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Gall Bladder Carcinoma 
Muhammad Haris Aslam Janjua 
Resident, Surgical Unit I 
SIMS/Services Hospital, Lahore
Case Summary 
• A 40 Year old female presented to OPD SHL on 11th Jan 14, with pain in upper 
abdomen for 15 days which was acute in onset, progressive, continuous, 
constricting, moderate to severe, radiating to back side, aggravated by fatty meals 
and relieved temporarily by medications. 
• No h/o fever, vomiting, constipation/diarrhea ,weight loss 
• Unremarkable medical and surgical history 
• On examination: RHC was tender with Murphy sign +ve. Rest of examination 
unremarkable. 
• USG showed gall stones with no edema and thick GB wall. 
• Serum amylase levels were 26, lipase levels were 11 and total bilirubin was 0.4 . 
TLC was 11.0 
• Patient was admitted and managed on lines of acute cholecystitis 
• During her stay in the ward departmental USG showed cholelithiasis and multiple 
enlarged lymph nodes in porta hepatis and peripancreatic area . Patient was sent 
on leave and advised follow up after CT scan and CA 19-9 report.
Case Summary 
• CT scan(17th Jan 14) showed multiple enlarged lymph nodes in porta 
hepatis and both para-aortic planes and pleuropericardial recess. CA19-9 
level (24th Jan 2014)were 15.68 (normal range less than 37) 
• Patient was re-evaulated and was discharged on conservative treatment 
• Patient again presented in ER on 7th Feb 14, with pain RHC and was 
readmitted for workup 
• Serum amylase was 60, total bilirubin was 0.7 ,TLC 10.0 
• Repeat USG showed Multiple Gallstones with soft tissue density mass. 
However wall is not thick and no pericholecystic fluid. CHD dilated upto 
6mm but distal CBD and intrahepatic duct was not dilated . Multiple 
enlarged lymph nodes in para aortic, celiac, peri pancreatic and porta 
hepatic regions with liver slightly coarse in echo texture. 
• Laparatomy was done on 13th Feb 14 and intraoperatively gall bladder 
mass was seen infiltrating the liver and GB biopsy was taken, which 
showed Poorly Differenciated adenocarcinoma.
Outline 
• Relevent anatomy 
• Introduction 
• Epidemiology 
• Etiology/Pathophysiology 
• Presentation 
• Workup 
• Treatment 
• Follow Up 
• References
Relevant Anatomy 
• Saccular structure located at the inferior surface of the 
liver, at the division of the right and left lobes, just 
below segments IV and V 
• Composed of 4 areas: fundus, body, infundibulum, and 
neck 
• Approx. 7-10 cm long and about 2.5-3.5 cm wide 
• Normally contains approx. 30-50 mL of fluid(max up to 
300 mL)
Relevant Anatomy 
Lymphatic Drainage 
• Cystic Node 
• pericholedochal nodes 
• regional nodal basins (superior mesenteric, 
retropancreatic, retroportal, and celiac) 
• aortocaval nodes*( directly or indirectly) 
*exposure of this region is a necessary step in the operative staging of gallbladder 
cancer
Relevant Anatomy 
Spread of GB cancer 
• spreads via the lymphatic channels and venous 
drainage 
• Peritoneal metastasis common 
• Due to adjacent location liver, bile duct, portal 
vein, hepatic artery, duodenum, and transverse 
colon involvement is common
Relevant Anatomy 
Cystic Plate* 
• It is reflection of the visceral peritoneum between the liver and the 
gallbladder. 
• Dissection between the gallbladder and the liver during 
cholecystectomy divides the plane between the cystic plate and 
the muscle layer of the gallbladder 
*anatomic basis for the improved survival in patients undergoing liver 
resection for T1b gallbladder cancer.
Introduction 
• Gallbladder carcinoma was first described by Maximilian Stoll in 
1777 and more than 200 years later it is still considered to be a 
highly malignant disease with a poor survival rate 
• G.B cancer is relatively uncommon but it is the 5th most common 
GIT malignancy(worldwide) 
• most frequent malignant tumor of the biliary tract 
• 90 % Adenocarcinomas. 
• Mucosal squamous metapalsia Squamous cell carcinoma
Introduction 
Premalignant Lesions 
• Adenomatous polyps 
– Papillary adenomas grow as pedunculated, complex, 
branching tumors projecting into the gallbladder lumen. 
– Tubular adenomas arise as a flat, sessile neoplasm. 
• Adenomyomatosis 
– extensions of Rokitansky-Aschoff sinuses through the 
muscular wall of the gallbladder 
– USG reveals a thickened gallbladder wall with intramural 
diverticula 
– serial evaluation with USG is indicated to rule out 
enlarging adenomatous polyps and gallbladder cancer
Epidemiology 
• incidence of GC  1 to 23 per 100,000 worldwide 
• over the last three decades there is decrease in incidence in 
developed and increase in incidence in developing countries 
• The highest incidence of gallbladder carcinoma is reported more 
recently from the Indian-Subcontinent including India and Pakistan 
(18-23/100,000)  mirror image of worldwide distribution of gall 
stones 
• A relatively rare malignancy worldwide but is the second 
commonest gastrointestinal cancer in Pakistani women 
• Most common cause of gastrointestinal cancer related mortality in 
females in subcontinent.[17,18]
Epidemiology 
• Rise in incidence of GC from Northern India and Southern Pakistan 
over the past two decades 
• Frequency of gallbladder cancer in Pakistan varies between 6-7%. 
[13-15] 
• Highest incidence is found in Chelians, American Indian and in parts 
of Northern India where it accounts for 9% of all biliary tract 
diseases. 
• Female to male ratio is 3:1 
• Peak incidence is in 7th decade of life.[2]
Etiology/Pathophysiology 
• Gallstones are present in 60-90 % of GB cancer cases (World wide) 
.[3][12]. 
– a small proportion of patients (1-3%) with gall stones developed G.B cancer 
[16,17] 
– inverse relationship between the incidence of GC and rate of cholecystectomy 
– In pakistan 98-100 % of cases of GC have gall stone[18][19] 
• Risk factors include 
– Chronic inflamation and infection. 
– Porcelain Gallbladder 
– Typhoid carrier 
– Adenomatous polyp (size of the polyp is strongest predictor of malignant 
transformation)[3] 
– Advanced age(>55 yr) 
– Multiparity(>5) 
– Presence of gallstone larger than 1[17]-3[18]cm. 
– Anomalous pancreatobiliary junction 
– Drugs :OCP, methyldopa
– Occupational exposure to rubber,cigrette smoking 
– Bile acid composition. 
– Diet: low fibre, low calories. High fine CHO, low protein 
• A 2008 study found evidence that excess body weight 
in women, specifically a 5 kg/m 2increase in the body-mass 
index, is strongly associated with an increased 
risk of gallbladder cancer.[4] 
• Numerous studies have investigated genetic 
abnormalities in gallbladder cancer and have shown 
that approximately 39-59% of gallbladder cancers are 
associated with the K-ras mutation, while more than 
90% of them are associated with a p53 mutation.[5]
Presentation 
• Usually asymptomatic at the time of diagnosis 
• Symptoms if present are similar to benign 
diseases such as cholecystitis or biliary colic. 
• Jaundice and anorexia are late features 
• Palpable mass is a late sign[2] 
• Given this presentation, less than 50% of 
gallbladder cancers are diagnosed preoperatively. 
Many are diagnosed incidentally in gallbladders 
removed for biliary colic or cholecystitis.
Work Up 
• Laboratory studies are generally nonspecific for gallbladder 
cancer. 
• In the later stages, liver function enzyme levels may be slightly 
elevated. These levels are generally not elevated in stages I 
and II. 
• An elevated bilirubin or alkaline phosphate level generally 
indicates advanced or obstructive disease. 
Tumour Marker Sensitivity Specificity 
CA 19-9 * 79.4 % 79.5% 
CEA 50 % 93% 
*Found in 80% of the cases
Imaging studies 
• Ultrasonography is a very useful tool in the workup of 
gallbladder cancer. Polypoid lesions need to be at least 5 
mm in size to be detected by ultrasonography. Cholesterol 
polyps (benign) generally appear as pedunculated lesions 
attached to the gallbladder wall. 
• Ultrasonographic findings that indicate possible malignancy 
– a thick gallbladder wall, 
– vascular polyp, 
– a mass projecting into the lumen or invading the wall, multiple 
masses or a fixed mass in the gallbladder, 
– a porcelain gallbladder, and an extracholecystic mass. Invasion 
of the liver can also be seen on ultrasonograms.
This image demonstrates heterogeneous 
thickening of the gallbladder wall (arrows). The 
diagnosis was primary papillary adenocarcinoma of 
the gallbladder.
• Computed tomography (CT) scanning and magnetic resonance 
imaging (MRI) are useful in evaluating the extent of invasion and 
resectability of gall bladder tumors. CT scan results suggestive of 
gallbladder cancer include asymmetrical wall thickening or 
gallbladder mass with or without invasion into the liver. 
• CT scanning of the chest, abdomen, and pelvis is a common staging 
modality that can determine the presence of distant metastases 
and give reliable information about involvement of other organs 
and vascular structures. 
• Positron emission tomography (PET) scanning has a sensitivity of 
75% and a specificity of 88% in gallbladder cancer but is not used 
routinely.
Partially calcified gallbladder (arrow). At 
laparotomy and histology, 
an infiltrating adenocarcinoma of the 
gallbladder was confirmed. 
CT scan showing squamous cell 
carcinoma of gall bladder showing Liver 
metastasis
Diagnostic procedures 
• Percutaneous CT scan – guided biopsy is avoided in patients 
considered resectable based on preoperative imaging. Because of 
the substantial risk of peritoneal seeding, percutaneous biopsy and 
diagnostic cholecystectomy are not necessary in the patient 
suspected of having gallbladder cancer. In these patients, 
exploration with curative intent is planned based on preoperative 
imaging alone. 
• Percutaneous CT scan – guided biopsy is a useful diagnostic tool in 
patients who appear to have a nonresectable tumor. Tissue 
diagnosis is necessary for palliative treatment. 
• Endoscopic ultrasonography with fine-needle aspiration Biopsy 
can be used to evaluate for peripancreatic and periportal 
lymphadenopathy.
Staging 
• The American Joint Committee on Cancer (AJCC) has designated staging by the TNM (primary t umor, regional 
lymph n odes, distant m etastasis) classification as follows [6] 
• TNM Definitions 
Primary tumor (T) 
• TX - Primary tumor cannot be assessed 
• T0 - No evidence of primary tumor 
• Tis - Carcinoma in situ 
• T1 - Tumor invades lamina propria or muscle layer . T1a - Tumor invades lamina propria 
• T1b - Tumor invades the muscularis 
• T2 - Tumor invades the perimuscular connective tissue; no extension beyond the serosa or into the liver 
• T3 - Tumor perforates the serosa (visceral peritoneum) and/or directly invades the liver and/or 1 other adjacent organ 
or structure, such as the stomach, duodenum, colon, pancreas, omentum, or extrahepatic bile ducts 
• T4 - Tumor invades the main portal vein or hepatic artery or invades multiple extrahepatic organs or structures 
Regional lymph nodes (N) 
• NX - Regional lymph nodes cannot be assessed 
• N0 - No regional lymph node metastasis 
• N1 - Portal lymph node metastasis 
• N2 - Distant lymph node metastasis such as periaortic, pericaval, superior mesenteric artery, or celiac artery 
Distant metastasis (M) 
• MX - Distant metastasis cannot be assessed 
• M0 - No distant metastasis 
• M1 - Distant metastasis
AJCC Stage Groupings 
• Stage 0: Tis, N0, M0 
• Stage I: T1 (a or b), N0, M0 
• Stage II: T2, N0, M0 
• Stage IIIA: T3, N0, M0 
• Stage IIIB: T1 to T3, N1, M0 
• Stage IVA: T4, N0 or N1, M0 
• Stage IVB: Any T, N2, M0, OR Any T, any N, M1
In Our case...................... 
• T3 (liver involvement) 
• N2 (para-aortic and celiac lymph node 
involvement ) 
• M1(as paraaortic LN involvement is 
considered sign of distant metastsis) 
• i.e. Stage IVB
Non surgical Management 
• Small gallbladder tumors are common and many can be safely followed 
with serial ultrasonographic examination. It is generally thought that 
polyps of less than 1 cm are safe to follow, although a study[7] has 
recommended that polyps that are greater than or equal to 6 mm should 
be considered for cholecystectomy. 
• Chemotherapy is used in the adjuvant and palliative treatment of 
gallbladder cancer. Phase II studies have shown that the use of single-agent 
chemotherapy (with gemcitabine or 5-fluorouracil) in the palliative 
setting can be beneficial. 
• Combination chemotherapy also has been shown to be beneficial and is 
usually based on gemcitabine, capecitabine, and 5-fluorouracil used in 
combination with cis-platinum or oxaliplatinum. Fluoropyrimidine-based 
chemoradiotherapy is commonly employed in the palliative and adjuvant 
setting as well.
Surgical management 
• Cholecystectomy recommended in 
– polyps larger than 1 cm or with polyps in the setting of primary sclerosing 
cholangitis 
– porcelain gallbladder.[2] 
• Diagnostic Laproscopy 
– In order to exclude the presence of undetected intra-abdominal metastases 
prior to curative laparotomy. 
– Surgery is contraindicated in the presence of distant metastases. 
• Exploratory Laparotomy 
– The initial exploration focuses on the presence of metastatic disease that was 
not detected by preoperative imaging and staging laparoscopy.(15%) 
– In view of North american surgeons Biopsy-proven metastases in the celiac 
nodes preclude resection. 
– Aortocaval nodal metastases are considered distant metastatic disease.
STAGE TREATMENT 
T1a Simple cholecystectomy 
T1b or deeper Hepatic resection + 
lymph node dissection 
(portal , peripancreatic , and retroduodenal)+ 
Resection of liver segments 
IVb and V +/- 
extended liver resection 
and/or bile duct resection
Intraoperative ultrasonography (IOUS) 
• To evaluate the extent of involvement of the liver, as well as 
the portal and intrahepatic vasculature. 
• This information is especially useful when ligating the pedicle 
to segment V and avoiding injury to the right anterior portal 
pedicle or segment VIII pedicle. Extended right hepatectomy 
may be necessary to achieve tumor clearance if the tumor 
involves the right portal pedicles
A schematic drawing of the 
extent of lymphadenectomy for 
gallbladder cancer, especially 
when the extrahepatic biliary 
tree is resected. 
Gallbladder tumors. 
A schematic 
drawing of the 
extent of resection 
of liver segments 
IV-b and V for 
gallbladder cancer.
• Surgical exploration 
– will determine the need to resect other organs that may 
be involved, such as the stomach, duodenum, and colon. 
– It may be difficult to distinguish scar from malignancy. In 
these cases, suspicious tissue should be treated as 
malignancy in order to improve the chances of a margin-negative 
resection. 
– If tumor is suspected on the bile duct based on a previous 
pathology report or operative exploration, the presence of 
tumor on the right hepatic duct must be evaluated. 
– Suspicion of tumorous involvement of the right hepatic 
duct will require an extended right hepatectomy, excision 
of the extrahepatic biliary tree, and Roux-en-Y 
hepaticojejunostomy to the left hepatic duct. 
• A recent study indicates that accurate staging requires 
examination of at least 6 lymph nodes.
No standard adjuvant treatment protocol has been 
defined for gall bladder cancer. 
– A 2008 study found that only 20% of patients with gall 
bladder cancer received adjuvant treatment.[9] 
– In the report, no benefit from adjuvant therapy could 
be demonstrated, but only a small number of patients 
received this treatment. 
– Generally, fluoropyrimidine-based chemoradiotherapy 
or single-agent chemotherapy with fluoropyrimidines 
or gemcitabine is used.[10] 
– Because of the high cure rate with surgery alone for 
T1N0 lesions, adjuvant therapy is not commonly 
offered to these patients.
Complications 
• The overall complication and morbidity rate is 
approximately 25%. 
• Complications are similar to those experienced 
with cholecystectomy and include infection, 
hematoma, and bile leaks. 
• Complication rates are higher in patients 
undergoing more extensive resections. 
• Liver failure can occur following extended 
hepatectomy, especially if jaundice is present 
preoperatively.
PROGNOSIS [5][11] 
STAGE 5 YEAR SURVIVAL RATE 
T1b 100% especially with hepatectomy 
T2 38% to 77% after extended 
cholecystectomy 
III and IV 25 % with extended resection 
Unresectabe disease < 5% ( 1 year survival rate) 
Patients with unresectable disease have a median survival of 2-4 months
Follow Up 
• There are no data to support aggressive 
surveillance following resection of gall bladder 
cancer, because treatment of recurrences is 
not generally effective. However, many 
clinicians and patients prefer follow-up 
imaging every 6 months.
References 
1. D'Hondt M, Lapointe R, Benamira Z, Pottel H, Plasse M, Letourneau R, et al. Carcinoma of the 
gallbladder: Patterns of presentation, prognostic factors and survival rate. An 11-year single centre 
experience. Eur J Surg Oncol. Jun 2013;39(6):548-53 
2. Bailey and Love edition 26th page 1116 
3. Robins and cotrans pathologic basis of disease 7th edition 
4. [Best Evidence] Renehan AG, Tyson M, Egger M, et al. Body-mass index and incidence of cancer: a 
systematic review and meta-analysis of prospective observational studies. Lancet. Feb 16 
2008;371(9612):569-78. 
5. Tumors of the gallbladder. In: Blumgart LH, ed. Surgery of the Liver, Biliary Tract, and Pancreas. 4th ed. 
Philadelphia, Pa: Saunders Elsevier; 2007:764-81 
6. American Joint Committee on Cancer. Gallbladder. In: AJCC Cancer Staging Manual. 6th ed. New York, 
NY: Springer; 2002:139-44. 
7. Zielinski MD, Atwell TD, Davis PW, et al. Comparison of surgically resected polypoid lesions of the 
gallbladder to their pre-operative ultrasound characteristics. J Gastrointest Surg. Jan 2009;13(1):19-25. 
8. [Best Evidence] Renehan AG, Tyson M, Egger M, et al. Body-mass index and incidence of cancer: a 
systematic review and meta-analysis of prospective observational studies. Lancet. Feb 16 
2008;371(9612):569-78. 
9. Duffy A, Capanu M, Abou-Alfa GK, et al. Gallbladder cancer (GBC): 10-year experience at Memorial 
Sloan-Kettering Cancer Centre (MSKCC). J Surg Oncol. Dec 1 2008;98(7):485-9. 
10. NCCN Clinical Practice Guidelines in Oncology™. Available at www.nccn.org. 
11. Okada K, Kijima H, Imaizumi T, et al. Wall-invasion pattern correlates with survival of patients with 
gallbladder adenocarcinoma. Anticancer Res. Feb 2009;29(2):685-91. 
12. 10. Zarin M, Ahmed M, Gohar A, Waheed D, Khurram S, Aurangzeb M, et al. Incidence of Gall stones in 
carcinoma gallbladder patients. Pak J Surg 2005;21(1):19-22.
13. Hassan TJ, Zuberi SJ, Maqsood R. Carcinoma of gallbladder. J 
Pak Med Assoc 1978;28:33-4. 
14. Mubarik A, Ahmed M, Khan AH, Mansoor A. Carcinoma of 
gallbladder - A study of 112 consecutive cases. Pak Armed Forces 
Med J 1990;43:1-7. 
15. Yaqin HU, Parmar BK. A comparative study of biliary tract disease 
in Karachi (Pakistan) and Aylesbury (England). J Pak Med 
Assoc 1976;26(8):162-4. 
16. Mohandas KM, Patil PS: Cholecystectomy for asymptomatic 
gallstones can reduce gall bladder cancer mortality in northern 
Indian women. Indian J Gastroenterology 2006, 25:147-151. 
17. John AP, Ashley R, Alan G: Primary carcinoma of the 
gallbladder.HBP 1991, 4:277-289 
18. Talat JH, Sarwar A J: Risk Factors for Gallbladder Cancer in Karachi.J 
Ayub Med Coll Abbottabad 2003. 
19. Bhurgri Y, Bhugri A, Hassan SH: Cancer Incidents in Karachi Pakistan: 
First results from Karachi cancer registry. Int J Cancer 2000, 85:325- 
9.
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Gall Bladder Carcinoma

  • 1. Gall Bladder Carcinoma Muhammad Haris Aslam Janjua Resident, Surgical Unit I SIMS/Services Hospital, Lahore
  • 2. Case Summary • A 40 Year old female presented to OPD SHL on 11th Jan 14, with pain in upper abdomen for 15 days which was acute in onset, progressive, continuous, constricting, moderate to severe, radiating to back side, aggravated by fatty meals and relieved temporarily by medications. • No h/o fever, vomiting, constipation/diarrhea ,weight loss • Unremarkable medical and surgical history • On examination: RHC was tender with Murphy sign +ve. Rest of examination unremarkable. • USG showed gall stones with no edema and thick GB wall. • Serum amylase levels were 26, lipase levels were 11 and total bilirubin was 0.4 . TLC was 11.0 • Patient was admitted and managed on lines of acute cholecystitis • During her stay in the ward departmental USG showed cholelithiasis and multiple enlarged lymph nodes in porta hepatis and peripancreatic area . Patient was sent on leave and advised follow up after CT scan and CA 19-9 report.
  • 3. Case Summary • CT scan(17th Jan 14) showed multiple enlarged lymph nodes in porta hepatis and both para-aortic planes and pleuropericardial recess. CA19-9 level (24th Jan 2014)were 15.68 (normal range less than 37) • Patient was re-evaulated and was discharged on conservative treatment • Patient again presented in ER on 7th Feb 14, with pain RHC and was readmitted for workup • Serum amylase was 60, total bilirubin was 0.7 ,TLC 10.0 • Repeat USG showed Multiple Gallstones with soft tissue density mass. However wall is not thick and no pericholecystic fluid. CHD dilated upto 6mm but distal CBD and intrahepatic duct was not dilated . Multiple enlarged lymph nodes in para aortic, celiac, peri pancreatic and porta hepatic regions with liver slightly coarse in echo texture. • Laparatomy was done on 13th Feb 14 and intraoperatively gall bladder mass was seen infiltrating the liver and GB biopsy was taken, which showed Poorly Differenciated adenocarcinoma.
  • 4. Outline • Relevent anatomy • Introduction • Epidemiology • Etiology/Pathophysiology • Presentation • Workup • Treatment • Follow Up • References
  • 5. Relevant Anatomy • Saccular structure located at the inferior surface of the liver, at the division of the right and left lobes, just below segments IV and V • Composed of 4 areas: fundus, body, infundibulum, and neck • Approx. 7-10 cm long and about 2.5-3.5 cm wide • Normally contains approx. 30-50 mL of fluid(max up to 300 mL)
  • 6. Relevant Anatomy Lymphatic Drainage • Cystic Node • pericholedochal nodes • regional nodal basins (superior mesenteric, retropancreatic, retroportal, and celiac) • aortocaval nodes*( directly or indirectly) *exposure of this region is a necessary step in the operative staging of gallbladder cancer
  • 7. Relevant Anatomy Spread of GB cancer • spreads via the lymphatic channels and venous drainage • Peritoneal metastasis common • Due to adjacent location liver, bile duct, portal vein, hepatic artery, duodenum, and transverse colon involvement is common
  • 8. Relevant Anatomy Cystic Plate* • It is reflection of the visceral peritoneum between the liver and the gallbladder. • Dissection between the gallbladder and the liver during cholecystectomy divides the plane between the cystic plate and the muscle layer of the gallbladder *anatomic basis for the improved survival in patients undergoing liver resection for T1b gallbladder cancer.
  • 9. Introduction • Gallbladder carcinoma was first described by Maximilian Stoll in 1777 and more than 200 years later it is still considered to be a highly malignant disease with a poor survival rate • G.B cancer is relatively uncommon but it is the 5th most common GIT malignancy(worldwide) • most frequent malignant tumor of the biliary tract • 90 % Adenocarcinomas. • Mucosal squamous metapalsia Squamous cell carcinoma
  • 10. Introduction Premalignant Lesions • Adenomatous polyps – Papillary adenomas grow as pedunculated, complex, branching tumors projecting into the gallbladder lumen. – Tubular adenomas arise as a flat, sessile neoplasm. • Adenomyomatosis – extensions of Rokitansky-Aschoff sinuses through the muscular wall of the gallbladder – USG reveals a thickened gallbladder wall with intramural diverticula – serial evaluation with USG is indicated to rule out enlarging adenomatous polyps and gallbladder cancer
  • 11. Epidemiology • incidence of GC  1 to 23 per 100,000 worldwide • over the last three decades there is decrease in incidence in developed and increase in incidence in developing countries • The highest incidence of gallbladder carcinoma is reported more recently from the Indian-Subcontinent including India and Pakistan (18-23/100,000)  mirror image of worldwide distribution of gall stones • A relatively rare malignancy worldwide but is the second commonest gastrointestinal cancer in Pakistani women • Most common cause of gastrointestinal cancer related mortality in females in subcontinent.[17,18]
  • 12. Epidemiology • Rise in incidence of GC from Northern India and Southern Pakistan over the past two decades • Frequency of gallbladder cancer in Pakistan varies between 6-7%. [13-15] • Highest incidence is found in Chelians, American Indian and in parts of Northern India where it accounts for 9% of all biliary tract diseases. • Female to male ratio is 3:1 • Peak incidence is in 7th decade of life.[2]
  • 13. Etiology/Pathophysiology • Gallstones are present in 60-90 % of GB cancer cases (World wide) .[3][12]. – a small proportion of patients (1-3%) with gall stones developed G.B cancer [16,17] – inverse relationship between the incidence of GC and rate of cholecystectomy – In pakistan 98-100 % of cases of GC have gall stone[18][19] • Risk factors include – Chronic inflamation and infection. – Porcelain Gallbladder – Typhoid carrier – Adenomatous polyp (size of the polyp is strongest predictor of malignant transformation)[3] – Advanced age(>55 yr) – Multiparity(>5) – Presence of gallstone larger than 1[17]-3[18]cm. – Anomalous pancreatobiliary junction – Drugs :OCP, methyldopa
  • 14. – Occupational exposure to rubber,cigrette smoking – Bile acid composition. – Diet: low fibre, low calories. High fine CHO, low protein • A 2008 study found evidence that excess body weight in women, specifically a 5 kg/m 2increase in the body-mass index, is strongly associated with an increased risk of gallbladder cancer.[4] • Numerous studies have investigated genetic abnormalities in gallbladder cancer and have shown that approximately 39-59% of gallbladder cancers are associated with the K-ras mutation, while more than 90% of them are associated with a p53 mutation.[5]
  • 15. Presentation • Usually asymptomatic at the time of diagnosis • Symptoms if present are similar to benign diseases such as cholecystitis or biliary colic. • Jaundice and anorexia are late features • Palpable mass is a late sign[2] • Given this presentation, less than 50% of gallbladder cancers are diagnosed preoperatively. Many are diagnosed incidentally in gallbladders removed for biliary colic or cholecystitis.
  • 16. Work Up • Laboratory studies are generally nonspecific for gallbladder cancer. • In the later stages, liver function enzyme levels may be slightly elevated. These levels are generally not elevated in stages I and II. • An elevated bilirubin or alkaline phosphate level generally indicates advanced or obstructive disease. Tumour Marker Sensitivity Specificity CA 19-9 * 79.4 % 79.5% CEA 50 % 93% *Found in 80% of the cases
  • 17. Imaging studies • Ultrasonography is a very useful tool in the workup of gallbladder cancer. Polypoid lesions need to be at least 5 mm in size to be detected by ultrasonography. Cholesterol polyps (benign) generally appear as pedunculated lesions attached to the gallbladder wall. • Ultrasonographic findings that indicate possible malignancy – a thick gallbladder wall, – vascular polyp, – a mass projecting into the lumen or invading the wall, multiple masses or a fixed mass in the gallbladder, – a porcelain gallbladder, and an extracholecystic mass. Invasion of the liver can also be seen on ultrasonograms.
  • 18. This image demonstrates heterogeneous thickening of the gallbladder wall (arrows). The diagnosis was primary papillary adenocarcinoma of the gallbladder.
  • 19. • Computed tomography (CT) scanning and magnetic resonance imaging (MRI) are useful in evaluating the extent of invasion and resectability of gall bladder tumors. CT scan results suggestive of gallbladder cancer include asymmetrical wall thickening or gallbladder mass with or without invasion into the liver. • CT scanning of the chest, abdomen, and pelvis is a common staging modality that can determine the presence of distant metastases and give reliable information about involvement of other organs and vascular structures. • Positron emission tomography (PET) scanning has a sensitivity of 75% and a specificity of 88% in gallbladder cancer but is not used routinely.
  • 20. Partially calcified gallbladder (arrow). At laparotomy and histology, an infiltrating adenocarcinoma of the gallbladder was confirmed. CT scan showing squamous cell carcinoma of gall bladder showing Liver metastasis
  • 21. Diagnostic procedures • Percutaneous CT scan – guided biopsy is avoided in patients considered resectable based on preoperative imaging. Because of the substantial risk of peritoneal seeding, percutaneous biopsy and diagnostic cholecystectomy are not necessary in the patient suspected of having gallbladder cancer. In these patients, exploration with curative intent is planned based on preoperative imaging alone. • Percutaneous CT scan – guided biopsy is a useful diagnostic tool in patients who appear to have a nonresectable tumor. Tissue diagnosis is necessary for palliative treatment. • Endoscopic ultrasonography with fine-needle aspiration Biopsy can be used to evaluate for peripancreatic and periportal lymphadenopathy.
  • 22. Staging • The American Joint Committee on Cancer (AJCC) has designated staging by the TNM (primary t umor, regional lymph n odes, distant m etastasis) classification as follows [6] • TNM Definitions Primary tumor (T) • TX - Primary tumor cannot be assessed • T0 - No evidence of primary tumor • Tis - Carcinoma in situ • T1 - Tumor invades lamina propria or muscle layer . T1a - Tumor invades lamina propria • T1b - Tumor invades the muscularis • T2 - Tumor invades the perimuscular connective tissue; no extension beyond the serosa or into the liver • T3 - Tumor perforates the serosa (visceral peritoneum) and/or directly invades the liver and/or 1 other adjacent organ or structure, such as the stomach, duodenum, colon, pancreas, omentum, or extrahepatic bile ducts • T4 - Tumor invades the main portal vein or hepatic artery or invades multiple extrahepatic organs or structures Regional lymph nodes (N) • NX - Regional lymph nodes cannot be assessed • N0 - No regional lymph node metastasis • N1 - Portal lymph node metastasis • N2 - Distant lymph node metastasis such as periaortic, pericaval, superior mesenteric artery, or celiac artery Distant metastasis (M) • MX - Distant metastasis cannot be assessed • M0 - No distant metastasis • M1 - Distant metastasis
  • 23. AJCC Stage Groupings • Stage 0: Tis, N0, M0 • Stage I: T1 (a or b), N0, M0 • Stage II: T2, N0, M0 • Stage IIIA: T3, N0, M0 • Stage IIIB: T1 to T3, N1, M0 • Stage IVA: T4, N0 or N1, M0 • Stage IVB: Any T, N2, M0, OR Any T, any N, M1
  • 24. In Our case...................... • T3 (liver involvement) • N2 (para-aortic and celiac lymph node involvement ) • M1(as paraaortic LN involvement is considered sign of distant metastsis) • i.e. Stage IVB
  • 25. Non surgical Management • Small gallbladder tumors are common and many can be safely followed with serial ultrasonographic examination. It is generally thought that polyps of less than 1 cm are safe to follow, although a study[7] has recommended that polyps that are greater than or equal to 6 mm should be considered for cholecystectomy. • Chemotherapy is used in the adjuvant and palliative treatment of gallbladder cancer. Phase II studies have shown that the use of single-agent chemotherapy (with gemcitabine or 5-fluorouracil) in the palliative setting can be beneficial. • Combination chemotherapy also has been shown to be beneficial and is usually based on gemcitabine, capecitabine, and 5-fluorouracil used in combination with cis-platinum or oxaliplatinum. Fluoropyrimidine-based chemoradiotherapy is commonly employed in the palliative and adjuvant setting as well.
  • 26. Surgical management • Cholecystectomy recommended in – polyps larger than 1 cm or with polyps in the setting of primary sclerosing cholangitis – porcelain gallbladder.[2] • Diagnostic Laproscopy – In order to exclude the presence of undetected intra-abdominal metastases prior to curative laparotomy. – Surgery is contraindicated in the presence of distant metastases. • Exploratory Laparotomy – The initial exploration focuses on the presence of metastatic disease that was not detected by preoperative imaging and staging laparoscopy.(15%) – In view of North american surgeons Biopsy-proven metastases in the celiac nodes preclude resection. – Aortocaval nodal metastases are considered distant metastatic disease.
  • 27. STAGE TREATMENT T1a Simple cholecystectomy T1b or deeper Hepatic resection + lymph node dissection (portal , peripancreatic , and retroduodenal)+ Resection of liver segments IVb and V +/- extended liver resection and/or bile duct resection
  • 28. Intraoperative ultrasonography (IOUS) • To evaluate the extent of involvement of the liver, as well as the portal and intrahepatic vasculature. • This information is especially useful when ligating the pedicle to segment V and avoiding injury to the right anterior portal pedicle or segment VIII pedicle. Extended right hepatectomy may be necessary to achieve tumor clearance if the tumor involves the right portal pedicles
  • 29. A schematic drawing of the extent of lymphadenectomy for gallbladder cancer, especially when the extrahepatic biliary tree is resected. Gallbladder tumors. A schematic drawing of the extent of resection of liver segments IV-b and V for gallbladder cancer.
  • 30. • Surgical exploration – will determine the need to resect other organs that may be involved, such as the stomach, duodenum, and colon. – It may be difficult to distinguish scar from malignancy. In these cases, suspicious tissue should be treated as malignancy in order to improve the chances of a margin-negative resection. – If tumor is suspected on the bile duct based on a previous pathology report or operative exploration, the presence of tumor on the right hepatic duct must be evaluated. – Suspicion of tumorous involvement of the right hepatic duct will require an extended right hepatectomy, excision of the extrahepatic biliary tree, and Roux-en-Y hepaticojejunostomy to the left hepatic duct. • A recent study indicates that accurate staging requires examination of at least 6 lymph nodes.
  • 31. No standard adjuvant treatment protocol has been defined for gall bladder cancer. – A 2008 study found that only 20% of patients with gall bladder cancer received adjuvant treatment.[9] – In the report, no benefit from adjuvant therapy could be demonstrated, but only a small number of patients received this treatment. – Generally, fluoropyrimidine-based chemoradiotherapy or single-agent chemotherapy with fluoropyrimidines or gemcitabine is used.[10] – Because of the high cure rate with surgery alone for T1N0 lesions, adjuvant therapy is not commonly offered to these patients.
  • 32.
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  • 34.
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  • 36.
  • 37. Complications • The overall complication and morbidity rate is approximately 25%. • Complications are similar to those experienced with cholecystectomy and include infection, hematoma, and bile leaks. • Complication rates are higher in patients undergoing more extensive resections. • Liver failure can occur following extended hepatectomy, especially if jaundice is present preoperatively.
  • 38. PROGNOSIS [5][11] STAGE 5 YEAR SURVIVAL RATE T1b 100% especially with hepatectomy T2 38% to 77% after extended cholecystectomy III and IV 25 % with extended resection Unresectabe disease < 5% ( 1 year survival rate) Patients with unresectable disease have a median survival of 2-4 months
  • 39. Follow Up • There are no data to support aggressive surveillance following resection of gall bladder cancer, because treatment of recurrences is not generally effective. However, many clinicians and patients prefer follow-up imaging every 6 months.
  • 40. References 1. D'Hondt M, Lapointe R, Benamira Z, Pottel H, Plasse M, Letourneau R, et al. Carcinoma of the gallbladder: Patterns of presentation, prognostic factors and survival rate. An 11-year single centre experience. Eur J Surg Oncol. Jun 2013;39(6):548-53 2. Bailey and Love edition 26th page 1116 3. Robins and cotrans pathologic basis of disease 7th edition 4. [Best Evidence] Renehan AG, Tyson M, Egger M, et al. Body-mass index and incidence of cancer: a systematic review and meta-analysis of prospective observational studies. Lancet. Feb 16 2008;371(9612):569-78. 5. Tumors of the gallbladder. In: Blumgart LH, ed. Surgery of the Liver, Biliary Tract, and Pancreas. 4th ed. Philadelphia, Pa: Saunders Elsevier; 2007:764-81 6. American Joint Committee on Cancer. Gallbladder. In: AJCC Cancer Staging Manual. 6th ed. New York, NY: Springer; 2002:139-44. 7. Zielinski MD, Atwell TD, Davis PW, et al. Comparison of surgically resected polypoid lesions of the gallbladder to their pre-operative ultrasound characteristics. J Gastrointest Surg. Jan 2009;13(1):19-25. 8. [Best Evidence] Renehan AG, Tyson M, Egger M, et al. Body-mass index and incidence of cancer: a systematic review and meta-analysis of prospective observational studies. Lancet. Feb 16 2008;371(9612):569-78. 9. Duffy A, Capanu M, Abou-Alfa GK, et al. Gallbladder cancer (GBC): 10-year experience at Memorial Sloan-Kettering Cancer Centre (MSKCC). J Surg Oncol. Dec 1 2008;98(7):485-9. 10. NCCN Clinical Practice Guidelines in Oncology™. Available at www.nccn.org. 11. Okada K, Kijima H, Imaizumi T, et al. Wall-invasion pattern correlates with survival of patients with gallbladder adenocarcinoma. Anticancer Res. Feb 2009;29(2):685-91. 12. 10. Zarin M, Ahmed M, Gohar A, Waheed D, Khurram S, Aurangzeb M, et al. Incidence of Gall stones in carcinoma gallbladder patients. Pak J Surg 2005;21(1):19-22.
  • 41. 13. Hassan TJ, Zuberi SJ, Maqsood R. Carcinoma of gallbladder. J Pak Med Assoc 1978;28:33-4. 14. Mubarik A, Ahmed M, Khan AH, Mansoor A. Carcinoma of gallbladder - A study of 112 consecutive cases. Pak Armed Forces Med J 1990;43:1-7. 15. Yaqin HU, Parmar BK. A comparative study of biliary tract disease in Karachi (Pakistan) and Aylesbury (England). J Pak Med Assoc 1976;26(8):162-4. 16. Mohandas KM, Patil PS: Cholecystectomy for asymptomatic gallstones can reduce gall bladder cancer mortality in northern Indian women. Indian J Gastroenterology 2006, 25:147-151. 17. John AP, Ashley R, Alan G: Primary carcinoma of the gallbladder.HBP 1991, 4:277-289 18. Talat JH, Sarwar A J: Risk Factors for Gallbladder Cancer in Karachi.J Ayub Med Coll Abbottabad 2003. 19. Bhurgri Y, Bhugri A, Hassan SH: Cancer Incidents in Karachi Pakistan: First results from Karachi cancer registry. Int J Cancer 2000, 85:325- 9.