Literature DB >> 21384340

Parenteral is more efficient than mucosal immunization to induce regression of human papillomavirus-associated genital tumors.

Loane Decrausaz1, Sonia Domingos-Pereira, Mélanie Duc, Martine Bobst, Pedro Romero, John T Schiller, Patrice Jichlinski, Denise Nardelli-Haefliger.   

Abstract

Cervical cancer is a public health concern as it represents the second cause of cancer death in women worldwide. High-risk human papillomaviruses (HPV) are the etiologic agents, and HPV E6 and/or E7 oncogene-specific therapeutic vaccines are under development to treat HPV-related lesions in women. Whether the use of mucosal routes of immunization may be preferable for inducing cell-mediated immune responses able to eradicate genital tumors is still debated because of the uniqueness of the female genital mucosa (GM) and the limited experimentation. Here, we compared the protective activity resulting from immunization of mice via intranasal (i.n.), intravaginal (IVAG) or subcutaneous (s.c.) routes with an adjuvanted HPV type 16 E7 polypeptide vaccine. Our data show that s.c. and i.n. immunizations elicited similar frequencies and avidity of TetE71CD81 and E7-specific Interferon-gamma-secreting cells in the GM, whereas slightly lower immune responses were induced by IVAG immunization. In a novel orthotopic murine model, both s.c. and i.n. immunizations allowed for complete long-term protection against genital E7-expressing tumor challenge. However, only s.c. immunization induced complete regression of already established genital tumors. This suggests that the higher E7-specific systemic response observed after s.c. immunization may contribute to the regression of growing genital tumors, whereas local immune responses may be sufficient to impede genital challenges. Thus, our data show that for an efficiently adjuvanted protein-based vaccine, parenteral vaccination route is superior to mucosal vaccination route for inducing regression of established genital tumors in a murine model of HPV-associated genital cancer.

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Year:  2011        PMID: 21384340      PMCID: PMC7462631          DOI: 10.1002/ijc.25973

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  50 in total

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6.  Human papillomavirus infections in a group of renal transplant recipients.

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7.  A novel mucosal orthotopic murine model of human papillomavirus-associated genital cancers.

Authors:  Loane Decrausaz; Ana-Rita Gonçalves; Sonia Domingos-Pereira; Christelle Pythoud; Jean-Christophe Stehle; John Schiller; Patrice Jichlinski; Denise Nardelli-Haefliger
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Review 8.  Mucosal immunity: induction, dissemination, and effector functions.

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  17 in total

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2.  Local Salmonella immunostimulation recruits vaccine-specific CD8 T cells and increases regression of bladder tumor.

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3.  Intravaginal immunization with HPV vectors induces tissue-resident CD8+ T cell responses.

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4.  Mucosal imprinting of vaccine-induced CD8⁺ T cells is crucial to inhibit the growth of mucosal tumors.

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Review 5.  Heat shock protein bystander antigens for peptide immunotherapy in autoimmune disease.

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6.  What is the influence of vaccination's routes on the regression of tumors located at mucosal sites?

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Review 7.  Dendritic cell-based vaccination in cancer: therapeutic implications emerging from murine models.

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8.  Immunotherapeutic strategies for bladder cancer.

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9.  Intravaginal TLR agonists increase local vaccine-specific CD8 T cells and human papillomavirus-associated genital-tumor regression in mice.

Authors:  S Domingos-Pereira; L Decrausaz; L Derré; M Bobst; P Romero; J T Schiller; P Jichlinski; D Nardelli-Haefliger
Journal:  Mucosal Immunol       Date:  2012-09-12       Impact factor: 7.313

10.  Heterosubtypic cross-protection induced by whole inactivated influenza virus vaccine in mice: influence of the route of vaccine administration.

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