MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2

Recent studies suggest that physiological and tumorigenic proliferation of mammalian cells is controlled by multiple cyclin-dependent kinases (CDKs) largely in tissue-specific manners. We and others previously demonstrated that adult mice deficient for the D-cyclin-dependent kinase CDK4 (Cdk4(−/−) m...

Descripción completa

Detalles Bibliográficos
Autores principales: Gillam, Mary P., Nimbalkar, Dipali, Sun, Limin, Christov, Konstantin, Ray, Dipankar, Kaldis, Philipp, Liu, Xianpeng, Kiyokawa, Hiroaki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4135037/
https://www.ncbi.nlm.nih.gov/pubmed/24531709
http://dx.doi.org/10.1038/onc.2014.3
_version_ 1782330930892898304
author Gillam, Mary P.
Nimbalkar, Dipali
Sun, Limin
Christov, Konstantin
Ray, Dipankar
Kaldis, Philipp
Liu, Xianpeng
Kiyokawa, Hiroaki
author_facet Gillam, Mary P.
Nimbalkar, Dipali
Sun, Limin
Christov, Konstantin
Ray, Dipankar
Kaldis, Philipp
Liu, Xianpeng
Kiyokawa, Hiroaki
author_sort Gillam, Mary P.
collection PubMed
description Recent studies suggest that physiological and tumorigenic proliferation of mammalian cells is controlled by multiple cyclin-dependent kinases (CDKs) largely in tissue-specific manners. We and others previously demonstrated that adult mice deficient for the D-cyclin-dependent kinase CDK4 (Cdk4(−/−) mice) exhibit hypoplasia in the pituitary and pancreatic islet due to primary postnatal defects in proliferation. Intriguingly, those neuroendocrine tissues affected in Cdk4(−/−) mice are the primary targets of tumorigenesis in the syndrome of multiple endocrine neoplasia type-1 (MEN1). Mice with heterozygous disruption of the tumor suppressor Men1 gene (Men1(+/−)) develop tumors in the pituitary, pancreatic islets and other neuroendocrine tissues, which is analogous to humans with MEN1 mutations. To explore the genetic interactions between loss of Men1 and activation of CDKs, we examined the impact of Cdk4 or Cdk2 disruption on tumorigenesis in Men1(+/−) mice. A majority of Men1(+/−) mice with wild-type CDKs developed pituitary and islet tumors by 15 months of age. Strikingly, Men1(+/−); Cdk4(−/−) mice did not develop any tumors, and their islets and pituitaries remained hypoplastic with decreased proliferation. In contrast, Men1(+/−); Cdk2(−/−) mice showed pituitary and islet tumorigenesis comparable to those in Men1(+/−) mice. Pituitaries of Men1(+/−); Cdk4(−/−) mice showed no signs of loss of heterozygosity (LOH) in the Men1 locus, while tumors in Men1(+/−) mice and Men1(+/−); Cdk2(−/−) mice exhibited LOH. Consistently, CDK4 knockdown in INS-1 insulinoma cells inhibited glucose-stimulated cell cycle progression with a significant decrease in phosphorylation of retinoblastoma protein (RB) at specific sites including Ser780. CDK2 knockdown had minimum effects on RB phosphorylation and cell cycle progression. These data suggest that CDK4 is a critical downstream target of MEN1-dependent tumor suppression and is required for tumorigenic proliferation in the pituitary and pancreatic islet, whereas CDK2 is dispensable for tumorigenesis in these neuroendocrine cell types.
format Online
Article
Text
id pubmed-4135037
institution National Center for Biotechnology Information
language English
publishDate 2014
record_format MEDLINE/PubMed
spelling pubmed-41350372015-08-12 MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2 Gillam, Mary P. Nimbalkar, Dipali Sun, Limin Christov, Konstantin Ray, Dipankar Kaldis, Philipp Liu, Xianpeng Kiyokawa, Hiroaki Oncogene Article Recent studies suggest that physiological and tumorigenic proliferation of mammalian cells is controlled by multiple cyclin-dependent kinases (CDKs) largely in tissue-specific manners. We and others previously demonstrated that adult mice deficient for the D-cyclin-dependent kinase CDK4 (Cdk4(−/−) mice) exhibit hypoplasia in the pituitary and pancreatic islet due to primary postnatal defects in proliferation. Intriguingly, those neuroendocrine tissues affected in Cdk4(−/−) mice are the primary targets of tumorigenesis in the syndrome of multiple endocrine neoplasia type-1 (MEN1). Mice with heterozygous disruption of the tumor suppressor Men1 gene (Men1(+/−)) develop tumors in the pituitary, pancreatic islets and other neuroendocrine tissues, which is analogous to humans with MEN1 mutations. To explore the genetic interactions between loss of Men1 and activation of CDKs, we examined the impact of Cdk4 or Cdk2 disruption on tumorigenesis in Men1(+/−) mice. A majority of Men1(+/−) mice with wild-type CDKs developed pituitary and islet tumors by 15 months of age. Strikingly, Men1(+/−); Cdk4(−/−) mice did not develop any tumors, and their islets and pituitaries remained hypoplastic with decreased proliferation. In contrast, Men1(+/−); Cdk2(−/−) mice showed pituitary and islet tumorigenesis comparable to those in Men1(+/−) mice. Pituitaries of Men1(+/−); Cdk4(−/−) mice showed no signs of loss of heterozygosity (LOH) in the Men1 locus, while tumors in Men1(+/−) mice and Men1(+/−); Cdk2(−/−) mice exhibited LOH. Consistently, CDK4 knockdown in INS-1 insulinoma cells inhibited glucose-stimulated cell cycle progression with a significant decrease in phosphorylation of retinoblastoma protein (RB) at specific sites including Ser780. CDK2 knockdown had minimum effects on RB phosphorylation and cell cycle progression. These data suggest that CDK4 is a critical downstream target of MEN1-dependent tumor suppression and is required for tumorigenic proliferation in the pituitary and pancreatic islet, whereas CDK2 is dispensable for tumorigenesis in these neuroendocrine cell types. 2014-02-17 2015-02-12 /pmc/articles/PMC4135037/ /pubmed/24531709 http://dx.doi.org/10.1038/onc.2014.3 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Gillam, Mary P.
Nimbalkar, Dipali
Sun, Limin
Christov, Konstantin
Ray, Dipankar
Kaldis, Philipp
Liu, Xianpeng
Kiyokawa, Hiroaki
MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title_full MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title_fullStr MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title_full_unstemmed MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title_short MEN1-tumorigenesis in the pituitary and pancreatic islet requires Cdk4 but not Cdk2
title_sort men1-tumorigenesis in the pituitary and pancreatic islet requires cdk4 but not cdk2
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4135037/
https://www.ncbi.nlm.nih.gov/pubmed/24531709
http://dx.doi.org/10.1038/onc.2014.3
work_keys_str_mv AT gillammaryp men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT nimbalkardipali men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT sunlimin men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT christovkonstantin men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT raydipankar men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT kaldisphilipp men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT liuxianpeng men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2
AT kiyokawahiroaki men1tumorigenesisinthepituitaryandpancreaticisletrequirescdk4butnotcdk2

Ejemplares similares