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      Circulating human papillomavirus DNA detected using droplet digital PCR in the serum of patients diagnosed with early stage human papillomavirus‐associated invasive carcinoma

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          Abstract

          Specific human papillomavirus genotypes are associated with most ano‐genital carcinomas and a large subset of oro‐pharyngeal carcinomas. Human papillomavirus DNA is thus a tumour marker that can be detected in the blood of patients for clinical monitoring. However, data concerning circulating human papillomavirus DNA in cervical cancer patients has provided little clinical value, due to insufficient sensitivity of the assays used for the detection of small sized tumours. Here we took advantage of the sensitive droplet digital PCR method to identify circulating human papillomavirus DNA in patients with human papillomavirus‐associated carcinomas.

          A series of 70 serum specimens, taken at the time of diagnosis, between 2002 and 2013, were retrospectively analyzed in patients with human papillomavirus‐16 or human papillomavirus‐18‐associated carcinomas, composed of 47 cases from the uterine cervix, 15 from the anal canal and 8 from the oro‐pharynx. As negative controls, 18 serum samples from women with human papillomavirus‐16‐associated high‐grade cervical intraepithelial neoplasia were also analyzed. Serum samples were stored at −80°C (27 cases) or at −20°C (43 cases). DNA was isolated from 200 µl of serum or plasma and droplet digital PCR was performed using human papillomavirus‐16 E7 and human papillomavirus‐18 E7 specific primers.

          Circulating human papillomavirus DNA was detected in 61/70 (87%) serum samples from patients with carcinoma and in no serum from patients with cervical intraepithelial neoplasia. The positivity rate increased to 93% when using only serum stored at −80°C. Importantly, the two patients with microinvasive carcinomas in this series were positive. Quantitative evaluation showed that circulating viral DNA levels in cervical cancer patients were related to the clinical stage and tumour size, ranging from 55 ± 85 copies/ml (stage I) to 1774 ± 3676 copies/ml (stage IV).

          Circulating human papillomavirus DNA is present in patients with human papillomavirus‐associated invasive cancers even at sub‐clinical stages and its level is related to tumour dynamics. Droplet digital PCR is a promising method for circulating human papillomavirus DNA detection and quantification. No positivity was found in patients with human papillomavirus‐associated high grade cervical intraepithelial neoplasia.

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          Natural history and epidemiology of HPV infection and cervical cancer.

          Xavier Castellsagué (2008)
          Cervical cancer is the most common cancer affecting women in developing countries. It has been estimated to have been responsible for almost 260 000 deaths annually, of which about 80% occurred in developing countries. Persistent infection by certain oncogenic HPV types is firmly established as the necessary cause of most premalignant and malignant epithelial lesions of the cervix and of a variable fraction of neoplastic lesions of the vulva, vagina, anus, penis, and oropharynx. There are more than 100 known HPV genotypes, at least 15 of which can cause cancer of the cervix and other sites. HPV 16 and 18, the two most common oncogenic types, cause approximately 70% of all cervical cancers worldwide. HPV, especially genotypes 6 and 11, can also cause genital warts. HPV is highly transmissible and it is now considered the most common sexually transmitted infection in most populations. Although most women infected with the virus become negative within 2 years, women with persistent high-risk HPV infections are at greatest risk for developing cervical cancer. Since the identification of HPV as the necessary cause of cervical cancer, HPV-based technology has become the centre of novel primary and secondary cervical cancer prevention strategies by the introduction of HPV testing in screening and of HPV vaccines in preadolescent girls and young women. If implemented widely and wisely the deployment of these protocols has the potential to complete Papanicolaou's goal of cervical cancer eradication by extending the benefits of prevention to the developing populations of the world.
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            Serial assessment of human tumor burdens in mice by the analysis of circulating DNA.

            Carlo Rago, David L. Huso, Frank Diehl (2007)
            Internal human xenografts provide valuable animal models to study the microenvironments and metastatic processes occurring in human cancers. However, the use of such models is hampered by the logistical difficulties of reproducibly and simply assessing tumor burden. We developed a high-sensitivity assay for quantifying human DNA in small volumes of mouse plasma, enabling in-life monitoring of systemic tumor burden. Growth kinetics analyses of various xenograft models showed the utility of circulating human DNA as a biomarker. We found that human DNA concentration reproducibly increased with disease progression and decreased after successful therapeutic intervention. A marked, transient spike in circulating human tumor DNA occurred immediately after cytotoxic therapy or surgery. This simple assay may find broad utility in target validation studies and preclinical drug development programs.
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              Frequent genomic structural alterations at HPV insertion sites in cervical carcinoma.

              P Cremoux, Nicolas Stransky, Benjamin Peter (2010)
              To investigate whether integration of HPV DNA in cervical carcinoma is responsible for structural alterations of the host genome at the insertion site, a series of 34 primary cervical carcinomas and eight cervical cancer-derived cell lines were analysed. DNA copy number profiles were assessed using the Affymetrix GeneChip Human Mapping 250K Sty array. HPV 16, 18 or 45 integration sites were determined using the DIPS-PCR technique. The genome status at integration sites was classified as follows: no change, amplification, transition normal/gain, normal/loss or gain/LOH. A single HPV integration site was found in 34 cases; two sites were found in seven cases; and three sites in one case (51 sites). Comparison between integration sites and DNA copy number profiles showed that the genome status was altered at 17/51 (33%) integration sites, corresponding to 16/42 cases (38%). Alterations detected were amplification in nine cases, transition normal/loss in four cases, normal/gain in three cases, and gain/LOH in one case. A highly significant association was found between genomic rearrangement and integration of HPV DNA (p < 10(-10)). Activation of the replication origin located in viral integrated sequences in a cell line derived from one of the primary cervical carcinomas induced an increase of the amplification level of both viral and cellular DNA sequences flanking the integration locus. This mechanism may be implicated in the triggering of genome amplification at the HPV integration site in cervical carcinoma. Structural alterations of the host genome are frequently observed at the integration site of HPV DNA in cervical cancer and may act in oncogenesis. (c) 2010 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
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                Author and article information

                Contributors
                Xavier Sastre‐Garau: x.sastregarau@nancy.unicancer.fr
                Journal
                Journal ID (nlm-ta): J Pathol Clin Res
                Journal ID (iso-abbrev): J Pathol Clin Res
                Journal ID (doi): 10.1002/(ISSN)2056-4538
                Journal ID (publisher-id): CJP2
                Title: The Journal of Pathology: Clinical Research
                Publisher: John Wiley and Sons Inc. (Hoboken )
                ISSN (Electronic): 2056-4538
                Publication date (Electronic): 28 June 2016
                Publication date Collection: October 2016
                Volume: 2
                Issue: 4 ( doiID: 10.1002/cjp2.v2.4 )
                Pages: 201-209
                Affiliations
                [ 1 ] Department of BiopathologyInstitut Curie 75248 Paris Cedex 05France
                [ 2 ] Department of BiopathologyInstitut Curie 92210 St CloudFrance
                [ 3 ] Department of RadiotherapyInstitut Curie 75248 Paris Cedex 05France
                [ 4 ]Institut Curie, PSL Research University, Centre National de la Recherche Scientifique, UMR 3244, Sorbonne Universités ParisFrance
                [ 5 ] Department of BiopathologyInstitut de Cancérologie de Lorraine 6, Avenue de Bourgogne‐CS30519, 54519 Vandoeuvre‐les‐NancyFrance
                Author notes
                [*] [* ]Correspondence to: Xavier Sastre‐Garau, Department of Biopathology, Institut de Cancérologie de Lorraine, 6, Avenue de Bourgogne‐CS30519, 54519 Vandoeuvre‐les‐Nancy Cedex, France. e‐mail: x.sastregarau@ 123456nancy.unicancer.fr
                Article
                Publisher ID: CJP247
                DOI: 10.1002/cjp2.47
                PMC ID: 5129558
                PubMed ID: 27917295
                SO-VID: d3318629-d00d-4def-9178-211ed35666ed
                Copyright © © 2016 The Authors The Journal of Pathology: Clinical Research published by The Pathological Society of Great Britain and Ireland and John Wiley & Sons Ltd
                License:

                This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.

                History
                Date received : 10 February 2016
                Date accepted : 08 April 2016
                Page count
                Figures: 4, Tables: 2, Pages: 9, Words: 4929
                Categories
                Subject: Original Article
                Subject: Original Articles
                Custom metadata
                source-schema-version-number 2.0
                component-id cjp247
                cover-date October 2016
                details-of-publishers-convertor Converter:WILEY_ML3GV2_TO_NLMPMC version:4.9.8 mode:remove_FC converted:24.11.2016

                Keywords: circulating hpv dna,ddpcr,cervical carcinoma,anal carcinoma,carcinoma of the head and neck
                Data availability:
                Keywords: circulating hpv dna, ddpcr, cervical carcinoma, anal carcinoma, carcinoma of the head and neck

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