Loss of Heterozygosity on the Short Arm of Chromosome 3 in Cervical Intra-Epithelial Neoplasia without Concomitant Cervical Carcinoma

Fouret, Pierre; Dabit, Dominique; Mergui, J.-L.; Uzan, Serge

doi:10.1159/000028038

Cited by 15 publications

(12 citation statements)

References 14 publications

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“…In a cervical-cancer cell line, integrated HPV DNA has been identified at a fragile site FRA3B within the FHIT locus (Greenspan et al, 1997). Our data indicate the important role of 3p deletion, a ''high-risk''-HPV-typeassociated genetic event, in the development of cervical cancer, as supported by the observation of 3p deletion in pre-cancerous lesions of cervical cancer (Wistuba et al, 1997;Fouret et al, 1998).…”

Section: Discussionsupporting

confidence: 78%

“…This present analysis of LOH at 3p and 5p in relation to ''high-risk'' HPV types 16/18 is of special interest. We have reported a common region of deletion at 5p both in pre-cancerous and in cancerous lesions (Mitra et al, 1995), and deletions have also been reported at 3p in pre-cancerous lesions of cervical carcinoma (Wistuba et al, 1997;Fouret et al, 1998). In view of the present data and other reported observations, it seems likely that multiple genetic events, such as deletion/mutation at 3p and 5p in association with HPV infection, are relevant in the development of cervical cancer.…”

Section: Discussionsupporting

confidence: 74%

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Genetic deletion and human papillomavirus infection in cervical cancer: Loss of heterozygosity sites at 3p and 5p are important genetic events

Mitra

1999

Int. J. Cancer

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''High-risk'' human papillomavirus (HPV) types 16/18 are recognized as being associated with cervical cancer. We have already reported frequent loss of heterozygosity (LOH) at 3p, 3q, 4q, 5p and 5q in primary cervical cancer, the frequency at these sites ranging from 31.0 to 56.3%. The present analysis deals with these frequent-deletion sites in relation to HPV infection. HPV Cancer of the uterine cervix is associated with human papillomavirus (HPV) infection. E6/E7 oncoprotein encoded by ''high-risk'' HPV types has been shown to interact with the tumour-suppressor gene p53/pRB, causing abnormal cell-cycle regulation. Thus, HPV infection appears to play an important role in cervical carcinogenesis, though HPV infection alone might not be capable of developing cervical cancer. Further, even the cases which show such development generally need a long latent period between the initial infection and the subsequent development of invasive cervical cancer. The precise mechanism of the role played by HPV remains controversial (zur Hausen, 1994). Genomic deletions are now considered to be an important factor in tumorigenesis. Cytogenetic studies, although limited, have revealed non-random chromosomal changes such as i (5p), deletion at 3p, 6q and 17p (Mitra et al., 1994b;Atkin, 1997), also a correlation between the common fragile sites and integration of HPV DNA (Cannizzaro et al., 1988;Popescu et al., 1990). Mutations or deletions of a tumoursuppressor gene (TSG) have been shown to be frequently accompanied by loss of the remaining allele, leading to homozygous inactivation of the gene (Marshall, 1991). Several molecular genetic studies (Mitra et al., 1994a;Mullokandov et al., 1996;Kersemaekers et al., 1998) have identified a few frequent loss of heterozygosity (LOH) sites, suggesting possible involvement of TSGs in the development of cervical cancer.The current study was undertaken to see (i) how far HPV infection in general is associated with genomic deletion in cervical cancer and (ii) whether any of the frequent LOH sites identified can be correlated with infection by ''high-risk'' HPV type 16/18. We have reported 11 LOH sites (Mitra et al., 1994a). Here, we present the results of detailed analysis of the more frequently observed LOH sites, namely, at 3p, 3q, 4q, 5p and 5q, in relation to HPV status. The study revealed strong evidence of HPV infection in cervical carcinomas. Deletion at 3p appeared dependent on HPV 16/18 infection, while deletion at 5p, the most frequent deletion site, was independent of ''high-risk'' HPV infection. MATERIAL AND METHODS SamplesA total of 53 tumour biopsies and their corresponding blood samples were collected at the cancer clinic, Lok Nayak hospital, Delhi, India. Tumours were histologically diagnosed as being invasive cervical carcinoma. DNA isolation and Southern-blot analysisStandard DNA extraction procedure was followed using the proteinase-K-phenol-alcohol method (Mitra et al., 1994a); 5 to 7 µg of each sample of DNA was digested with appropriate restriction enzymes, and the ...

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Section: Discussionsupporting

confidence: 78%

Section: Discussionsupporting

confidence: 74%

Genetic deletion and human papillomavirus infection in cervical cancer: Loss of heterozygosity sites at 3p and 5p are important genetic events

Mitra

1999

Int. J. Cancer

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“…Fouret et al [11] found loss of heterozygosity or MSI in 6 of 16 (38%) and 9 of 23 (39%) informative cases of cervical carcinoma at 3p13 and 3p21, respective-ly. Mitra et al [12] observed MSI in 6 (13%) of 46 cases of cervical carcinoma using 5 microsatellite loci (D5S392, D5S406, D5S208, D5S117 and D5S432) mapped to 5p.…”

Section: Discussionmentioning

confidence: 98%

Microsatellite Instability, Expression of hMSH2 and hMLH1 and HPV Infection in Cervical Cancer and Their Clinico-Pathological Association

Chung¹,

Cheung²,

Wang

et al. 2001

Gynecol Obstet Invest

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Infection with specific genotypes of human papillomavirus (HPV) has been strongly implicated in cervical carcinogenesis. However, HPV infection alone is insufficient for malignant transformation of the cervical epithelium. An alteration of microsatellite repeats is the result of slippage owing to strand misalignment during DNA replication and is referred to as microsatellite instability (MSI). These defects in DNA repair pathways have been related to human carcinogenesis; however, the role of MSI in the tumorigenesis of cervical cancer remains unclear. The clinical and pathological features of cervical cancers which are MSI-positive have also not been fully characterized. This study investigated the prevalence of MSI in cervical cancer and its relationship to clinico-pathological characteristics and HPV infection. Polymerase chain reaction-based microsatellite assay combined with tissue microdissection was used to examine for MSI in 50 cervical squamous cell carcinomas in Hong Kong women. In addition, the immunohistochemical staining was performed to determine the expression of major DNA mismatch repair genes, hMSH2 and hMLH1. Six cases (12%) displayed a low frequency of MSI (MSL-L) showing MSI at one locus only in 5 loci examined. Seven cases (14%) showed a high frequency of MSI (MSI-H) having MSI at 2 or more loci. Grouping MSI-L and MSI-H cases together as MSI-positive, statistical analysis of HPV infection, tumor grade, clinical stage and clinical status failed to disclose differences between MSI-positive and MSI-negative cases (p > 0.05). However, MSI-H correlated with advanced stage of disease (p < 0.05). Individuals with MSI-H tumors appeared to have reduced overall survival compared to individuals with MSI-L and MSI-negative tumors, but the difference was not statistically significant (p = 0.059). An absence of either MSH2 or MLH1 expression was observed in 2 MSI-L and 4 MSI-H cases, respectively. The results suggest that MSI is present in a subgroup of cervical squamous cell carcinomas, and defects resulting in MSI may be related to tumor progression and possibly poor prognosis in cervical cancer.

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“…Moreover, 3p and 6p were also involved at the early precancer stages and during progression of cervical intraepithelial neoplasia to invasive cervical cancer (Larson et al, 1997b;Wistuba et al, 1997;Fouret et al, 1998;Guo et al, 1998Guo et al, , 2000Guo et al, , 2001Umayahara et al, 2002). Different studies reported various 3p LOH rates in the range 50-76% (Wistuba et al, 1997;Braga et al, 1999;Guo et al, 2000;Helland et al, 2000;Herzog et al, 2001;Acevedo et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

Deletion mapping using quantitative real-time PCR identifies two distinct 3p21.3 regions affected in most cervical carcinomas

et al. 2003

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We report chromosome 3p deletion mapping of 32 cervical carcinoma (CC) biopsies using 26 microsatellite markers located in frequently deleted 3p regions to detect loss of heterozygosity and homozygous loss. In addition, two STS markers (NLJ-003 and NL3-001) located in the 3p21.3 telomeric (3p21.3T) and 3p21.3 centromeric (3p21.3C) regions, respectively, were used for quantitative real-time PCR as TaqMan probes. We show that quantitative real-time PCR is reliable and sensitive and allows discriminating between 0, 1 and 2 marker copies per human genome. For the first time, frequent (five of 32 cases, i.e. 15.6%) homozygous deletions were demonstrated in CCs in both 3p21.3T and 3p21.3C regions. The smallest region homozygously deleted in 3p21.3C was located between D3S1568 (CACNA2D2 gene) and D3S4604 (SEMA3F gene) and contains 17 genes previously defined as lung cancer candidate Tumor suppressor genes (TSG(s)). The smallest region homozygously deleted in 3p21.3T was flanked by D3S1298 and NL1-024 (D3S4285), excluding DLEC1 and MYD88 as candidate TSGs involved in cervical carcinogenesis. Overall, this region contains five potential candidates, namely GOLGA4, APRG1, ITGA9, HYA22 and VILL, which need to be analysed. The data showed that aberrations of either NLJ-003 or NL3-001 were detected in 29 cases (90.6%) and most likely have a synergistic effect (Po0.01). The study also demonstrated that aberrations in 3p21.3 were complex and in addition to deletions, may involve gene amplification as well. The results strongly suggest that 3p21.3T and 3p21.3C regions harbor genes involved in the origin and/or development of CCs and imply that those genes might be multiple TSG(s).

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Loss of Heterozygosity on the Short Arm of Chromosome 3 in Cervical Intra-Epithelial Neoplasia without Concomitant Cervical Carcinoma

Cited by 15 publications

References 14 publications

Genetic deletion and human papillomavirus infection in cervical cancer: Loss of heterozygosity sites at 3p and 5p are important genetic events

Genetic deletion and human papillomavirus infection in cervical cancer: Loss of heterozygosity sites at 3p and 5p are important genetic events

Microsatellite Instability, Expression of hMSH2 and hMLH1 and HPV Infection in Cervical Cancer and Their Clinico-Pathological Association

Deletion mapping using quantitative real-time PCR identifies two distinct 3p21.3 regions affected in most cervical carcinomas

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