Objective

Gallbladder carcinoma (GBC) is one of the digestive cancers with poor prognosis, for which surgical resection is the only potentially curative therapy. Prognostic value of macroscopic inflammatory status of the resected gallbladder in patient with GBC has not been fully investigated. We retrospectively investigated the relation between macroscopic inflammatory status and disease-free as well as overall survival after radical resection for GBC.

Method

The subjects were 44 patients who underwent radical resection for GBC between January 2004 and April 2011 at Jikei University Hospital. We retrospectively investigated the relationship between clinicopathologic variables, including macroscopic inflammatory status and disease-free as well as overall survival.

Results

In univariate analysis, disease-free survival was poor in patients with Tumor-Nodes-Metastasis (TNM) stage ≥III (P < 0.0001) and positive vascular invasion (P = 0.0001). Patients with macroscopic chronic inflammation tended to have poor disease-free survival than those with normal type (P = 0.0930). Overall survival was poor in patients with TNM stage ≥III (P < 0.0001), presence of intraoperative blood transfusion (P = 0.0125), positive vascular invasion (P = 0.0055), and macroscopic chronic inflammation (P = 0.0281). In multivariate analysis, TNM stage ≥III (P < 0.0114) and macroscopic chronic inflammation (P = 0.0350) were independent predictors of disease-free survival. For overall survival, TNM stage ≥III (P = 0.0054) and macroscopic chronic inflammation (P = 0.0124) were the independent predictors. Moreover, macroscopic chronic inflammation correlated with the presence of gallstones.

Conclusion

The macroscopic Inflammation status of resected gallbladder cancer correlates with oncologic outcome in patients with GBC treated by radical resection.

Gallbladder carcinoma (GBC) is a cancer of the digestive tract with poor prognosis and is the most common cancer of the biliary tract. The prognosis of advanced GBC remains poor, even with recent advances in diagnostic modalities and surgical techniques.13  It is well known that surgical resection is the only treatment that can achieve long-term survival in patients with GBC. The prognosis of patients with early GBC is associated with a 5-year survival rate ranging from 90% to 100%.46  On the other hand, advanced GBC is characterized by a very poor prognosis, with the 5-year survival rate below 20%.7  Therefore, assessment of prognostic predictors is important for the management of patients with GBC.

Recent studies reported that perioperative findings of immunologic and inflammatory responses correlate with tumor recurrence and prognosis in various types of malignant tumor, including GBC.811  Several investigators have suggested that inflammatory cells and cytokines found in tumors are likely to contribute to tumor growth, progression, and immunosuppression.12,13  Preoperative C-reactive protein (CRP) concentrations may be related to poor tumor-specific survival in patients undergoing curative resection for colorectal cancer14  and pancreatic cancer.15 

Macroscopic chronic inflammation (MCI) is frequently observed in patients charring GBC. This condition reflects both acute and chronic inflammation of gallbladder. However, the association between MCI and prognosis in patients with GBC remains unclear. In this study, therefore, we retrospectively investigated the relation between macroscopic inflammation status of resected gallbladder and disease-free as well as overall survival in patients with GBC after radical resection.

Between January 2004 and December 2011, 56 patients underwent radical resection for GBC at the Department of Surgery, Jikei University Hospital, Tokyo, Japan. Of these, 12 patients were excluded, 3 patients for insufficient data, and 9 patients who were lost to follow-up, leaving the remaining 44 patients (20 male and 24 female; mean age: 68.0 years; range: 38–88 years) for this study. All patients underwent macroscopically curative resection for GBC. When the patient was diagnosed as GBC preoperatively, we performed open cholecystectomy or cholecystectomy with extended hepatectomy, liver bed resection, hepatic resection of segment 4a and segment 5 of Couinaud's classification, or right lobectomy according to depth of liver invasion in preoperative imaging. Lymph node and bile duct resection were performed when the regional lymph node metastasis was suspected by intraoperative histologic examination or preoperative diagnostic imaging. When the patient diagnosed as GBC incidentally after noncurative cholecystectomy, we performed additional hepatic resection with or without bile duct and lymph node resection. Of these, 3 patients underwent liver bed resection, one patient hepatic resection of segment 4a and segment 5 of Couinaud's classification, leaving 4 patients who could not undergo additional resection mainly for poor general condition or advanced age.

At first, we investigated the relationship between clinicopathologic variables and disease-free and overall survival after radical resection for GBC by univariate and multivariate analyses. The factors consisted of the following 11 criteria: age, gender, duration of operation, operative procedure, simple cholecystectomy or not, intraoperative blood loss, presence or absence of intraoperative blood transfusion, presence or absence of gallstones, tumor stage, vascular and or perineural invasion based on tumor pathology, maximum tumor diameter, and the macroscopic appearance of the resected gallbladder. Clinicopathologic continuous variables were classified into 2 groups for the log-rank test and the Cox proportional hazard regression model as follows: age < 60 or ≥ 60 years, duration of operation < 300 or ≥ 300 min, blood loss < 1,000 or ≥ 1,000 g, and tumor diameter < 50 or ≥ 50 mm. Tumor stage was classified into 2 groups: Tumor-Nodes-Metastasis (TNM) stage ≤ II or ≥ III. Vascular and or perineural invasion was defined by positive venous invasion, perineural invasion, or angiolymphatic invasion. The macroscopic appearance was classified into 2 groups: MCI and normal type (N). MCI was defined as wall thickening of the gallbladder and or adhesion with other organs including the duodenum, colon, or omentum. These classifications of tumor stage, vascular invasion, and the macroscopic appearance were based on the 5th Japanese edition of the General Rules for Surgical and Pathological Studies on Cancer of the Biliary Tract.16 

Next, to assess the risk factor for MCI, we analyzed the relationship between the patients' characteristics and the macroscopic appearance, using the following 9 factors: age, gender, duration of operation, intraoperative blood loss, intraoperative blood transfusion, presence or absence of gallstone, tumor diameter, vascular and or perineural invasion, and TNM stage.

Recurrence of GBC was defined as newly detected abdominal or extra-abdominal tumors by computed tomography or magnetic resonance image, with or without an increase in serum carcinoembryonic antigen (CEA) or carbohydrate antigen 19-9 (CA 19-9). For recurrence of GBC, chemotherapy or conversion to other chemotherapy were chosen based on performance status. For patients with poor performance status or refusal, best supportive care was given.

This retrospective study was approved by the Ethics Committee of the Jikei University School of Medicine (#21-121).

Data are expressed as a mean ± standard deviation (SD). Univariate analysis was performed using the non-paired Student's t test and chi-square test. Disease-free and overall survivals were analyzed using the log-rank test. Factors where P value was less than 0.1 were then used in the Cox proportional hazard model for multivariate analysis. These analyses were performed using STATA version 14. All P values were considered statistically significant when the associated probability was <0.05.

Patient characteristics and clinicopathologic variables

Patient characteristics and clinicopathologic variables are outlined in Table 1. Among the study population, the mean age was 67.4 years, with a range from 38 to 88 years, and 20 of them were male. Twenty-eight out of the 44 patients had TNM stage ≤II disease on tumor pathology. In this study, the 5-year disease-free and overall survival rates after elective resection of GBC were 51.4% (Fig. 1A) and 61.2% (Fig. 1B), respectively.

Comparison of clinical variables in relation to disease-free survival after radical resection of GBC

Table 2 lists the relationship between the clinicopathologic variables and disease-free survival after resection. In univariate analysis, disease-free survival was poor in patients who did not undergo simple cholecystectomy (P = 0.0319) and patients with TNM stage ≥III (P < 0.0001), and positive vascular and or perineural invasion (P = 0.0001). Patients with MCI tended to have poor disease-free survival than those with N, which did not achieve significant difference (P = 0.0930; Fig. 2A). In multivariate analysis, TNM stage ≥III (P < 0.0114) and MCI (P = 0.0350) were independent and significant predictors of poor disease-free survival.

Comparison of clinical variables in relation to overall survival after radical resection of GBC

Table 3 lists the relationship between the clinicopathologic variables and overall survival after resection. In univariate analysis, overall survival was poor in patients with TNM stage ≥III (P < 0.0001), intraoperative blood transfusion (P = 0.0125), positive vascular and or perineural invasion (P = 0.0055), and MCI (P = 0.0281; Fig. 2B). In multivariate analysis, TNM stage ≥III (P = 0.0054) and MCI (P = 0.0124) were independent and significant predictors of poor survival.

Univariate analysis of clinicopathologic variables in relation to the macroscopic appearance after radical resection of GBC

Table 4 lists the relationship between clinicopathologic variables and the macroscopic appearance. In univariate analysis, only the presence of gallstone correlated with MCI (P = 0.0316).

According to the Japanese registry of GBC, the resection rate and the curative resection rate in Japan are reported as 69.8% and 37.7%, respectively.7  Recently, reported prognostic factors associated with good outcome in patients with GBC included early TNM stage, extent of surgical resection, microscopic curative resection, negative perineural invasion, well-differentiation, adenocarcinoma, age <70 years, and female gender.1719  The presence of preoperative inflammation has also been reported as an independent prognostic factor for poor survival in patients with GBC.20 

MCI is characterized by features such as wall-thickening of the gallbladder, adhesions with other organs and so on,16  and the appearance reflects long-term inflammatory response of the gallbladder. In the present study, the macroscopic appearance was shown to be an independent factor of disease-free survival and a significant and independent prognostic factor of overall survival. Moreover, the macroscopic appearance of resected gallbladder correlated with the presence of gallstone, but not with the other factors including TNM stage. These results suggest that GBC with long-term inflammation have poor prognosis after resection, compared to that without inflammation. Chronic inflammation and cholelithiasis are correlated with cancer generation in GBC.2123  It has been presumed that longstanding chronic inflammation caused by cholelithiasis plays a role in the tumor progression, and that gallstones are regarded as a co-morbid condition in 54%–97% of the patients of GBC.24  Coussens et al reported that the host inflammatory response in the form of cytokines and other chemical messengers plays an important role in cancer growth and metastasis.25  At the molecular level, it has been shown that chronic inflammation of the gallbladder may lead to an allele-specific mutation, particularly loss of heterozygosity of the p53 gene and excessive expression of p53 protein, which may result in malignant transformation.26,27  However, there are a lot of cases in which GBC was generated without inflammation. In this study, a remarkable new finding is that the GBC developed in the condition with chronic cholecystitis has worse prognosis than those developed in the normal gallbladder. This result means consecutive inflammation or past inflammation in gallbladder generates relatively aggressive cancer with high metastatic potential. However, the reason for that is unclear.

Recent studies showed preoperative inflammation is associated with poor prognosis in GBC.11,20,28  Glasgow Prognostic Score (GPS), neutrophil to lymphocyte ratio (NLR), or CRP were shown to be one of prognostic predictors in the patient with GBC. However, MCI reflects not only preoperative acute inflammation but also chronic or past inflammation. Therefore, MCI in pathologic finding may be a new possible marker that predicts the prognosis of the GBC patient.

In the present study, the number of patients was 44, which was a small sample size. Therefore, we could not perform further analysis according to each pathologic stage or include details of an operative procedure such as hepatectomy, bile duct resection, or lymph node dissection. That is a major limitation of this study. Because survival benefit of adjuvant chemotherapy has not been established on gallbladder cancer after surgery,29  further assessments of correlation between inflammation and cancer recurrence by multicenter trial may improve therapeutic outcome of GBC after curative resection.

The macroscopic appearance of the resected gallbladder positively correlates with tumor recurrence and survival in patients with GBC after resection. Macroscopic inflammatory status of the resected gallbladder may help risk stratification and decision-making in the management of patients with GBC after radical resection.

1. 
Zhu
AX,
Hong
TS,
Hezel
AF,
Kooby
DA.
Current management of gallbladder carcinoma
.
Oncologist
2010
;
15
(2)
:
168
181
.
Google Scholar
 
2. 
Chijiiwa
K,
Kai
M,
Nagano
M,
Hiyoshi
M,
Ohuchida
J,
Kondo
K.
Outcome of radical surgery for stage IV gallbladder carcinoma
.
J Hepatobiliary Pancreat Surg
2007
;
14
(4)
:
345
350
Google Scholar
 
3. 
Liu
C,
Berger
NG,
Rein
L,
Tarima
S,
Clarke
C,
Mogal
H
et al
Gallbladder carcinoma: an analysis of the national cancer data base to examine hispanic influence
.
J Surg Oncol
2018
;
117
(8)
:
1664
1671
Google Scholar
 
4. 
Toyonaga
T,
Chijiiwa
K,
Nakano
K,
Noshiro
H,
Yamaguchi
K,
Sada
M
et al
Completion radical surgery after cholecystectomy for accidentally undiagnosed gallbladder carcinoma
.
World J Surg
2003
;
27
:
266
271
Google Scholar
 
5. 
Kokudo
N,
Makuuchi
M,
Natori
T,
Sakamoto
Y,
Yamamoto
J,
Seki
M
et al
Strategies for surgical treatment of gallbladder carcinoma based on information available before resection
.
Arch Surg
2003
;
138
(7)
:
741
750
Google Scholar
 
6. 
Frena
A,
Guardia
G,
Martin
F.
Outcome of radical surgery for carcinoma of the gallbladder according to the tumor node metastasis and Japanese Society of Biliary Surgery stages
.
J Gastrointest Surg
2004
;
8
(5)
:
580
590
Google Scholar
 
7. 
Miyakawa
S,
Ishihara
S,
Horiguchi
A,
Takada
T,
Miyazaki
M,
Nagakawa
T.
Biliary tract cancer treatment: 5,584 results from the Biliary Tract Cancer Statistics Registry from 1998 to 2004 in Japan
.
J Hepatobiliary Pancreat Surg
2009
;
16
(1)
:
1
7
Google Scholar
 
8. 
Liu
Y,
Wang
ZX,
Cao
Y,
Zhang
G,
Chen
WB,
Jiang
CP.
Preoperative inflammation-based markers predict early and late recurrence of hepatocellular carcinoma after curative hepatectomy
.
Hepatobiliary Pancreat Dis Int
2016
;
15
(3)
:
266
274
Google Scholar
 
9. 
Aurello
P,
Tierno
SM,
Berardi
G,
Tomassini
F,
Magistri
P,
D'Angelo
F
et al
Value of preoperative inflammation-based prognostic scores in predicting overall survival and disease-free survival in patients with gastric cancer
.
Ann Surg Oncol
2014
;
21
(6)
:
1998
2004
Google Scholar
 
10. 
Suzuki
Y,
Okabayashi
K,
Hasegawa
H,
Tsuruta
M,
Shigeta
K,
Kondo
T
et al
Comparison of preoperative inflammation-based prognostic scores in patients with colorectal cancer
.
Ann Surg
2018
;
267
(3)
:
527
531
Google Scholar
 
11. 
Wu
XS1,
Shi
LB,
Li
ML,
Ding
Q,
Weng
H,
Wu
WG
et al
Evaluation of two inflammation-based prognostic scores in patients with resectable gallbladder carcinoma
.
Ann Surg Oncol
2014
;
21
:
449
457
Google Scholar
 
12. 
Balkwill
F,
Mantovani
A.
Inflammation and cancer: back to Virchow?
Lancet
2001
;
357
(9255)
:
539
545
Google Scholar
 
13. 
Roshani
R,
McCarthy
F,
Hagemann
T.
Inflammatory cytokines in human pancreatic cancer
.
Cancer Lett
2014
;
345
(2)
:
157
163
Google Scholar
 
14. 
Crozier
JE,
McKee
RF,
McArdle
CS,
Angerson
WJ,
Anderson
JH,
Horgan
PG
et al
Preoperative but not postoperative systemic inflammatory response correlates with survival in colorectal cancer
.
Br J Surg
2007
;
94
(11)
:
1028
1032
Google Scholar
 
15. 
Tingstedt
B,
Johansson
P,
Andersson
B,
Andersson
R.
Predictive factors in pancreatic ductal adenocarcinoma: role of the inflammatory response
.
Scand J Gastroenterol
2007
;
42
(6)
:
754
759
Google Scholar
 
16. 
Japanese Society of Biliary Surgery.
General Rules for Surgical and Pathological Studies on Cancer of the Biliary Tract. 6th ed
.
Tokyo
:
Kanehara
,
2013
17. 
Sakata
J,
Shirai
Y,
Wakai
T,
Ajioka
Y,
Hatakeyama
K.
Number of positive lymph nodes independently determines the prognosis after resection in patients with gallbladder carcinoma
.
Ann Surg Oncol
2010
;
17
:
1831
1840
Google Scholar
 
18. 
Feo
CF,
Cossu
ML,
Ginesu
GC,
Ginesu
GC,
Fancellu
A,
Scanu
AM.
Perineural infiltration as a prognostic factor in surgically treated gallbladder cancer A single center experience and literature review
.
Ann Ital Chir
2017
;
88
:
485
490
Google Scholar
 
19. 
Kayahara
M,
Nagakawa
T,
Nakagawara
H,
Kitagawa
H,
Ohta
T.
Prognostic factors for gallbladder cancer in Japan
.
Ann Surg
2008
;
248
(5)
:
807
814
Google Scholar
 
20. 
Han
HS,
Cho
JY,
Yoon
YS,
Ahn
KS,
Kim
H.
Preoperative inflammation is a prognostic factor for gallbladder carcinoma
.
Br J Surg
2011
;
98
(1)
:
111
116
Google Scholar
 
21. 
Kumar
S,
Kumar
S,
Kumar
S.
Infection as a risk factor for gallbladder cancer
.
J Surg Oncol
2006
;
93
(8)
:
633
639
Google Scholar
 
22. 
Hsing
AW,
Gao
YT,
Han
TQ,
Rashid
A,
Sakoda
LC,
Wang
BS
et al
Gallstones and the risk of biliary tract cancer: a population-based study in China
.
Br J Cancer
2007
;
97
(11)
:
1577
1582
Google Scholar
 
23. 
Ahrens
W,
Timmer
A,
Vyberg
M,
Fletcher
T,
Guénel
P,
Merler
E
et al
Risk factors for extrahepatic biliary tract carcinoma in men: medical conditions and lifestyle: results from a European multicentre case-control study
.
Eur J Gastroenterol Hepatol
2007
;
19
(8)
:
623
630
Google Scholar
 
24. 
Batra
Y,
Pal
S,
Dutta
U,
Desai
P,
Garg
PK,
Makharia
G
et al
Gallbladder cancer in India: a dismal picture
.
J Gastroenterol Hepatol
2005
;
20
(2)
:
309
314
Google Scholar
 
25. 
Coussens
LM,
Werb
Z.
Inflammation and cancer
.
Nature
2002
;
420
(6917)
:
860
867
Google Scholar
 
26. 
Wistuba
II,
Sugio
K,
Hung
J,
Kishimoto
Y,
Virmani
AK,
Roa
I
et al
Allele-specific mutations involved in the pathogenesis of endemic gallbladder carcinoma in Chile
.
Cancer Res
1995
;
55
(12)
:
2511
2515
Google Scholar
 
27. 
Wee
A,
Teh
M,
Raju
GC.
Clinical importance of p53 protein in gall bladder carcinoma and its precursor lesions
.
J Clin Pathol
1994
;
47
(5)
:
453
456
Google Scholar
 
28. 
Saqib
R,
Pathak
S,
Smart
N,
Nunes
Q,
Rees
J,
Finch Jones
M
et al
Prognostic significance of pre-operative inflammatory markers in resected gallbladder cancer: a systematic review
.
ANZ J Surg
2018
;
88
(6)
:
554
559
Google Scholar
 
29. 
Horgan
AM,
Amir
E,
Walter
T,
Knox
JJ.
Adjuvant therapy in the treatment of biliary tract cancer: a systematic review and meta-analysis
.
J Clin Oncol
2012
;
30
:
1934
1940
Google Scholar
 
2022