Success or failure of vaccination for HPV16-positive vulvar lesions correlates with kinetics and phenotype of induced T-cell responses

Welters, Marij J.P.; Kenter, Gemma G.; Steenwijk, Peggy J. de Vos van; Löwik, Margriet J.; Meer, Dorien M A Berends-van der; Essahsah, Farah; Stynenbosch, Linda F. M.; Vloon, Annelies P G; Ramwadhdoebé, Tamara H.; Piersma, Sytse J.; Hulst, Jeanette M. van der; Valentijn, A. Rob P. M.; Fathers, Lorraine M.; Drijfhout, Jan W.; Franken, Kees L. M. C.; Oostendorp, Jaap; Fleuren, Gert Jan; Melief, Cornelis J.M.; Burg, Sjoerd H. van der

doi:10.1073/pnas.1006500107

Cited by 218 publications

(228 citation statements)

References 34 publications

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“…In HNSCC the ratio between CD8þ and regulatory T cells is associated with disease. 5,33 Similarly, in HPV16 induced genital malignancies the presence of FoxP3 positive as well as FoxP3 negative HPV16 specific regulatory T cells in tumor and LN is described 30,36,38 and a low CD8/Treg T-cell ratio is associated with worse outcome. 39 While the regulatory function of the CD4þCD25þFoxp3þ T cells present in TILs needs to be confirmed, at least one of our isolated clones clearly exerted regulatory function.…”

Section: Discussionmentioning

confidence: 98%

“…In TIL we find different subsets of HPV16-specific T cells (Th1, Th2, CTL and Tregs) with different cytokine profiles (IL-2, IFNc, IL-5) comparable to what is found in anogenital HPV16 induced lesions. 29,35,36 Together this advocates that local adaptive immune cells might play a role in the response to therapy and the altered survival of this patient group.…”

Section: Discussionmentioning

confidence: 98%

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Systemic and local human papillomavirus 16‐specific T‐cell immunity in patients with head and neck cancer

Heusinkveld

Goedemans

Briët

et al. 2011

Intl Journal of Cancer

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Squamous cell carcinomas of the head and neck (HNSCC), in particular those of the oropharynx, can be caused by human papilloma virus Type 16 (HPV16). Whereas these HPV-induced oropharyngeal carcinomas may express the HPV16 E6 and E7 oncoproteins and are associated with better survival, the nonvirally induced HNSCC are associated with overexpression of p53. In this study we assessed the presence of systemic and local T cells reactive against these oncoproteins in HNSCC. An exploratory study on the presence, type and function of HPV16-and/or p53-specific T cells in the blood, tumor and/or metastatic lymph node as measured by several immune assays was performed in an unselected group of 50 patients with HNSCC. Tumor tissue was tested for HPV DNA and the overexpression of p53 protein. Almost all HPV161 tumors were located in the oropharynx. Circulating HPV16-and p53-specific T cells were found in 17/47 and 7/45 tested patients. T cells were isolated from tumor cultures and/or lymph nodes of 20 patients. HPV16-specific T cells were detected in six of eight HPV1 tumors, but in none of the 12 HPV-tumors. Tumor-infiltrating p53-specific T cells were not detected. In depth analysis of the HPV16-specific T-cell response revealed that this response comprised a broad repertoire of CD41 T-helper Type 1 and 2 cells, CD41 regulatory T cells and CD81 T cells reactive to HPV16. The local presence of HPV16-specific T-cell immunity in HPV16-induced HNSCC implicates a role in the antitumor response and support the development of immunotherapy for HNSCC.

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Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 98%

Systemic and local human papillomavirus 16‐specific T‐cell immunity in patients with head and neck cancer

Heusinkveld

Goedemans

Briët

et al. 2011

Intl Journal of Cancer

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“…In human, the group of Peter Van der Bruggen has demonstrated that the CD4 + T-cell response of melanoma patients to a MAGE-A3-derived peptide vaccine involves regulatory T cells [88]. In individuals vaccinated with E6/E7-derived long peptides, immunosuppressive cells has been shown to expand [89], correlating to the development of resistance against an anti-HPV therapeutic vaccine [90]. A better identification of the specificity of Tregs in cancer patients will help to design TAAbased vaccine that induce optimal Teff responses while failing to activate Tregs to significant extents.…”

Section: Specificity Of Tregsmentioning

confidence: 99%

Tumor-Infiltrating Regulatory T Cells: Phenotype, Role, Mechanism of Expansion In Situ and Clinical Significance

Tanchot

Terme

Péré

et al. 2012

Cancer Microenvironment

112

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In immunocompetent individuals, the immune system initially eradicates potentially tumorigenic cells as they develop, a capacity that is progressively lost when malignant cells acquire alterations that sustain immunosubversion and/or immunoevasion. One of the major mechanisms whereby cancer cells block antitumor immune responses involves a specific class of immunosuppressive T cells that-in the vast majority of cases-express the Forkhead box P3 (FOXP3) transcription factor. Such FOXP3 + regulatory T cells (Tregs) accumulate within neoplastic lesions as a result of several distinct mechanisms, including increased infiltration, local expansion, survival advantage and in situ development from conventional CD4 + cells.

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“…The importance of a robust effector T-cell response in mediating successful outcomes to immunotherapy has been recently shown in a clinical human papillomavirus vaccine trial for pre-malignant vulval intraepithelial neoplasia, in which measured T-cell responses strongly correlated with regression of lesions (Kenter et al, 2009;Welters et al, 2010; Figure 2). However, in other clinical trials of tumour vaccines against larger, invasive malignancies the effective generation of tumour antigenspecific T cells in peripheral blood has not predicted clinical efficacy Gajewski et al, 2006).…”

Section: Why Does An Anti-tumour T-cell Response Still Fail To Eradicmentioning

confidence: 93%

Harnessing the immune response to treat cancer

et al. 2010

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It is well established that the immune system has the capacity to attack malignant cells. During malignant transformation cells acquire numerous molecular and biochemical changes that render them potentially vulnerable to immune cells. Yet it is self-evident that a growing tumour has managed to evade these host defence mechanisms. The exact ways in which the immune system interacts with tumour cells and how cancers are able to escape immunological eradication have only recently started to be fully elucidated. Understanding the relationship between the tumour and the anti-tumour immune response and how this can be altered with conventional treatments and immune-targeted therapies is crucial to developing new treatments for patients with cancer. In this review, focusing on the anti-tumour T-cell response, we summarize our understanding of how tumours, cancer treatments and the immune system interact, how tumours evade the immune response and how this process could be manipulated for the benefit of patients with cancer.

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Success or failure of vaccination for HPV16-positive vulvar lesions correlates with kinetics and phenotype of induced T-cell responses

Cited by 218 publications

References 34 publications

Systemic and local human papillomavirus 16‐specific T‐cell immunity in patients with head and neck cancer

Systemic and local human papillomavirus 16‐specific T‐cell immunity in patients with head and neck cancer

Tumor-Infiltrating Regulatory T Cells: Phenotype, Role, Mechanism of Expansion In Situ and Clinical Significance

Harnessing the immune response to treat cancer

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