Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.

Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.

Human chorionic gonadotropin (hCG) was initially thought to be made only during pregnancy, but is now known to also be synthesized by a variety of cancers and is associated with poor patient prognosis. Transgenic expression of βhCG in mice causes hyper-luteinized ovaries, a loss in estrous cyclicity...

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Main Authors: Ruchi Sachdeva, Neetu Bhardwaj, Ilpo Huhtaniemi, Usha Aggrawal, Swatantra Kumar Jain, Rana Zaidi, Om Singh, Rahul Pal
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3511405?pdf=render
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spelling doaj-a08924453bde4b8eb3a1311ab0a0e2702020-11-24T21:46:28ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01711e5112510.1371/journal.pone.0051125Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.Ruchi SachdevaNeetu BhardwajIlpo HuhtaniemiUsha AggrawalSwatantra Kumar JainRana ZaidiOm SinghRahul PalHuman chorionic gonadotropin (hCG) was initially thought to be made only during pregnancy, but is now known to also be synthesized by a variety of cancers and is associated with poor patient prognosis. Transgenic expression of βhCG in mice causes hyper-luteinized ovaries, a loss in estrous cyclicity and infertility, increased body weight, prolactinomas and mammary gland tumors. Strategies were devised to generate antibody responses against hCG to investigate whether reversal of the molecular processes driving tumorigenesis would follow. hCG-immunized transgenic mice did not exhibit increases in body weight or serum prolactin levels, and gross ovarian and pituitary morphology remained normal. While non-immunized transgenic animals demonstrated heightened levels of transcripts associated with pituitary tumorigenesis (HMG2A, E2F1, CCND1, PRL, GH, GAL, PTTG1, BMP4) and decreased levels of CDK inhibitors CDKN1B (p27), CDKN2A (p16) and CDKN2c (p18), immunization led to a reversal to levels found in non-transgenic animals. Serum derived from transgenic (but not non-transgenic) mice led to enhanced transcription as well as expression of VEGF, IL-8, KC (murine IL-8) and MMP-9 in tumor cells, effects not seen when sera derived from hCG-immunized transgenic mice was employed. As the definitive indication of the restoration of the reproductive axis, immunization led to the resumption of estrous cyclicity as well as fertility in transgenic mice. These results indicate that hCG may influence cancer pathogenesis and progression via several distinct mechanisms. Using a stringent in vivo system in which βhCG acts both a "self" antigen and a tumor-promoting moiety (putatively akin to the situation in humans), the data builds a case for anti-gonadotropin vaccination strategies in the treatment of gonadotropin-dependent or secreting malignancies that frequently acquire resistance to conventional therapy.http://europepmc.org/articles/PMC3511405?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Ruchi Sachdeva
Neetu Bhardwaj
Ilpo Huhtaniemi
Usha Aggrawal
Swatantra Kumar Jain
Rana Zaidi
Om Singh
Rahul Pal
spellingShingle Ruchi Sachdeva
Neetu Bhardwaj
Ilpo Huhtaniemi
Usha Aggrawal
Swatantra Kumar Jain
Rana Zaidi
Om Singh
Rahul Pal
Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
PLoS ONE
author_facet Ruchi Sachdeva
Neetu Bhardwaj
Ilpo Huhtaniemi
Usha Aggrawal
Swatantra Kumar Jain
Rana Zaidi
Om Singh
Rahul Pal
author_sort Ruchi Sachdeva
title Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
title_short Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
title_full Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
title_fullStr Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
title_full_unstemmed Transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
title_sort transgenesis-mediated reproductive dysfunction and tumorigenesis: effects of immunological neutralization.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Human chorionic gonadotropin (hCG) was initially thought to be made only during pregnancy, but is now known to also be synthesized by a variety of cancers and is associated with poor patient prognosis. Transgenic expression of βhCG in mice causes hyper-luteinized ovaries, a loss in estrous cyclicity and infertility, increased body weight, prolactinomas and mammary gland tumors. Strategies were devised to generate antibody responses against hCG to investigate whether reversal of the molecular processes driving tumorigenesis would follow. hCG-immunized transgenic mice did not exhibit increases in body weight or serum prolactin levels, and gross ovarian and pituitary morphology remained normal. While non-immunized transgenic animals demonstrated heightened levels of transcripts associated with pituitary tumorigenesis (HMG2A, E2F1, CCND1, PRL, GH, GAL, PTTG1, BMP4) and decreased levels of CDK inhibitors CDKN1B (p27), CDKN2A (p16) and CDKN2c (p18), immunization led to a reversal to levels found in non-transgenic animals. Serum derived from transgenic (but not non-transgenic) mice led to enhanced transcription as well as expression of VEGF, IL-8, KC (murine IL-8) and MMP-9 in tumor cells, effects not seen when sera derived from hCG-immunized transgenic mice was employed. As the definitive indication of the restoration of the reproductive axis, immunization led to the resumption of estrous cyclicity as well as fertility in transgenic mice. These results indicate that hCG may influence cancer pathogenesis and progression via several distinct mechanisms. Using a stringent in vivo system in which βhCG acts both a "self" antigen and a tumor-promoting moiety (putatively akin to the situation in humans), the data builds a case for anti-gonadotropin vaccination strategies in the treatment of gonadotropin-dependent or secreting malignancies that frequently acquire resistance to conventional therapy.
url http://europepmc.org/articles/PMC3511405?pdf=render
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