Gastric Cancer Open Access
Copyright ©The Author(s) 2002. Published by Baishideng Publishing Group Inc. All rights reserved.
World J Gastroenterol. Oct 15, 2002; 8(5): 787-791
Published online Oct 15, 2002. doi: 10.3748/wjg.v8.i5.787
Mutation analysis of APC gene in gastric cancer with microsatellite instability
Dian-Chun Fang, Yuan-Hui Luo, Shi-Ming Yang, Xiao-An Li, Xian-Long Ling, Li Fang, Department of Gastroenterology, Southwest Hospital, Third Military Medical University, Chongqing 400038, China
Author contributions: All authors contributed equally to the work.
Supported by the National Natural Science Foundation of China, No.30070043, and “10.5” Scientific Research Foundation of Chinese PLA, No.01Z075.
Correspondence to: Dian-Chun Fang, M.D., Ph.D. Southwest Hospital, Third Military Medical University, Chongqing 400038, China. fangdianchun@hotmail.com
Telephone: +86-23-68754624 Fax: +86-23-68754124
Received: March 13, 2002
Revised: April 22, 2002
Accepted: April 29, 2002
Published online: October 15, 2002

Abstract

AIM: To evaluate the role of APC mutation in gastric carcinogenesis and to correlate APC mutation with microsatellite instability (MSI) in gastric carcinomas.

METHODS: APC mutation was measured with multiplex PCR, denaturing gradient gel electrophoresis and DNA sequencing; and MSI was analyzed by PCR-based methods.

RESULTS: Sixty-eight cases of sporadic gastric carcinoma were studied for APC mutation at exon 15 and MSI. APC mutaions were detected in 15 (22.1%) gastric cancers. Frequence of APC mutation (33.3%) in intestinal type of gastric cancer was significantly higher than that in diffuse type (13.1%, P < 0.05). On the contrary, no association was observed between APC mutation and tumor size, differentiation, depth of invasion, metastasis or clinical stages. Using five microsatellite markers, MSI in at least one locus was detected in 17 of 68 (25%) of the tumors analyzed. APC mutations were all detected in MSI-L (only one locus, n = 9) or MSS (tumor lacking MSI or stable, n = 51), but no mutation was found in MSI-H (≥ 2 loci, n = 8).

CONCLUSION: APC mutation is involved in carcinogenesis of intestinal type of gastric cancer and is independent of MSI phenotype but related to the LOH pathway in gastric cancer.


INTRODUCTION

The mechanisms of carcinogenesis in the gastric mucosa remain unclear. Adenomatous polyposis coli or APC, has been characterized as a tumor suppressor gene and considered a “gatekeeper” because alterations in this gene occur as an early event in the neoplastic transformation[1-3]. The APC gene was first identified in the germline of individuals with the condition known as familial adenomatous polyposis or FAP[4] and has been shown to play a role in the developmemt of sporadic colorectal cancer[5,6]. Studies have attempted to characterize the mutation of APC in sporadic gastric cancer[7-10] and in a limited number of familial gastric cancer[11,12]. It has been found that inactivation of APC plays a role in the development of some gastric cancers, particularly very well differentiated adenocarcinomas and signet-ring cell carcinomas[13,14], and that the mutations of the APC gene, similar to those in colorectal tumorigenesis, occur during the early stages of gastric adenoma development[15,16].

Genetic instability is strongly involved in neoplastic transformation and progression[17]. In gastrointestinal carcinomas, such genetic instability may be classified into two different forms in which hypermutability occurs either by means of chromosomal instability or microsatellite instability (MSI)[18-23]. MSI represents an important new form of genetic alteration characterized by widespread instability in repetitive nucleotide sequences. MSI has been found in the majority of tumors associated with hereditary non-polyposis colorectal cancer (HNPCC)[24,25] in which germ-line mutation occurs within the mismatch repair genes hMSH2, hMLH1, hPMS2 or hMSH6[26-28]. Mutations of the transforming growth factor type β receptor gene (TGF-βRII), and BAX gene are strongly correlated with MSI[29-31]. MSI is also a distinctive feature in about 10%-15% of sporadic colorectal tumors and to a varying degree in tumors of other organs, including the stomach[32-34]. Although mutations of APC have been reported in gastric cancer, less clear, however, is the relevance of APC mutation as a potential factor in MSI-positive gastric cancer. The aim of the present study is to correlate APC mutation with MSI in gastric carcinomas.

MATERIALS AND METHODS
Tissue samples

Sixty-eight cancer and corresponding normal tissues were obtained from surgically resected gastric carcinoma in Southwest Hospital. Each specimen was frozen immediately and stored at -80 °C until analyzed. A 5 μm section was cut from each tissue and stained with hematoxylin/eosin in order to confirm whether the cancer cells in tissues were predominant or not. Genomic DNA was isolated by standard proteinase-K digestion and phenol-chloroform extraction protocols. Of the 68 patients with gastric cancer, 45 were men and 23 were women with an age range of 30-76 years (mean age of 56.2 years at diagnosis). None of the patients included in the present series had a family history suggestive of HNPCC and had received chemotherapy or radiation therapy.

Multiplex PCR

Multiplex PCR was utilized in order to visualize the product of several regions simultaneously. Singleplex PCR was also used to help confirm cases and for regions that were difficult to amplify. Multiplex PCR analysis of APC exon 15 was performed using primers with a GC clamp (Table 1). Genomic DNA (100-400 ng), 0.25 μM primer for multi-primer reaction, 1 × buffer, 1.5 mM MgCl2, 0.25 mM of each dNTPs, and 0.1 U/μL Amplitaq Gold were combined in 10 μL reaction. The PCR reaction consisted of a denaturation step at 95 °C for 12 min followed by 32 cycles of 40 s at 94 °C, 60 s at 49 °C, and 90 s at 72 °C. Elongation occurred through 10 min at 72 °C, 10 min at 98 °C, 30 min at 50 °C and 30 min at 37 °C.

Table 1 Primer Sequences used in APC mutation analysis.
ExonGC ClampPrimer SequencesSize (bp)
15.12/0F-TTCAGGCAAATCCTAAGAGA/R-TTGAGCCAGGAGACATAATA329
15.20/2F-GGAATCTCATGGCAAATAGG/R-TCATCATGTCGATTGGTGTC284
15.32/0F-AGCAAAGTCTCTATGGTGAT/R-TGACACTTCTTCCATGACTT387
15.40/2F-CTACCATCCAGCAACAGAAA/R-TGGCATAAGGCATAGAACAT312
15.52/0F-AAGCTCTGCTGCCCATACAC/R-CTAGGTCGGCTGGGTATTGA282
15.62/5F-CTTATGCCAAATTAGAATAC/R-ACTGCTCATCTGAATATTTA306
15.77/5F-ATGATGGAGAACTAGATACA/R-ATCAGTGCTCTCAGTATAAA253
15.82/5F-AAGACCCAAACACATAATAG/R-TAATTGGTAGGCTTATCATC327
15.92/0F-AAATCGAGTGGGTTCTAATC/R-TTCTCACTGCTTGAAGACAT355
15.102/6F-CAGCCTATTGATTATAGTTT/R-AACATATTGGAGTATCTTCT344
15.112/0F-TTAACCAAGAAACAATACAG/R-CTTCGCTCACAGGATCTT320
15.122/0F-GGAAGCAGATTCTGCTAATA/R-ATAGTGTTCAGGTGGACTTT287
15.132/5F-AGAATCAGCCAGGCACAAAG/R-CATGGTTTGTCCAGGGCTAT310
15.142/6F-TGGTAAGTGGCATTATAAGC/R-AGTATCAGCATCTGGAAGAA279
15.155/2F-AAACCAAGCCAGAAGTACCT/R-AGGCTGCTCTGATTCTGTTT335
15.162/5F-CGATGAGCCATTTATACA/R-TTTGCTTTACGTGATGAC291
15.174/2F-ATTATTTCTGCCATGCCAAC/R-TTCGATTGTTAGATCACTTA300
15.182/6F-TGCCACGGGTGTATTGTGTT/R-TTTCCCTTTGGGCATAGCAG351
15.194/2F-GGTGATATTCTTGCAGAATG/R-CACGTGTCCTATATTCAGTA250
15.202/0F-GAAACCAACTTCACCAGTAA/R-AATAGGCGTGTAATGATGAG378
15.212/0F-AGCTCCCAAATAATGAAGAT/R-GATTGTTGGTTGGAGGTTAG342
15.222/6F-GCTAAAGTTACCAGCCACAC/R-TTGGTCAATGTCACTGAGAG
15.232/0F-CCAGTCATCCAAAGACATAC/R-CAACAGGTCATCTTCAGAGT
15.242/5F-TCACAGGGAGAACCAAGTAA/R-TTTGCACCTTCCTGAATAGC
15.252/3F-ATGGGTGGCATATTAGGTGA/R-TCGTGGGCCTTTATTACTTG
GC clamp: 1 = CGCCCGCCGCGCCCCGCGCCCGTCCCGCCGCCCCCGCCCG; 2 = CGCCCGCCGCGCCCCGCGCCCGGCCCGCCGCCCCCGCCCG; 3 = CG; 4 = GCGCG; 5 = CGTCCCGC; 6 = GCGCCCGTCCCGCCC; 7 = CGCCCGCCGCGCCCCGCGCCCGTCCCGCCGCCCCCGCCCGGCCCG
Denaturing gradient gel electrophoresis (DGGE)

DGGE analysis was performed for scanning mutations at 15 exon of APC gene. Eight μL of each sample was loaded on the gels consisting of 10% polyacrylamide and 10%-60% urea-formamide. The gels were run at 90 V for 17 h in tanks of buffer at 50 °C. Gels were stained with 0.5 × Sybr Green I and Sybr Green II for 20 min and visualized by UV transillumination. Heteroduplex samples were further analyzed by manual sequencing.

Manual sequencing

Samples were amplified for sequencing with PCR primers that did not include the GC clamp (Appendix A). The PCR reaction included 200-400 ng of genomic DNA, 0.25 μM primer, 1 × buffer, 1.5 mM MgCl2, 0.25 mM of each dNTPs, and 2.5 U Amplitaq Gold were combined in a 10 μL reaction. The PCR reaction consisted of a denaturation step at 94 °C for 3 min followed by 35 cycles of 60 s at 94 °C, 60 s at 55 °C, and 60 s at 72 °C. A final extension step included 10 min at 72 °C. 1.5% agarose gels were run at 150 V to confirm the existence of PCR product. The product was purified following the instructions of the Wizard PCR Preps DNA Purification System (Promega, Madison, WI). Following the purification process, the product was run on a 1.5% agarose gel at 150 V to verify the product. Sequencing was performed following the instruction of the system. The film was read independently by two individuals according to the APC sequence.

MSI detection

MSI analyses included five microsatellite markers: BAT25, BAT26, BAT40, D2S123, and D5S346. PCR was performed as previously described[35]. MSI was defined as the presence of band shift in the tumor DNA that was not present in the corresponding normal DNA. Based on the number of mutated MSI markers in each tumor, carcinomas were characterized as MSI-H if they manifested instability at two or more markers, MSI-L if unstable at only one marker, and MSS if they showed no instability at any marker.

Statistical analysis

Chi-square test with Yates’ correction was used. A P value < 0.05 was considered significant.

RESULTS

Multiplex PCR and DGGE were used to scan the mutation at the exon 15 of APC in 68 gastric cancers (Figure 1). The samples that showed alterations by DGGE were further analyzed through munual sequencing (Figure 2). APC mutaions were detected in 15 samples (22.1%) held APC mutations that lead to premature protein truncation (Table 2). The truncation of the protein occurred as a result of a stop codon created through a base pair change, an insertion, or a deletion.

Figure 1
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Figure 1 Abnormal four-band patterns in lane 5 after multiplex PCR and denaturing gradient gel.
Table 2 APC mutation in 12 gastric carcinomas.
Exon regionNucleotide alterationNucleotide locationCodon number
15.4C→A2883940
15.5insA2866935
15.10del A3835 or 38361258
15.11del AAAA39811307
15.12del AAAGA39881309
15.12G→T40101317
15.13delT41461362
15.13delGT42541398
15.13delT42821407
15.14C→T44101450
15.14G→T44521464
15.15delAG44551465
15.19insCT53261755
15.21insT55961845
15.22delG59401960
Figure 2
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Figure 2 DNA sequencing shows a G→T change at 1464 coden.

We compared mutation of exon 15 of APC gene in gastric cancer with various clinicopathological parameters including tumor size, differentiation, TNM status, clinical stage and Lauren’s types. Table 3 shows the association of mutations of APC to the clinicopathological parameters of 68 gastric carcinomas. Mutations of APC gene were observed more common in intestinal type than in diffuse type tumors (P < 0.05).

Table 3 The relationship between the APC mutation and clinicopathological parameters.
ParametersNo. of casesAPC mutation
Size
< 5 cm317
> 5 cm378
Differentiation
Well144
Moderate206
Poor283
Mucinous62
Lauren classification
Intestinal type3010a
Diffuse type385
Serosal invasion
Absent306
Present389
Metastasis
Absent338
Present357
Clinical stage
I and II369
III and IV326
aP < 0.05 vs diffuse type

Alterations of electrophoretic patterns of PCR products of five microsatellite markers were compared between tumor and normal DNA in each patient. MSI affecting at least one locus was observed in 17 (25%) of 68 tumors, among which eight (11.8%) were MSI-H, nine (13.2%) were MSI-L, and fifty-one (75%) were MSS. Table 4 shows the association of mutations of APC to MSI of 68 gastric carcinomas. Three mutations were found in 9 tumors with MSI-L and 12 were found in 51 tumors with MSS, and no mutation was found in 8 tumors with MSI-H.

Table 4 The relationship between MSI and APC mutation.
MSI statusNo. of casesAPC mutation
MSI-H80
MSI-L92
MSS5113
DISCUSSION

Mutations of APC gene has been shown to play an important role in colorectal tumorigenesis. A germline mutation in APC contributes significantly to the development of colitis-associated neoplasia[36]. In the current study, we investigated mutations of the APC gene in 68 gastric carcinomas obtained surgically. Mutations at exon 15 of APC gene were detected in 22.1% of gastric cancers. This finding is similar to the previous studies[14,15]. This proportion may be an underestimate because the mutation of exons 1 through 14 were not detected in this study. Previous investigations have found that the 5’ half of APC holds the majority of the germline mutations[3,37]. The mutations identified in the study were spread throughout the exon 15 of APC sequence. Sequencing analysis confirmed that the mutations resulted in truncation of the gene products or in an amino acid change. The APC gene encodes a large protein with multiple cellular functions and interactions. Mutations in this gene would lead to alterations in signal transduction of cell, differentiation, mediation of intercellular adhesion, stabilization of the cytoskeleton and possibly regulation of the cell cycle and apoptosis[38,39]. Our results imply that APC plays a crucial role in gastric carcinogenesis, as was observed in colorectal carcinogenesis.

In the current study, we did not find an obvious relationship between the APC mutation and tumor size, depth of invasion, node metastasis or clinical stages, indicating a limited role of the APC mutation in predicting prognosis of gastric carcinomas. This finding is in agreement with the recently published data on cholangiocarcinoma and breast cancer[40,41]. Gastric carcinomas can be divided into "intestinal" type and "duffuse" type. The intestinal type of gastric cancer is the predominant type in elderly population at high risk and preceded by well-defined precancerous lesions, such as intestinal metaplasia and atrophic gastritis. The diffuse type is relatively more frequent in low risk populations and is not as often preceded by intestinal metaplasia. A distinct genetic pathway exists in gastric carcinogenesis of different histological subtypes and their tumor progression[42-45]. Increased beta-catenin mRNA levels and mutational alterations of the APC and beta-catenin gene were present in intestinal type gastric cancer[46,47], whereas epigenetic inactivation of E-cadherin via promoter hypermethylation may be an early critical event in the development of undifferentiated tumors[48-51]. In this study, marked difference in APC mutation was noted in gastric cancer by histological type. APC mutations were significantly more frequent in intestinaltype gastric cancers as compared with diffusetype gastric cancers, suggesting that APC gene is not only a predisposing gene in colorectal cancer but also a predisposing gene in intestinal type of gastric cancer. The mutation of APC gene may be considered makers for intestinal or colonic differentiation. The mutation of APC in the majority of intestinal type cancers also supports the theory that these cancers result from transformation of intestinal metaplasia.

There is evidence that MSI cancer comprises distinctive MSI-H and MSI-L categories[14]. MSI-H cancers are distingushed clinicopathologically and in their spectrum of genetic alterations from cancers showing MSI-L and MSS cancers[14]. Our previous studies indicated that MSI-H gastric cancers often show lower frequency of LOH of APC, MCC and DCC genes than do MSI-L and MSS cancers[1]. In present study, 15 APC mutations were all detected in MSI-L and MSS, but no mutation was found in those showing MSI-H. This result indicates that APC is mutational target in MSI-L and MSS tumor cells and support the notion that APC mutation-positive tumors may identify an alternative pathway which is probably different from MSI-related phenomenon observed in HNPCC. Our analysis of APC mutation should further provide some clues to the molecular mechanisms underlying the profound genomic instability in the MSI and LOH pathway for gastric carcinoma.

Footnotes

Edited by Ma JY

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