High frequency of loss of heterozygosity in vulval intraepithelial neoplasia (VIN) is associated with invasive vulval squamous cell carcinoma (VSCC)

Rosenthal, Adam N.; Ryan, Andy; Hopster, Deborah J.; Surentheran, T.; Jacobs, Ian

doi:10.1002/ijc.1549

Cited by 21 publications

(24 citation statements)

References 18 publications

(22 reference statements)

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“…Indeed, few studies have previously examined the genetic changes associated with highgrade VIN using lower resolution techniques. One investigation (Rosenthal et al, 2001) reported that, of 6 loci (3p, 4q, 5p, 9p, 11p and 17p) examined for LOH using microsatellite marker analysis, 3p was the most frequently affected with LOH in 8 of 28 (29%) informative HPV-positive VIN3 samples, comparable to this study. Elsewhere, metaphase CGH was used to analyse the genetic events Reanalysed data from a previous study on cervical carcinomas (Scotto et al, 2008b).…”

Section: Comparison With Previous Studies On Vulval Neoplasiasupporting

confidence: 85%

“…Limited data are available on the genetic alterations associated with VSCC and VIN precursor lesions; previous studies have used microsatellite marker analysis and metaphase comparative genomic hybridisation (CGH) rather than higher resolution arraybased techniques (Pinto et al, 1999;Jee et al, 2001;Rosenthal et al, 2001;Allen et al, 2002;Micci et al, 2003;Bryndorf et al, 2004;Huang et al, 2005). In contrast, the genetic changes associated with CIN and CxSCC have been extensively studied, most recently using array-based methods (Hidalgo et al, 2005;Wilting et al, 2006Wilting et al, , 2009Choi et al, 2007;Kloth et al, 2007;Scotto et al, 2008a, b).…”

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confidence: 99%

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High-resolution genomic profiling of human papillomavirus-associated vulval neoplasia

et al. 2010

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BACKGROUND: The incidence of human papillomavirus-associated vulval neoplasia is increasing worldwide; yet the associated genetic changes remain poorly understood. METHODS: We have used single-nucleotide polymorphism microarray analysis to perform the first high-resolution investigation of genome-wide allelic imbalance in vulval neoplasia. Our sample series comprised 21 high-grade vulval intraepithelial neoplasia and 6 vulval squamous cell carcinomas, with paired non-lesional samples used to adjust for normal copy number variation. RESULTS: Overall the most common recurrent aberrations were gains at 1p and 20, with the most frequent deletions observed at 2q, 3p and 10. Copy-neutral loss of heterozygosity at 6p was a recurrent event in vulval intraepithelial neoplasia. The pattern of genetic alterations differed from the characteristic changes we previously identified in cutaneous squamous cell carcinomas. Vulval neoplasia samples did not exhibit gain at 5p, a frequent recurrent aberration in a series of cervical tumours analysed elsewhere using an identical protocol. CONCLUSION: This series of 27 vulval samples comprises the largest systematic genome-wide analysis of vulval neoplasia performed to date. Despite shared papillomavirus status and regional proximity, our data suggest that the frequency of certain genetic alterations may differ in vulval and cervical tumours.

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Section: Comparison With Previous Studies On Vulval Neoplasiasupporting

confidence: 85%

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confidence: 99%

High-resolution genomic profiling of human papillomavirus-associated vulval neoplasia

et al. 2010

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“…LOH autoradiographs from these samples were shown in our previous report. 7 Similarly, samples exhibiting Ͼ50% reduction in the intensity ratio of the VIN-or VSCC-modified androgen receptor alleles compared to unmodified alleles were classed as having skewed X-chromosome inactivation, indicative of a monoclonal origin. Examples are shown in Figure 1.…”

Section: Separation Visualisation and Interpretation Of Pcr Productsmentioning

confidence: 99%

“…These LOH frequencies were known from our previous study. 7 Where identical losses occurred at more than 1 locus in a sample pair, the odds of this occurring were calculated as the product of the probabilities for loss at each locus. The total probability of observing common losses in the different sample groups was calculated as the product of the probabilities of each sample in that group.…”

Section: Probability Analysismentioning

confidence: 99%

“…We then wanted to document the patterns of LOH events and X-chromosome inactivation in VSCC samples and contiguous and noncontiguous VIN, to examine whether VIN and VSCC could have arisen from the same clone. Because we had already studied the frequency of LOH at 6 chromosomal loci in lone VIN and VSCC, 7 it was possible to calculate the odds of identical losses occurring by chance in both VSCC and associated VIN. Finally, as primary cancers and their metastases are thought to have the same clonal origin, we compared the number of identical losses occurring in primaries and their metastases with the number of identical losses occurring in VSCC and associated VIN.…”

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confidence: 99%

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Molecular evidence of a common clonal origin and subsequent divergent clonal evolution in vulval intraepithelial neoplasia, vulval squamous cell carcinoma and lymph node metastases

Rosenthal

Ryan

Hopster

et al. 2002

Intl Journal of Cancer

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VIN is thought to be the precursor of some VSCCs because it is monoclonal, frequently occurs contiguously with VSCC and shares similar risk factors with a subgroup of VSCC. There has been no conclusive molecular evidence supporting this assumption. We performed X-chromosome inactivation analysis on 9 cases of lone VIN, 10 cases of VSCC and associated contiguous VIN and 11 cases of VSCC and associated noncontiguous VIN. Eight of the 9 cases of lone VIN appeared to be monoclonal. All 7 informative and monoclonal cases of VIN with contiguous VSCC and 6/9 informative cases of VIN with noncontiguous VSCC showed patterns of X-chromosome inactivation consistent with a common monoclonal origin for both VIN and VSCC. Two of the 9 cases of VIN with noncontiguous VSCC showed X-chromosome inactivation patterns consistent with a separate clonal origin. We performed LOH analysis at 6 chromosomal loci on these samples and 7 cases with lymph node metastases. Identical losses occurred 7 times in VIN and contiguous VSCC (random probability 1.2 ؋ 10 -9 ), twice in VIN and noncontiguous VSCC (random probability 1.5 ؋ 10 -3 ) and 3 times in VSCC and associated metastases (random probability 1.8 ؋ 10 -5 ). Some losses occurring in VSCC did not appear in the contiguous VIN or associated metastases and vice versa. These data provide molecular evidence that VIN is the precursor of VIN-associated VSCC, that multifocal disease may arise via either different clones or a single clone and that continued divergent clonal evolution may occur in vulval neoplasia. © 2002 Wiley-Liss, Inc. Key words: vulval intraepithelial neoplasia; vulval cancer; loss of heterozygosity; X-chromosome inactivation; vulval squamous cell carcinomaVIN has long been thought to be a premalignant condition that may progress to invasive VSCC. This assumption is based on observations that VIN frequently occurs contiguously with VSCC, 1 that VIN and a subgroup of VSCC are associated with similar risk factors (smoking, 2 immunosuppression 3 and HPV infection 2,4 ) and that VIN and VSCC are monoclonal neoplastic conditions. 5,6 Confirmation of this hypothesis is important for gaining insight into the process of vulval carcinogenesis. Furthermore, identifying molecular markers for risk of progression of VIN to VSCC is possible only if molecular evidence is compatible with a common monoclonal origin of the 2 conditions. We first wanted to confirm that VIN is a monoclonal condition. We then wanted to document the patterns of LOH events and X-chromosome inactivation in VSCC samples and contiguous and noncontiguous VIN, to examine whether VIN and VSCC could have arisen from the same clone. Because we had already studied the frequency of LOH at 6 chromosomal loci in lone VIN and VSCC, 7 it was possible to calculate the odds of identical losses occurring by chance in both VSCC and associated VIN. Finally, as primary cancers and their metastases are thought to have the same clonal origin, we compared the number of identical losses occurring in primaries and their metastases with the...

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A pre‐existing coordinated inflammatory microenvironment is associated with complete response of vulvar high‐grade squamous intraepithelial lesions to different forms of immunotherapy

Abdulrahman

Miranda

Hellebrekers

et al. 2020

Intl Journal of Cancer

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Immunotherapy of vulvar high-grade squamous intraepithelial lesion (vHSIL) is investigated as an alternative for surgery, because of high comorbidity and risk of recurrence. Limited evidence exists on the role and composition of the immune microenvironment in current immunotherapeutic approaches for vHSIL. The vHSIL of 29 patients biopsied before treatment with imiquimod were analyzed by two multiplex seven-color immunofluorescence panels to investigate the pre-existing T-cell and myeloid cell composition in relation to treatment response. The samples were scanned with the Vectra multispectral imaging system. Cells were automatically phenotyped and counted with inForm advanced image analysis software. Cell counts and composition were compared to that of vHSIL patients before therapeutic vaccination (n = 29) and to healthy vulva (n = 27). Our data show that the immune microenvironment of complete responders (CR) to imiquimod resembled the coordinated infiltration with type 1 CD4 + and CD8 + T cells and CD14 + inflammatory myeloid cells also found in healthy vulva. However, more CD8 + T cells and FoxP3 + regulatory T cells were present in CR. The lesions of partial responders (PR) lacked such a coordinated response and displayed an impaired influx of CD14 + inflammatory myeloid cells. Importantly, complete responses after imiquimod or

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High frequency of loss of heterozygosity in vulval intraepithelial neoplasia (VIN) is associated with invasive vulval squamous cell carcinoma (VSCC)

Cited by 21 publications

References 18 publications

High-resolution genomic profiling of human papillomavirus-associated vulval neoplasia

High-resolution genomic profiling of human papillomavirus-associated vulval neoplasia

Molecular evidence of a common clonal origin and subsequent divergent clonal evolution in vulval intraepithelial neoplasia, vulval squamous cell carcinoma and lymph node metastases

A pre‐existing coordinated inflammatory microenvironment is associated with complete response of vulvar high‐grade squamous intraepithelial lesions to different forms of immunotherapy

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