patients (95% Cl 2.5

to 15.0:P-0.006).Steroid- free remission occurred in12.6% ol vedolizumab patients and 21.8% oladalimumab patients (95% Cl18.9 to 0.4).

Conclusions:In patients with moderale-lo-severe UC,vedolizumab wassuperior to adalimumab with respect to achievementof clinical

remission and endoscopic improvement,but nolcorticosteroidfreeclnical remission.

A Comparison of NEJM 2000;342:1627- 32

Methotrexate with Placebo

for theMaintenance of

Remission in Crohn's

Disease

Adalimumab Induction

Therapy for Crohn's

Disease Previously Treated

with Infliximab

Ann Intern Med

2007:146:829 38

UNIFI NEJM 2019:381:1201-14

VARSIIY NEJM 2019:381:1215 26

r i

<- > i

+

Activate Windows

Go to Settings to activate Windows.

G57 Gastroenterology Toronto Notes 2023

Trial Name Reference Clinical Trial Details

LIVER DISEASE

MELD Score as A Predictor Gastroenterology

Of Death in Chronic liver 2003:124:91-96

Oisease

Title:MELD Score as A Predictor 01Death in Chronic liver Disease

Purpose:Assess the capability for the MELD score lo correctly rank potential liver transplant recipients.

Methods:the MELD score was prospectively applied to estimate 3-mo mortality in 3437 adult liver transplant candidates with chronic liver

disease.

Results:Waiting list mortality increased directly in proportion lo the MEID score.Using 3-mo mortality as the endpoint,the ROC curve lor

MEID was 0.83 compared to 0.76 lor the Chlld- Turcotle-Pugli score.

Conclusions:MEID score can be applied lor allocation ol donor livers as it accurately predicts 3-mo mortality inpatients with chronic liver

lailurc.

NEJM 2010:362:1292- Title:tetaprevir lor Previously Treated Chronic HCV Infection

Purpose:Study the efficacy of tetaprevir in patients without a sustained virologic response to pcgmlcrlerontherapy.

Methods:Patients with HCV genotype 1without sustained virologic response topcginlerleron therapy were randomned to one ol lour

tetaprevir and pcginlerleron treatment groups. The primary endpoint was sustained virologic response 24 wk alter the last dose.

Results:Ihe rates ol sustained virologic response in the three tetaprevir groups were significantly higher than the control group rales|14%,

P'0.001.P'

0.001.P'0.02).Discontinuation ol the drugs due to adverse events wasmore frequent in Ihe tetaprevir groups than In the control

group (1S% vs. 4%).

Conclusions:In HCV infected patients m whom initial pcginlerleron therapy failed,retreatment with tetaprevir in combination with

peginterferon andribavirin was mote cllectivc than the latter two atone.

HEJM 2011:364:1196-1206 Title:8oceprevlt lor Untreated Chronic HCV Genotype 11nfection

Purpose:Evaluate virologic response with additional boccprcvir treatment in patients with HCV genotype 1inlection.

Methods:Previously untreated adults with HCV genotype1infection were randomiied lo placebo plus peginlctleton ribavirin or boccprevir

plus peginterleion ribavirin. The primary endpoint was sustained virologic response.

Results:A virologic response was achieved in 40% of group 1.67% in group 2 and 68% in group 3.

Conclusions:Ihe additionolboceprevir to standard therapy ol peginlerleron-ribavirin,compared with standard therapy alone,increased

rales of sustained virologic response in chronically HCV infected adults.

PROVE 3

1303

SPRINT 2

Rifaiimin Treatment in

Hepatic Encephalopathy

NEJM 2010:362:1071-81 Title:Rilaximin Irealment in HepaticEncephalopathy

Purpose:Evaluate the efficacy olrilaximinin the prevention ol hepatic encephalopathy secondary locirrhosis.

Methods:299 patients in remission from recurrent hepatic encephalopathy were randomiied to rilaximin 550 mg SID or placebo lor 6 mo.The

primary endpoint was time lor the first breakthrough episode.

Results:Rilaximin reduced the risk ol a hepatic encephalopathy episode (hazard ratio 0.42:95% Cl 0.28 to 0.64;P'

0.001).A breakthrough

episode occurred in 22.1% of rifaximin-treated patients compared to 45.9% ol placebo patients (hazard ratio 0.5:95% Cl 0.29 to 0.87;

P-0.01). The incidence of adverse events was similar between groups.

Conclusions:The antibiotic rilaximin was successful in maintaining remission from hepatic encephalopathy and reducing hospitalizations.

NEJM 2015:372:1619-28 Title:Prednisolone or Pentoxifylline For Alcoholic Hepatitis

Purpose:To elucidate the benefits olpentoxifylline and prednisolone lor the treatments of severe alcoholic hepatitis.

Methods:Patients with severe alcoholic hepatitis were randomized to one of lour groups:double-matched placebo,prednisolone plus

matched placebo,pentoxifylline plus matched placebo,or prednisolone plus pentoxifylline.The primary endpoint was mortality at 28 d.

Results:Mortality at 28 d was 17% in the first group,14%in the second group,19% in the third group,and13% in the fourth group.At 90 d and

1yt.there were no significant differences between groups.

Conclusions:For alcoholic hepatitis,prednisolone improved survival ata level below statistical significance.Pentoxifylline did not improve

survival.

Prednisolone or

Pentoxifylline For Alcoholic

Hepatitis

References

Angulo P.Primary biliary cirrhosis and primary sclerosing cholangitis.Clin liver Dis1999:3:529-570.

Andreoli T,Carpenter C.Griggs R.et at.Cecil essentials of medicine.5th ed.Philadelphia:WB Saunders Company.2001.

Aranda- Michel J.Giannella R.Acute diarrhea:a practicalreview.Am J Med 1999:106|6):670-676.

Armstrong MJ.Gaunt P. Aithal GP.et al.Liraglutide safety and efficacy in patients with non-alcoholic steatohepatitis (LEAN):a multicentre,double-blind,randomised,placebo-controlled phase 2sludy.Lancet

2016;387:679-90.

Buckingham IJ,BornmanPC.ABC of diseases olliver,pancreas,and biliary system.Acute pancreatitis.BMJ 2001;322:595-598.

Beckingham IJ.Botnman PC.ABC of diseases ol liver,pancreas,and biliary system. Chronic pancreatitis.BMJ 2001;322:660- 663.

Benchimot El.Bernstein CN. 8itlon A. et al.Iheimpactof inflammatory bowel disease in Canada 2018: a scientific report from Ihe Canadian gastro intestinal epidemiology consortium toCrohn'sand Colitis

Canada. J Can Assoc Gastroenterol 2019:2:51-55.

Black RE.Morris 55. Bryce J. Where and why are 10 millionchildren dying every year? lancet 2003:361:2226 2234.

Chalasani N. Younossi 2. Lavine JE.et aL Ihe diagnosis and management of non-alcoholic latty liver disease:practice guideline by the American GastroenterologicalAssociation.Amencan Association for the 5!udy

of Liver Diseases,and American College olGastroenterology. Gastroenterology 2012:142:1592 1609

Caro G.Volta U.Sapoite A.clal.Celiac disease:acomprehensive current review. BMC Med 2019:17:142.

Colorectal cancer screening:recommendation statement fromIhe Canadian task force on preventative health cate.CMAJ 2001;165:206- 208.

Connor BA. CDC Yellow Book 2020 (Internet).Atlanta: Centers for Disease Control and Prevention|U5):2020. Chapter 2.Preparing International Travelers.Tiavelets'Diarrhea. Available from: https://wwwnc.cdc.

gov/travel/yeltowbook/2D20/preparing intctnationattiavelers/lravelers'diairhea.

Crockett 50. Wani 5.Gardner IB. cl al.American Gastroenterological Association Institute Guideline In Initial Management of Acute Pancreatitis.Gastroenterology 2018:154:1096-1101.

Custis K. Common biliary tract disorders.ClinEarn Pract 20002:141 154.

DeBarros J,Rosas L.Cohen J.ct al.The changingpaiadigm lor Ihelicalmenl of colonic hemorrhage: supersetective angiographic embolization.Dis Colon Rectum. 2002:45(6):802-8D8.

Devault KR.Castclt DO.Guidelines for the diagnoses and treatment of gastroesophagealreflux disease. Arch Intern Med 1995:115:2165-2173.

Diehl AM.Alcoholic liver disease.Clinliver Dis 1998:2:103-118.

OiPalma JA. Management of severe gastroesophageal reflux disease.J Clin Gastroenterol 2001;32:19-26.

Donowili M. KokkeFI. 5aidi R. Evaluation of patients withchronic diarrhea.NEJM 1995;332:725-729.

Drossma DA. The functional gastrointestinal disorders and the Rome IIIprocess. Gastroenterology 2006:130:1377-1390.

Feldman M.Friedman15.5letscnger MH.Gastrointestinal and liver disease:pathophysiology,diagnosis, management. 7lh ed.,vol. 2.Philadelphia:WB 5aunders Company.2004.

Fine K0.Nelson AC. Ellington RT.etal.Comparison of the color of fecaf blood with the anatomical location of gastrointestinal bleeding lesions:potential misdiagnosis using only flexible sigmoidoscopy foi bright

red blood per rectum.Am J Gastroenterol.1999;94|11):3202-3210.

Forrest JA,Finlayson ND.Shearman 0J.Endoscopy in gastrointestinal bleeding,lancet 1974:2:394 397.

Gardner T.Adler D.Forsmark C.etal.American College of Gastroenterology Guidelines.Chronic Pancreatitis. Am J Gastroenterol 202:115:322-339.

Ghosh 5.Shand A.Ulcerative colitis.BMJ 2000:3204119-1123.

Grover SA,BarkunAN.Sackett Dl.Does this patienthave splenomegaly? JAMA 1993:270:2218-2221.

Hanauer SB.Drug therapy:inflammatory bowel disease.NEJM 1996:334:841-848.

Harris JB. LaRocque RC.Oadri F.et al.Cholera.Lancet 2012:379:2466-2476.

Hatchette IF.Farina 0.Infectious diarrhea:when to testand when to treat.CMAJ 2011:183:339-344.

Haubrich WS,Schaffner F,Berk JE.Bockus gastroenterology.5th ed..vol 4.Philadelphia:WB Saunders Company.1995. Chapter 74,Pregnancy-related hepatic and gastrointestinal disorders:p.1448-58.

Haubrich WS,Schaffner F.Berk JE.Bockus gastroenterology.5th ed..vol 4.Philadelphia: WB Saunders Company.1995.Chapter 184,Pregnancy and the gastrointestinal trad.p.3446-52.

Horwiti BJ.Fisher RS.Current concepts:the irritable bowel syndrome.NEJM 2001;344:1846-1850.

r i

L J

+

Activate Windows

T5o to Settings to activate Windows.

058 Gastroenterology Toronto Notes 2023

Howden CW.Hunt RH.Guidelines lor the management ol Helicobacter pylori infection.Am J Gastroenterol 1998;93:2330-2338.

Hunt RH,Fallone CA,Thomson ABR.Canadian Helicobacter pylori consensus conference update:infectioninadults. J Gastroenterol1999:13:213-216.

Jennings JSR.Howdle PD.Celiac disease.Curt Opin Gastroen 2001;17:118-126.

Jensen DM.Machicado GA. Jutabha R.et at Urgent colonoscopy for the diagnosis and treatmentof severe diverticular hemorrhage.N Engl J Med 2000;342(2):78-82.

Jostins L,RipkeS,Weersma RK,et at Host-microbe interactions have shaped the genetic architecture of inflammatory bowel disease.Nature 2012;491:119-124.

Kitchens JM.Does this patient have an alcohol problem? JAMA 1994;272:1782-1787.

Kohli A.Shaffer A.Sherman A,et at Treatment of hepatitis C:a systematic review.JAMA 2014:312:631-640.

lainel,Peterson WL. Bleeding peptic ulcer.NEJM 1994;331:717-727.

lainel.Sahota A,Shah A.Does capsule endoscopy improve outcomes in obscure gastrointestinal bleeding? Randonured trial vs. dedicated small bowelradiography.Gastroenterology 2010;138:1673-1680.

lania FI. A guideline for the treatment andprevention of NSAID induced ulcer.Am JGastroenterol1998:93:2037-2046.

Liu J2.van Sommeren S.Huang H. et at Association analyses identify 38 susceptibility loci lor inflammatory bowel disease andhightight shaicd genetic risk across populations.NatGenel. 2016:47:979 986.

Malik AH. Acute and chronlcviral hepatitis.Clin Fam Pract 2000:2:35 67.

Matheny SC.Kingery JE. Hepatitis A.Am Fam Physician 2012:86:1027-1034.

McClave SA,DiBaise JK.Mullin GE,et at AmericanCollege ol Gastroenterology Clinical Guideline:Nutrition Therapy in theAdult Hospitalized Patient Am JGastroenterol 2016:111:315-334.

McColl KE.Clinical practice helicobacter pylori infection.NEJM 2010:362:1597-601.

McCrea Gt.Miaskowski C,Stotts NA.etal.A review of the literature on gender and age differences in the prevalence and characteristicsolconstipation in North America.J Pain Symptom Manage 2009:37:737-

745.

Meyers MA.Alonso DR,Gray GE, et atPathogenesis of bleeding colonic diverticulosis.Gastroenterology.1976:71(4|:577-583.

Moayyedi PM.Lacy 8ME,Andrews CN.et at ACG and CAG clinical guideline:management of dyspepsia.Am J Gastroenterol 2017;112:988-1013.

Moayyedi P.Andrews CN. MacOueen G. et al.Canadian Association of Gastroenterology ClinicalPractice Guideline for the Management olIrritable Bowel Syndrome (IBS).J Can Assoc Gastroenterol 2019:2:6-29.

Naylor CD.Physical exam of the liver.JAMA1994:271:1859-1865.

Patil M.Sheth KA.Krishnamurthy AC.et at A renewandcurrent perspective on Wilson disease.J Clin Exp Hepatol 2013:3:321-36.

Peck RM.Baser MJ. Pathophysiology of Helicobacter pylotl-induced gastribs andpeptic ulcer disease. Am J Med1997:102:200-207.

Pimentel M.leinbo A,Chey W0, et at Rilanmin therapy foi patients with irritable bowel syndrome without constipation. NEJM 2011:364:22- 32.

Remus JF.BrandiIJ.Vascular ectasias and diverticulosis. Common causes of lower intestinal bleeding.GastroenterolClin N.1994:23|1):1-20.

Reynolds T.Ascites.Clin Liver Dis 2000:4:151 168.

Riddle MS,DuPont HL. Connor BA.ACGCImical Guideline:Diagnosis, Treatment,andPrevention of Acute Diarrheal Infections in Adults:Am. J.Gastroenterol 2016;111:602-622.

Rubio-Tapia A.HillID. Kelly CP.et al.ACG clinical guidelines:Diagnosis and management of celiac disease. Am JGastroenterol 2013;108:656-676.

Runyon BA. Montano AA,Akriviadis EA.et al.Theserum-ascites albumin gradient is superior to the exudate-transudate concept in the differential diagnosis of ascites.Ann Intern Med1992;117:215-20.

Salcedo JA,Al-Kavras F.Treatment of helicobacler pylori infection.Arch Intern Med1998:158:842-851.

Sandbom WJ.Feagan BG,Fedorak RN.et al.Ustekinumab Crohn’s Disease Study Group.A randomized trial of Ustekinumab,a humaninterleukin-12723 monoclonal antibody,in patients with moderate-to-severe

Crohn's disease.Gastroenterology 2008:135:1130-41.

Sands BE.Sandbom WJ.Panaccione R.etal.Ustekinumabas induction andmaintenance therapy for ulcerative colitis.NEJM 2019:381:1201-14.

Sandowski SA. Cirrhosis.Clin Fam Pract 2000:2:59- 77.

Schmid CK.Whitting G.Cory 0,et al.Omeprazole plus antibiotics m the eradication of Helicobacter pylori infection:a meta regression analysis of randomized,controlled trials.Am J Thor 1999:6:25-36.

Shaheen NJ.Weinberg OS. Dcnberg ID.etal.Upper endoscopy lor gastroesophagealreflux disease: best practiceadvice fromthe clinical guidelines committee of the AmericanCollege of Physicians.Ann Intern

Med 2012:167:808 816.

Shaima P.Sarin SK. Improved survival with the patients with variccal bleed.Int J Hepatol 2011:2011.

Sherman M.Chronic viral hepatitis and chronic liver disease.Can J Diag 2001;18:81-90.

Soli AH.Practice parameters: committee of theAmerican College of Gastroenterology:medical treatmentof peptic ulcer disease.JAMA1996:275:622-629.

Slernby B.O’BrienJF,Zinsmeister AR. elal.What is the best biochemical test todiagnose acute pancreatitis? Aprospective clinical study.MayoClinProc1996;71:1138-1144.

SlemliebL Wilson’s disease.Clin Liver Dis 2000:4:229-239.

Thijs JC.van Zwet AA,Thijs WJ.et al.Diagnostic tests for Helicobacter pylori:a prospective evaluation of their accuracy,without selecting a single test as the gold standard.Am J Gastroenterol1996;91:2125-2129.

Turgeon DK.fritsche TR.Laboratory approaches to infectious diarrhea.GastroenterolClin N 2001:30|3|:693-707.

Verbeek RE. vanOijen MG. tenKate FJ.etal.Surveillance and follow-up strategies in patients withhigh-grade dysplasia in Barrett's esophagus:a Dutch population- based study.Am J Gastroenterol 2012:107:534-

Wang KK,Sampliner RE.Updated guideIines 2008 (or the diagnosis,surveillance andtherapy ol Barrett's esophagus. Am JGastroenterol 2008:103:788- 797.

Wilcox CM. Karowe MW.Esophageal infections: etiology,diagnosis, andmanagement.Gastroenterology 1994;2:188- 206.

Wilkins1.Pepilone C. Alex B.et al.Diagnosis and Management of IBS in Adults.Am Fam Physician 2012:86:419 426.

Williams JW. Simel 01. Does this patient have ascites? How todlvinc fluid in the abdomen. JAMA 1992:267:2645 2648.

Wong SK.Ho YH.leong AP. etal.Clinical behavior ol complicatedright-sided andfelt-sided diverticulosis.Dis Colon Rectum 1997;40|3):344-348.

Yapp TR.Hemochromatosis. Clin Liver Ois 2000:4:211 228.

Yu AS,Hu K0.Management of ascites.Clin trver Dis 2001:5:641- 568.

ZuccaroGJr.Management of theadultpatient with acute lower gastrointestinal bleeding.American College olGastroenterology.PracticeParameters Committee.Am JGastroenterol1998;93(8):1202-1208.

542

r -i

+

Activate Windows

Go toGettingsto activate Windows.

General and Thoracic Surgery

Ryan Daniel,Jacqueline Lim, and Smruthi Ramesh, chapter editors

Vrati M.Mehra and Chunyi Christie Tan, associate editors

Arjan S. Dhoot, HBM editors

Dr. Abdullah Behzadi, Dr. Sayf Gazala, Dr.Jesse Pasternak, and Dr. Faycz Quercshy,staff editors

Acronyms

Basic Anatomy Review

Differential Diagnoses of Common Presentations,

Acute Abdominal Pain

Abdominal Mass

Gastrointestinal Bleeding

Jaundice

Preoperative Preparations

Surgical Complications

Postoperative Fever

Wound/Incisional Complications

Urinary and Renal Complications

Postoperative Dyspnea

Respiratory Complications

Cardiac Complications

Intra-Abdominal Abscess

Paralytic Ileus

Delirium

Thoracic and Foregut Surgery

Approach to the Solitary Pulmonary Nodule

Lung Cancer

Pleura,Lung,and Mediastinum

Complicated Parapneumonic Effusion

Empyema

Pneumothorax

Tube Thoracostomy

Lung Transplantation

Chronic Obstructive Pulmonary Disease

Mediastinal Masses

Thymoma

Esophageal Carcinoma

Esophageal Perforation

Hiatus Hernia

Achalasia

Stomach and Duodenum

Peptic Ulcer Disease

Gastric Carcinoma

Gastrointestinal Stromal Tumour

Bariatric Surgery

SMALL INTESTINE

Small BowelObstruction

Mechanical Small Bowel Obstruction

Paralytic Ileus

Intestinal Ischemia

Tumours of SmallIntestine

Short Gut Syndrome

Abdominal Flernia

Groin Hernias

Appendix.

Appendicitis

Inflammatory Bowel Disease

Crohn's Disease

UlcerativeColitis

URGE INTESTINE

Large BowelObstruction.

Mechanical Large Bowel Obstruction

Functional Large Bowel Obstruction:Colonic Pseudo-Obstruction

(Ogilvie’s Syndrome)

GS2 Diverticular Disease

Diverticulosis

Diverticulitis

Colorectal Neoplasms

Colorectal Polyps

Familial Colon Cancer Syndromes

Colorectal Carcinoma

Other Conditions of theLarge Intestine

Angiodysplasia

Volvulus

Toxic Megacolon

Fistula

Stomas

Anorectum

Hemorrhoids

Anal Fissures

Anorectal Abscess

Fistula-In-Ano

Pilonidal Disease

Rectal Prolapse

Anal Neoplasms

Liver.

Liver Cysts

Liver Abscesses

Neoplasms

Liver Transplantation

Biliary Tract

Cholelithiasis

Biliary Colic

Acute Cholecystitis

Acalculous Cholecystitis

Choledocholithiasis

Acute Cholangitis

Gallstone Ileus

Carcinoma of the Gallbladder

Cholangiocarcinoma

Pancreas

Acute Pancreatitis

Chronic Pancreatitis

Pancreatic Cancer

Spleen

Splenic Trauma

Splenectomy

Splenic Infarct

Breast

Benign Breast Lesions

Breast Cancer

Surgical Endocrinology.

Thyroid and Parathyroid

Adrenal Gland

Pancreas

Paediatric Surgery

Skin Lesions

Common Medications

Landmark General and Thoracic Surgery Trials..

References

GS39

GS2

GS4

GS41

.GS44 GS7

GS8

GS47

GS13

GS51

.GS55

GS25

GS60

.GS29

GS63 GS29

GS65

GS33

GS71

GS35

GS36 GS73

GS75

GS37 GS76 ri

L J

GS37 GS77

GS78

+

GS1 General and Thoracic Surgery Toronto Notes 2023

Activate Windows

Go To Settings re activate Windows.

GS2 General and Thoracic Surgery Toronto Notes 2023

Acronyms

5-FU 5-fluorouracil

AAA abdominal aortic aneurysm

ABG arterial blood gas

ABI ankle brachial index

ALNO axillary lymph node dissection

APR abdominoperineal resection

ARDS acute respiratory distress

syndrome

ATN acute tubular necrosis

AXR abdominal x-ray

BRBPR bright ted blood per rectum

BCS breast conserving surgery

CBD common bile duct

CEA carcinocmbryonic antigen

CF cystic fibrosis

CHD common hepatic duct

CRC colorectal cancer

CVA costovertebral angle

CVP central venous pressure

DCIS ductal carcinoma insitu

DIC disseminated intravascular

coagulation

DPI diagnostic peritoneal lavage

DRE digital rectal exam

EBL estimated blood loss

ERCP endoscopic retrograde

cholangiopancreatography

LCIS lobular carcinoma in situ

LES lower esophageal sphincter

lower gastrointestinal bleed

left lower quadrant

IMWH low molecular weight heparin

LUO left upper quadrant

LVRS lung volume reduction surgery

MALL mucosa-associated lymphoid

tissue

mechanical bowelpreparation

MEN multiple endocrine neoplasia

MIBG motalodobcnzylguanidino

MIS minimally invasive surgery

MRCP magnetic resonance

cholangiopancreatography

MSAFP maternal scrum a- fctoprotcin

NET neuroendocrine tumour

normal saline

OCP oral contraceptive pill

OGD oesophagogastroduodenoscopy URTI

PMN polymorphonuclear neutrophils VATS

POD postoperative day

proton pump inhibitor

PTC percutaneous transhepatic

cholangiography

partial thromboplastin time

PUD peptic ulcer disease

EUA examination under anesthesia

EUS endoscopic ultrasound

FAP familial adenomatous polyposis LGIB

FAST focused abdominal sonography LLO

for trauma

FNA fine needle aspiration

FNH focal nodular hyperplasia

FOBT fecal occult blood test

GERD gastroesophageal reflux disease

GIST gastrointestinal stromal tumour MBP

GU genitourinary

HCC hepatocellular carcinoma

HDGC hereditary diffuse gastric

carcinoma

RAI radioactive iodine

Ringer’s lactate

RIO right lower quadrant

RUO right upper quadrant

SBO small bowel obstruction

SBFT small bowel follow-through

SCC squamous cell carcinoma

SIADH syndrome of inappropriate

anti-diuretic hormone

SMA superior mesenteric artery

SMV superior mesenteric vein

SNLB sentinel lymph node biopsy

TED thromboembolic deterrent

TEE transesophageal

echocardiogram

TTE transthoracic echocardiogram

ulcerative colitis

UGI upper gastrointestinal series

UGIB upper gastrointestinal bleed

upper respiratory tract infection

video-assisted thoracoscopic

surgery

vasoactive intestinal peptide

VTE venous thromboembolism

RL

HIDA hepatobiliary imino diacetic acid

HNPCC hereditary nonpolyposis

colorectal cancer

ISO incision and drainage

IBD inflammatory bowel disease

IPAH idiopathic pulmonary arterial

hypertension

UC

NS

IPF idiopathic pulmonary fibrosis

intrauterine growth restriction

inferior vena cava

IUGR PPI VIP

IVC

IVIG intravenous immune globulin

low anterior resection

large bowel obstruction

LAR PTT

LBO

Basic Anatomy Review

Access to RUQor LUQ contents

i.e. gallbladder,spleen

Kocher’s

(subcostal)

Upper Midline Access to stomach,duodenum,

gallbladder,liver,transverse colon Kocher's

(subcostal)

04

Paramedian Can make similar incision in each

quadrantfor access to eachquadrant's §

contents

Postoperative ventral hernias common s

Not commonly used =

Lateral At outer 1/3 - medial 2/3 border of rectus s

Paramedian Modification of paramedianbutwith

lower risk of dehiscence or ventral hernia s

'

Not commonly used

Lower Midline Access to pelvic organs,sigmoid

colon,and rectum

Suprapubic incision for access to

pelvic cavity

McBurney’s Access to appendix,other RLQ and

LLQ contents

Paramedian

Lateral

paramedian

McBumey's

o

Upper midline

Lower midline

I

Arcuate line

2

Pfannenstiel Pfannenstiel |

3u

©

Figure 1. Abdominal incisions

Lateral Abdominal Wall Layers and their Continuous Spermatic and Scrotal Structures

(superficial to deep)

1. skin (epidermis, dermis,subcutaneous fat)

2. superficial fascia

• Campers fascia (fatty) > Dartos muscle/fascia

• Scarpa'

s fascia (membranous) > Colles'

superficial perineal fascia

3. muscle (see figure 2 and figure 3)

• external oblique > inguinal ligament > external spermatic fascia

• internal oblique > cremasteric muscle/fascia

• transversus abdominis > posterior inguinal wall

4. transversalis fascia > internal spermatic fascia

5. preperitoneal fat

6. peritoneum > tunica vaginalis

Midline Abdominal Wall Layers (superficial to deep)

1. skin

2. superficial fascia

3. rectus abdominis muscle:in rectussheath, divided by linea alba (see figure 3)

• above arcuate line (midway between symphysis pubis and umbilicus)

anterior rectus sheath = external oblique aponeurosis and anterior leaf of internal oblique

aponeurosis

posterior rectussheath = posterior leaf of internal oblique aponeurosis and transversus

abdominis aponeurosis

• below arcuate line

aponeuroses of external oblique, internal oblique, and transversus abdominis all pass in front

of rectus abdominis

r i

L J

+

Activate Windows

Go to Settings to activate Windows.

GS3 General and Thoracic Surgery Toronto Notes 2023

4. arteries:superior epigastric (branch of internal thoracic), inferior epigastric (branch of external iliac);

both arteries anastomose and lie behind the rectus muscle (superficial to posterior rectus sheath

above arcuate line)

5. transversalis fascia

6. peritoneum

Transversus abdominismuscle

Internal oblique muscle I

I

Peritoneum i

IC I

artery

-Inferior epigastric

^

vein

“

—Transversalis fascia

5 Deepinguinalnng

_ Membranous layer

of superficial fascia

(Scarpa's fascial

-External oblique muscle

-Internal oblique muscle

-Aponeurosis of internal

oblique muscle

-Aponeurosis of external

oblique muscle (cut edge)

Cremaster muscle

-Spermatic cord

Fatty layer of superficial fascia

(Camper's fascial

Superficial inguinalnng

Tunica vaginalis

Tesos

Internal spermatic fascia

Cremaster muscle

External spermatic fascia

Code's superficialpenneal fascia

Dartos muscle

Skin of scrotum

Figure 2. Continuity of the abdominal wall with layers of the scrotum and spermatic cord

Rectus Skin abdominis Above arcuate line Superficial fascia

(Camper'

s +Scarpa’

s fascial

External oblique

Internal oblique

Transversus abdominis

Transversalis fascia

Preperitoneal fat

Peritoneum

)

Below arcuate line Inferior epigastric artery

Skin

Superficial fascia

Externaloblique

Internal oblique

Transversus abdominis

Transversalis fascia

Preperitoneal fat

Peritoneum

5

J Organ Arterial Blood Supply

S

Lell andright hepatic

(branches of hepatic proper)

Splenic

Cystic (branch of right hepatic)

1. Lesser curvature:right and

left gastric

2. Greater curvature:right

(branch of gastroduodenal)

and left (branch of splenic)

gastroepiploic

3. Fundus:short gastnes

(branches of splenic)

1. Gastroduodenal

2. Pancreaticoduodenal

(superior branch of

gastroduodenal,inferior

branch of superior

mesenteric)

1. Pancreabc branches of

splenic

2. Pancreabcoduodenai5

Superior mesenteric branches:

jejunal,ileal,ileocolic

1. Superior mesenteric

branches:right colic,

middle colic

2. Inferior mesenteric

branches:left colic,

sigmoid,superior rectal

1 liver

V

Spleen

Gallbladder

Figure 3.Midline cross-section of abdominal wall

Stomach

Celiac trunk (1)

i) Common hepatic artery (2)

•Hepatic proper (3)

-left hepatic artery (4)

-Right hepatic artery (5)

•Right gastric artery (7)

•Gastroduodenal artery (81

ii) left gastric artery (6)

iii) Splenic artery (9)

Duodenum

Superior mesenteric artery (10)

i) Middle colic artery (11)

ii) Right colic artery (121

iii) Ileocolic artery (13)

iv) Ileal and jejunal branches 114)

Pancreas

Small

Inferior mesenteric artery (15)

il Left colic artery (16)

iilSigmoid arteries (17)

ii)Superior rectal artery (181

intestine

Large

intestine

5

+ ,Z

-

Figure 4. Arterial blood supply to the Gl tract

Activate Windows

rcr terSettings to activate Windows.

GS4 General and Thoracic Surgery Toronto Notes 2023

Venous Flow

Portal vein (II

Superior mesenteric vein (7)

i) Ileal and jejunal veins(131

ill Ileocolic vein (141

iiil Right colic vein (121

hr) Middle colic vein (II)

v) Pancreaticoduodenal vein (8)

vi) Right gastroepiploic vein (9)

Splenic vein (51

i) I nferior mesenteric vein (10)

(superior rectal vein until crossing

common iliac vessels)

•Left colic veins (15)

•Sigmoid veins (16)

•Superior rectal veins(17)

ii) Pancreatic veins

ml Left gastroepiploic vein

hr) Short gastric veins(6)

Left gastric (coronary) vein (2)

Right gastric vein (3)

Cystic vein (4)

Paraumbilical vein-(within round ligament, notshown) <3

a

a

|

-

?

9

Figure 5. Venousdrainage of the Gl tract

Differential Diagnoses of Common

Presentations

In All Patients Presenting with an Acute

Abdomen.Order the Following:

Ifcy Testsfor Specific Diagnosis

. ALP.ALT.AST. bilirubin

• Lipase/ amylase

• Urinalysis

• R-hCG (in women of childbearing Acute Abdominal Pain age)

• Troponins

• Lactate

Key Testsfor OR Preparation

• CBC.electrolytes, creatinine,glucose

. INR/PTT

• CXR (if history of cardiac or

pulmonary disease)

• ECG if clinically indicated by history

or if >69 yr and no risk factors

Note:Choosing Wisely does not

recommend routine preoperative blood

work for ambulatory/elective surgery

• acute abdomen = severe abdominal pain of acute onset and requires urgent medical attention

• in patients with acute abdominal pain, the first diagnoses that you should consider are those requiring

potential urgent surgical intervention,including:

peritonitis

bowel obstruction

Table 1. Differential Diagnosis of Acute Abdominal Pain

Right Upper Quadrant (RUO) Right Lower Quadrant (RLO)

Hepatobiliary

Biliary colic

Cholecystitis"

Cholangitis

CBD obstruction (e.g.stone, tumour)

Hepatitis (includes perihepatitis'

f itr Hugh Curtissyndrome)

Portal vein thrombosis

Budd -Chiari syndrome

Hepatic abscess(mass

Right subphrenic abscess*

Gastrointestinal

Pancreatitis

Presentation of gastric,duodenal,or pancreatic pathology

Hepatic flexure pathology (e.g. CRC.subcostal incisional hernia)

Genitourinary

Nephrolithiasis’

Pyelonephritis

Renal: mass,ischemia, trauma

Cardiopulmonary

Right lower lobe pneumonia

Effusion/empyema

CHF (causing hepatic congestion and right pleural effusion)

Gastrointestinal

Appendicitis"

Crohn'

s disease

Tuberculosis of the ileocecal junction

Cecal tumour

Intussusception

Mesenteric lymphadenitis(Yersinia)

Cecal diverticulitis

Cecal volvulus'

Hernia:femoral,inguinal obstruction.Amyand'

s(and

resulting cecal distention)

Gynaecological

See'suprapubic'

Genitourinary

See 'suprapubic'

Extraperitoneal

Abdominal wall hematoma,abscess

Psoas abscess

Types of Peritonitis

• Primary peritonitis:spontaneous

without dear etiology

• Secondary peritonitis:due to a

perforated viseus

• Tertiary peritonitis: recurrent

secondary peritonitis more often with

resistant organisms

Localization of Pain

• Most digestive tract pain is perceived

in the midline because of bilaterally

symmetric innervation:kidney, ureter,

ovary,or somatically innervated

structures are more likely to cause

lateralized pain

• Parietal peritoneum:supplied by

somatic sensory nerves of body wall.

Pain is sharp and well-localized

• Visceral peritoneum:supplied by

autonomic sensory fibres. Pain is

colicky and poorly localized

Ml r T

i J

Pericarditis

Pleurilis

Miscellaneous

Herpes roster

Trauma

Costochondritis(Infectious*

)

"indicated need tor urgentsurgical evaluation

+

Activate Windows

Go to Settings to activate Windows.

GS5 General and Thoracic Surgery Toronto Notes 2023

Table 1. Differential Diagnosis of Acute Abdominal Pain

Left Upper Quadrant (LUO) Left Lower Quadrant (LLO)

Referred Pain

• Biliary colic to right shoulder or

scapula

. Renal coSc to groin

• Appendicitis:periumbilicalto RLQ

• Pancreatitis:to back

• Ruptured AAA:to back or flank

• Perforated ulcer to RLO (right

paracolic gutter)

• Hip pain:to groin

• Ovarian torsion:to flank or groin

Pancreatic

Pancreatitis (acute»s.chronic)

Pancreatic pseudocyst

Pancreatic tumours'

Gastrointestinal

Gastritis

Gastrointestinal

Diverticulitis*

Diverticulosis

Colorsigmodrectal cancer

fecal impaction

Proctitis (e.g.UC.infectious:

i.e.gonococcus or Cbbmydio)

Sigmoid votvulus*

Hernia (mcarceraledslrangulaled*)

Gynaecological

See 'suprapubic'

Genitourinary

See 'suprapubic'

Extraperitoneal

Abdominal wall hematoma/abscess'

Psoas abscess

PUD

Splenic flexure pathology

(e.g.CRC.ischemia)

Splenic

Splenic infarcllabscess*

Splenomegaly

Splenic rupture'

Splenic artery aneurysm

Cardiopulmonary (see RUOand Epigastric)

Genitourinary (see DUO) Most Common Presentations of

Surgical Pain

• Sudden onset with rigid abdomen “

perforated visors

• Pain out of proportiontophysical

findings -ischemic bowel

• Vague pain that subsequently

localizes ~ appendicitis or other intraabdominal process that imitates the

parietal peritoneum

• Waves of colicky pain - bowel

obstruction

SeeG»nae::.CTi.Urslinv.Respiroloav,and Cardiology and

Cardiac Surgery for further details regarding respective

etiologies of acute abdominal pain

EPIGASTRIC SUPRAPUBIC DIFFUSE

Cardiac

Aortic dissechonruplured AAA'

Gastrointestinal (see RL0/LL0)

Acute appendicitis*

Gastrointestinal

Peritonitis*

Early appendicitis,perforated appendicitis*

Mesenteric ischemia*

Gasboenteritisi'colitis

Constipation

Bowel obstruction*

Pancreatitis

Ml IBO

Pericarditis

Gastrointestinal

Gastritis

GERD esopha;;s

Gynaecological

Ectopic pregnancy*

Pelvic inflammatory disease

Endometriosis

Threatened/incomplete abortion*

Hydrosalpinx/salpingitis

Ovarian torsion*

Hemorrhagic fibroid

Tubo-ovarian abscess

Gynaecological lumours

Genitourinary

Cystitis (infectious,hemorrhagic)

Hydroureter/urinary colic

Epididymitis

Testicular torsion*

Acute urinary retention

Extraperitoneal

Rectus sheath hematoma

PUD

Pancreabtrs

Malloty-Weiss tear

IBD

Irritable bowel syndrome Acute Abdominal Pain Mnemonic

Ogilvie'

s syndrome

Cardiovascular,Hematological

Aortic dissection*

Ruptured AAA*

Sidde cellcrisis

Genitourinary.Gynaecological

Perforated ectopic pregnancy*

Pehric inflammatory disease

Acute urinary retention

Endocrinological

Carcinoid syndrome*

Diabetic ketoacidosis

Addisonian crisis

Hypercalcemia

Other

lead poisoning

Tertiary syphilis

ABDOMINAL

Appendicitis

Biliary tract disease

Diverticulitis

Ovarian disease

Malignancy

Intestinal obstruction

Nephritic disorders

Acute pancreatitis

Liquor/ethanol

’indicated need tor urgent surgical evaluation

Abdominal Mass

Table 2. Differential Diagnosis of Abdominal Mass

RUO Upper Midline LUO

Gallbladder:cholecystitis,

cholangiocarcinoma,peri-ampullary

malignancy,cholelithiasis

Biliary tract Klatskin tumour

Liver:hepatomegaly,hepatitis,abscess.

Pancreas:pancreaticadenocarcinoma,other Spleeo:splenomegaly,tumour,abscess,

pancreatic neoplasms,pseudocyst subcapsular splenic hemorrhage,can also

present as RLO mass if extreme splenomegaly

Stomach:tumour

Abdominal aorta:AAA (pulsatile)

Gl:gastric tumour (adenocarcinoma,

gaslrointestinal stromal tumour,carcinoid

tumour (hepatocellular carcinoma,metastatic tumour). MALT lymphoma

tumour,etc.)

Pancreatitis can look like a surgical

abdomen,but is rarely an indication for

immediate surgical intervention

RLO Lower Midline LLO

Intestine:stool,tumour (CRC).mesenteric Uterus:pregnancy,leiomyoma (fibroid).

adenitis,appendicitis,appendicealphlegmon uterine cancer,pyometra.hematometra

or other abscess,typhlitis,intussusception. GU:bladder dislention,tumour

Crohn's inflammation

Ovary:ectopic pregnancy,cyst

(physiological vs.pathological),tumour

(serous,mucinous,struma ovarii,germ

cell.Krukenberg)

Fallopian tube:ectopic pregnancy,

tubo-ovarian abscess,hydrosalpinx,tumour

Intestine:stool,tumour,abscess (see RLO)

Ovary:see RLO

Fallopian tube:see RLO

rt

lJ

+

Activate Windows

Go TO Ser ctivate Windows.

GS6 General and Thoracic Surgery Toronto Notes 2023

Gastrointestinal Bleeding

• see Gastroenterology. G28 and G30

Indications for Surgery

• failure of medical management (after at least 2 endoscopic attempts at management)

• exsanguinating hemorrhage: hemodynamic instability despite vigorous resuscitation

• recurrent hemorrhage with up to two attempts of endoscopic hemostasis

• prolonged bleeding with transfusion requirement >3 units

• bleeding at rate >1 unit/8h

Indications for Urgent Operation

IHOP

Isc hernia

Hemorrhage

Obstruction

Perforation

Surgical Management of Gl Bleeding

• UC.IB

bleeding from a source proximal to the ligament of Ireitz

often presents with hematemesis and rnelena unless very brisk (then can present with

hematochezia), may present with anemia, hypovolemic shock

initial management with PPls and endoscopy; if fails, then consider surgical management

appropriate to etiology

• PUD accounts for approximately 55% ofsevere UCilB

Overt Bleeding:obvious hematemesis.

hematochezia or rnelena per rectum (i.e.

visible to naked eye)

Occult Bleeding: bleeding per rectum is

not obvious to naked eye (c.g. positive

guaiac FOBT)

Obscure Bleeding:bleeding with no

identifiable source after colonoscopy

and endoscopy (source usually in small

bowel).Can be either overt or occult

. LGIB

bleeding from a source distal to the ligament of T'

reitz

often presents with BRBPR unless proximal to transverse colon, rarely rnelena (right-sided colonic

bleeding)

initial management with colonoscopy to detect and potentially stop source of bleeding

75% of patients will spontaneously stop bleeding, however if bleeding continues, barium enema

should NOT'

be performed

angiography or RBC scan to determine source as indicated

surgery indicated if bleeding is persistent - aimed at resection of area containing source of

bleeding

for obscure bleed conduct wireless capsule endoscopy, may require blind total colectomy if the

source is not found

diverticular bleeding is the most common cause of LG1B (accounting for 40% of cases)

Table 3. Differential Diagnosis of Gl Bleeding

Anatomical Source Etiology

Excess anticoagulation (warfarin, heparin, etc.) DIC

Excess antiplatelet (dopidogrel. ASA)

Epistaxis

Esophageal varices

Mallory-Weiss tear

Esophagitis

Gastritis

Castric varices

Dieulaloy’slesion

Duodenal ulcer

Perforated duodenal ulcer*

Tumours'

Polyps

Ulcers

Meckel's diverticulum

Small bowel obstruction

Colorectal cancer*

Mesenteric tlrrombosis/isthemic bowel*

UC’(subtotal colectomy if failure of medical

management)

Angiodysplasia

Diverticulosis (’if bleeding is persistent)

Diverhculosis ('

if bleeding is persistent)

Sigmoid cancer*

Bleeding postpolypcclomy

Hemorrhoids

Fissures

Pedal cancer*

Anal varices

Hematological

Congenital bleeding disorders

BloodworkforGI Bleeds

CBC (including platelet count), serum

chemistries (electrolytes. BUN,LFTs,

etc,), coagulation studies (INR, PT, PTT),

blood type and crossmatch if anticipate

transfusion

Nose

Aorto- esophageal fistula (generally postendovascular

aortic repair)*

Esophageal cancer

Castric ulcer

Gastric cancer *

Esophagus

Stomach

Duodenum Duodenal cancer’

Jejunum

Crohn'

s disease*

Tuberculosis of ileocecal junction

Crohn’s disease (less frequently presents with bleeding)’

Pancolitis (infectious,chemotherapy,or radiation

induced)

Bleeding post-gastrointestinal anastomosis

Ileum and Ileocecal

Junction

large Intestine

Sigmoid Polyps ('

if not amenable tocolonoscopic polypectomy)

ypsj'

il nolamenable tocolonoscopic polypectomy)

Crohn’s orUC*

Solitary rectal ulcer syndrome

Rectum and Anus Pa Biochemical Signs for Differentiating

Jaundice

Hepatocellular Elevated bilirubin +

elevated ALT/AST

Cholestatic:Elevated bilirubin +

elevated ALP/GGT t duct dilatation upon

biliary UfS

Hemolysis:

*

haptoglobin t LDH

r n

’Managed surgically in most cases L J

Jaundice

+

• see Gastroenterology, G45

Note: cholestatic jaundice is often

surgical

Activate Windows

Go to Settings to activate Windows,

GS7 General and Thoracic Surgery Toronto Notes 2023

Considerations

Preoperative Preparations m

Bilirubin Levels

• informed consent (see Ethical, Legal, and Organizational Medicine. ELOM11 )

• screening questionnaire to determine risk factors e.g. age,exercise capacity,medication use,allergies,

exposure to people with infection (i.e.COVID-19)

• consider preoperative anesthesia, medicine consult as indicated to optimize patient status

Prc- bitra- Posthepatic hepatic hepatic

Serum Bilirubin

Indited t » N

Owed N t t

• IV-balanced crystalloid at maintenance rate (4:2:1 rule for paediatrics, roughly 100-125 cc/h for

adults): NS or RL (RL most common); bolus to catch up on estimated losses including losses from

bowel prep

appropriate use of fluids perioperatively decreases risk of cardiorespiratory complications

• patients can take their regular medications except for hypoglycemic agents, diuretics, and ACEis

• patients with primary adrenal insufficiency (e.g. Addison'

s disease) or secondary adrenal insufficiency

(e.g. glucocorticoid use) may reuuire additional glucocorticoid stress dose coverage

• anticoagulation /antiplatelet medication must be managed to decrease surgical bleeding but not put

patient at risk for increased thrombotic events(e.g. Bridging:switching from warfarin to LMWH,

easier to start/stop as needed)

• prophylactic antibiotics depending on wound class (immediately/within 1 h prior to incision):

cefazolin (skin flora coverage) ± metronidazole (Gl flora coverage) for contaminated cases

• role of MBP:Current evidence suggests that use of MBP preoperatively has no impact on postoperative

complications, and therefore, routine use of MBP for non-LAK elective colorectal surgery is not

recommended

MBP is indicated in open or laparoscopic anterior resection i.e.rectal resection where

anastomosis is at or below sacral promontory;given with antibiotics

• assess risk for postoperative V I E prior to surgery based on procedure- and patient-related factors;

tools such as Caprini Score can be used

only hold VT'

E prophylaxis if epidural is expected

• smoking cessation and weight loss preoperatively can significantly decrease postoperative

complications

• infection:delay elective surgery until infection managed, including respiratory infection (particularly

in asthma patients)

• when scheduling elective surgeriesfollowing a COVID-19 diagnosis, consider the severity of

COVID-19 illness, the risks of complications, and risks of delaying surgery

Urine

Urobilinogen t

Bilirubin

t

Fecal

Urobilinogen t e

In

m

patients with liver disease and an

acute abdomen,spontaneous bacterial

peritonitis must be ruled out

Surgical Emergencies:Take an AMPLE

History

Allergies

Medications

fast medical/surgical history (including

anesthesia and bleeding disorders)

Last meal

Events - HPI

Best Practice InGeneral Surgery

(BPIGS)

http://www.bpigs.ca/

Best Practice in Surgery is a resource

from the quality improvement program

at theUniversity of Toronto Department

of Surgery.Since its inception,it has

expanded beyond general surgery best

practices and provides EBM guidelines

for a variety of fields and procedures

Table 4. Recommendations for Timing of Surgery following Recovery from COVID-19 with

Consideration of Individual Risk/Benefits

ClinicalSeverity of COVID-19 Infection

Moderate Priority of Surgical

Procedure Mild Severe

Moderalc symptomatic Lung involvement

requiring hospilalnalion

and/or significant

comorbidities and/or

immunocompromised

«7 wk post-infection

consider non- operative

oplionsil sale and

available

7 wkpost infection 7 wk post inlection

Critically ill

Severe C0VID-19 wrlh

ICU admission and/or

meet criteria lor severe

disease and/or severely

immunocompromised

<7 wk post-infection

consider non- operative

options if sale and

available

12 wk postinfection

Mild (suspected or

confirmed) COVID-19 and/ COVID-19 not requiring

or asymptomatic and/or hospitalization and/or

upper respiratory tract persistent symptoms

infection

Urgent orEmergent «2wk Do case urgently/

ACATS and PCATS Urgent emergently

within 3,7 or 14 days

Do case urgently/

emergently Mechanical BowelPreparationStrategies:A

ClinkalPractice Guideline developed bylbe

University olToronto's lestPractice inSurgery

Informed by:Can J Surg 2010:53:385-395

14ICIs (5071participants).8 meta-analyses

1. All open,

'

laparoscopic colorectal procedures

(excluding LAfts tdiverting stoma)

• l

,a MBP

• Ho dietary restrictions before IPO

• fleet enemalor left cotononastomows with

bansrectal stapling

2. Open/laparoscopicIAR

- divertingstoma

- MBP

• Ho dietary restrictionsbefore MBP;cleat

fluids after MBPcomplete

Urgent (28 or 42 days) 4 -7 wk post infection

2-SwkACATS/PCATS

Elective (»43 days) »6wk

ACATS/PCATS

Investigations

• see Anesthesia, A4

• routine preoperative laboratory investigations for elective procedures should be selective

only ASA class and surgical risk have been found to independently predict postoperative adverse

effects

• blood components: group and screen or cross and type depending on procedure

• CBC, electrolytes, creatinine

• INR/PT. PTT

• CXR ( PA and lateral) for patients with history of cardiac or pulmonary disease

• ECG asindicated by history or age>69 and no risk factors

• P-hCG testing in all women of reproductive age

• for patients undergoing low-risk surgery withoutsystemic disease (ASA 1 or II), routine preoperative

chest x-rays,CBC, 1NR, and PTT should be avoided

r 1

L J

+