Post on 09-Apr-2017
Approach & management Acute lower Gastrointestinal Bleeding
DR ABDUL RUB PGY3 MEM
Definitions
Upper GI bleed – arising from the esophagus, stomach, or proximal duodenum
Mid-intestinal bleed – arising from distal duodenum to ileocecal valve
Lower intestinal bleed – arising from colon/rectum
Stool color and origin/pace of bleeding
• Guaiac positive stool– Occult blood in stool – Does not provide any localizing information– Indicates slow pace, usually low volume bleeding
• Melena– Very dark, tarry, pungent stool– Usually suggestive of UGI origin (but can be small
intestinal, proximal colon origin if slow pace)• Hematochezia
– Spectrum: bright red blood, dark red, maroon – Usually suggestive of colonic origin (but can be UGI
origin if brisk pace/large volume)
APPROACH TO A PATIENT WITH GI BLEED
68 yo male presents with a chief complaint of a large amount of “bleeding from the rectum”
Physical examination: BP 105/70, Pulse 100, (+) orthostatic changes Alert and mentating, but anxious appearing
Case – Physical Exam
HOPI: Describes bleeding as large volume, very dark maroon colored stool
Has occurred 4 times over past 3 hours He felt light headed and nearly passed out upon
trying to get up to go the bathroom
Case - HPI
Denies abdominal pain, nausea, vomiting, antecedent retching
No history of heartburn, dysphagia, weight loss No history of diarrhea or constipation/hard stools
Case – PMHx, Meds
Hepatitis C CAD – h/o MI AAA – s/p elective repair 3
years ago HTN HypercholesterolemiaScreening colonoscopy 10
years ago – no polyps, (+) diverticulosis
• Medications:– Aspirin– Clopidogrel– Atorvastatin– Atenolol– Lisinopril
examination
Anicteric Mid line scar, benign abdomen, no tender liver edge
palpable in epigastrium, no splenomegaly Rectal examination – no masses, dark maroon blood
APPROACH STARTS FROM HISTORY & PHYSICAL EXAM
History Localizing symptoms History of prior GIB NSAID/aspirin use Liver disease/cirrhosis Vascular disease Aortic valvular disease,
chronic renal failure AAA repair Radiation exposure Family history of GIB
Physical Examination
• Vital signs, orthostatics• Abdominal tenderness• Skin, oral examination • Stigmata of liver disease• Rectal examination
– Objective description of stool/blood
– Assess for mass, hemorrhoids– No need for guaiac test
Case - Labs
Labs Hct 21% (Baseline 33%) Plt 110K BUN 22, Cr 1.0 Alb 3.5 INR 1.6 ALT 51, AST 76
Initial Considerations
Differential diagnosis? What is most likely source? What diagnosis can you least afford to miss?
How sick is this patient? (risk stratification) Determines disposition Guides resuscitation Guides decision re: need for/timing of endoscopy
Differential Diagnosis – Upper GIB
Peptic ulcer disease Gastroesophageal varices Erosive esophagitis/gastritis/duodenitis Mallory Weiss tear Vascular ectasia Neoplasm Dieulafoy’s lesion Aortoenteric fistula Hemobilia, hemosuccus pancreaticus
Rare, but cannot afford to
miss
Most commo
n
Differential Diagnosis – Lower GIB
Diverticular-20% AVM-10% Malignancy-2-26% Inflammatory Bowel Disease-10% Ischemic Colitis Acute Infectious Colitis Radiation Colitis/Proctitis Aortoenteric Fistula
Most common diagnosis
Narrowing the DDx: Upper or Lower Source?
Predictors of UGI source: Age <50 Melenic stool BUN/Creatinine ratio
If ratio ≥ 30, think upper GIB
J Clin Gastroenterol 1990;12:500Am J Gastroenterol 1997;92:1796Am J Emerg Med 2006;24:280
Utility of NG Tube
Most useful situation: patients with severe hematochezia, and unsure if UGIB vs. LGIB Positive aspirate (blood/coffee grounds) indicates UGIB
Can provide prognostic info: Red blood per NGT – predictive of high risk endoscopic lesion Coffee grounds – less severe/inactive bleeding
Negative aspirate – not as helpful; 15-20% of patients with UGIB have negative NG aspirate
Ann Emerg Med 2004;43:525Arch Intern Med 1990;150:1381Gastrointest Endosc 2004;59:172
Initial Assessment Always remember to assess A,B,C’s Assess degree of hypovolemic shock
Resuscitation
IV access: large bore peripheral IVs best (alt: cordis catheter) Use crystalloids first Anticipate need for blood transfusion
Threshold should be based on underlying condition, hemodynamic status, markers of tissue hypoxia Should be administered if Hgb ≤ 7 g/dL 1 U PRBC should raise Hgb by 1 (HCT by 3%) Remember that initial Hct can be misleading (Hct remains the same with loss of whole blood, until re-equilibration occurs)
Correct coagulopathy
Resuscitation
IV access: large bore peripheral IVs best (alt: cordis catheter) Use crystalloids first Anticipate need for blood transfusion
Threshold should be based on underlying condition, hemodynamic status, markers of tissue hypoxia Should be administered if Hgb ≤ 7 g/dL 1 U PRBC should raise Hgb by 1 (HCT by 3%) Remember that initial Hct can be misleading (Hct remains the same with loss of whole blood, until re-equilibration occurs)
Correct coagulopathy
Transfusion Strategy
Randomized trial: 921 subjects with severe acute GIB Restrictive (tx when Hgb<7; target 7-9) vs. Liberal
(tx when Hgb<9; target 9-11) Primary outcome: all cause mortality rate within 45
days
NEJM 2013;368;11-21
Restrictive Strategy SuperiorRestrictive Liberal P value
Mortality rate 5% 9% 0.02Rate of further
bleeding10% 16% 0.01
Overall complication
rate
40% 48% 0.02
NEJM 2013;368;11-21
Benefit seen primarily in Child A/B cirrhotics
Resuscitation
IV access: large bore peripheral IVs best (alt: cordis catheter) Use crystalloids first Anticipate need for blood transfusion
Threshold should be based on underlying condition, hemodynamic status, markers of tissue hypoxia Should be administered if Hgb ≤ 7 g/dL 1 U PRBC should raise Hgb by 1 (HCT by 3%) Remember that initial Hct can be misleading (Hct remains the same with loss of whole blood, until re-equilibration occurs)
Correct coagulopathy
Weigh risks and benefits of reversing anticoagulation
Assess degree of coagulopathy
Vitamin K – slow acting, long-lived
FFP – fast acting, short lived- Give 1 U FFP for every 4 U PRBCs
Correction of Coagulopathy
FFP transfusion Synthetic liver dysfunction Warfarin
Consider Vitamin K Dilutional coagulopathy Goal INR <1.5
Platelet transfusion in bleeding pt if less than 50K Platelet dysfunction
Anti-platelet agents or uremia Goal platelets >50, 000/mm³
action
Early resuscitation and supportive measures are
critical to reduce mortality from GIB
Resuscitation
Early intensive resuscitation reduces mortality Consecutive series of patients with hemodynamically
significant GIB First 36 subjects = Observation Group (no
intervention) Second 36 subjects = Intensive Resuscitation Group
(intense guidance provided) – goal was to decrease time to correction of hemodynamics, Hct and coagulopathy
Am J Gastroenterol 2004;99:619
Risk Stratification
Identify patients at high risk for adverse outcomes Helps determine disposition (ICU vs. floor vs.
outpatient) May help guide appropriate timing of endoscopy
Lower GI Bleed
Bleeding arising from the colorectum In patients with severe hematochezia, first
consider possibility of UGIB 10-15% of patients with presumed LGIB are found to
have upper GIB
Lower GI Bleed
Differential Diagnosis- Diverticulosis (# 1 cause)- Angioectasias- Hemorrhoids- Colitis (IBD, Infectious, Ischemic)- Neoplasm- Post-polypectomy- Dieulafoy’s lesion
Large volume, painless
Smaller volume, pain, diarrhea
LGIB – Risk Stratification
Predictors of severe* LGIB: HR>100 SBP<115 Syncope nontender abdominal examination bleeding during first 4 hours of evaluation aspirin use >2 active comorbid conditions
0 factors: ~6% risk
1-3 factors: ~40%
>3 factors: ~80%
Arch Intern Med 2003;163:838Am J Gastroenterol 2005;100:1821
* Defined as continued bleeding within first 24 hours (transfusion of 2+ Units, decline in HCT of 20+%) and/or recurrent bleeding after 24 hours of stability
LGIB – Risk Factors for Mortality
• Age• Intestinal ischemia• Comorbid illnesses
• Secondary bleeding (developed during admission for a separate problem)
• Coagulopathy• Hypovolemia• Transfusion requirement• Male gender
Clinical Gastro Hepatol 2008;6:1004
Role of Colonoscopy
Like UGIB, ~80% of LGIBs will resolve spontaneously; of these, ~30% will rebleed Lack of standardized approach
Traditional approach: elective colonoscopy after resolution of bleeding, bowel prep – low therapeutic benefit Angiography for massive bleeding, hemodynamically unstable patient
Urgent colonoscopy approach Similar to UGIB – identify stigmata of hemorrhage, perform therapy
Radiographic Studies
Tagged RBC scan Noninvasive, highly
sensitive (0.05-0.1 ml/min) Ability to localize bleeding
source correctly only ~66% More accurate when
positive within 2 hours (95-100%)
Lacks therapeutic capability
Coordinate with IR so that positive scan is followed closely by
angiography
Role of Surgery
Reserved for patients with life-threatening bleed who have failed other options
General indications: hypotension/shock despite resuscitation, >6 U PRBCs transfused
Preoperative localization of bleeding source important
Algorithmic Evaluation of Patient with Hematochezia
Hematochezia
Assess activity of
bleed
NG lavage Prep for Colonoscopy
Positive
EGD
Negative
active inactive
Risk for UGIB
Hemodynamically stable?
No risk for UGIB
negativeTreat lesion positiv
e
Evaluation ACUTE LOWER GI BLEED
Study Yield % Comments
Colonoscopy 69-80 Therapeutic
Arteriography 40-78 1 ml/min, risks
Tagged RBC Scan 20-72 Localization
Zuccaro. ASGE Clinical Update. 1999.
Take Home Points
Always get objective description of stool color (best way – examine it yourself)
Don’t order guaiac tests on inpatients
Severe hematochezia can be from UGIB, even if NG lavage is negative
Take Home Points
• All bleeding eventually stops (and majority of nonvariceal bleeds will stop spontaneously, with the patient alive)
• Early resuscitation and supportive care are key to reducing morbidity and mortality from GIB
Always get objective description of stool
Take Home Point
Avoid noninformative terms such as “grossly guaiac positive”
If you need a card to tell you whether there’s blood in the stool, it’s NOT an
acute GIB
Take Home Point
Take Home Point
Upper GI bleed must still be considered in patients with severe hematochezia, even
if NG aspirate negative
THANKS