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Mitotic Arrest in Teratoma Susceptible Fetal Male Germ Cells

Author: A Aravin
A Goriely
A Kocer
A McLaren
A Suzuki
A Suzuki
AD Krentz
AE Baltus
AG Byskov
Andrew H. Sinclair
B Madan
Camden Lo
CM Spiller
D Best
D Bourc'his
Denise C. Miles
G Durcova-Hills
H Masaki
IR Adams
J Bowles
J Bowles
J Brennan
J Koubova
J Maldonado-Saldivia
Jocelyn A. van den Bergen
KA Ewen
KK Youngren
L DiNapoli
LC Stevens
LC Stevens
LC Stevens
Martin Pera
MH Kaufman
MS Cook
MS Cook
NE Skakkebaek
P Western
P Western
Patrick S. Western
PS Western
PS Western
Rachael A. Ralli
S Kumar
S Kuramochi-Miyagawa
S Kuramochi-Miyagawa
S Yamaguchi
Stephanie I. Wakeling
T John
T Kimura
T Noguchi
TC Shovlin
Y Lin
Y Sakai
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

Formation of germ cell derived teratomas occurs in mice of the 129/SvJ strain, but not in C57Bl/6 inbred or CD1 outbred mice. Despite this, there have been few comparative studies aimed at determining the similarities and differences between teratoma susceptible and non-susceptible mouse strains. This study examines the entry of fetal germ cells into the male pathway and mitotic arrest in 129T2/SvJ mice. We find that although the entry of fetal germ cells into mitotic arrest is similar between 129T2/SvJ, C57Bl/6 and CD1 mice, there were significant differences in the size and germ cell content of the testis cords in these strains. In 129T2/SvJ mice germ cell mitotic arrest involves upregulation of p27KIP1, p15INK4B, activation of RB, the expression of male germ cell differentiation markers NANOS2, DNMT3L and MILI and repression of the pluripotency network. The germ-line markers DPPA2 and DPPA4 show reciprocal repression and upregulation, respectively, while FGFR3 is substantially enriched in the nucleus of differentiating male germ cells. Further understanding of fetal male germ cell differentiation promises to provide insight into disorders of the testis and germ cell lineage, such as testis tumour formation and infertility

Public Library of Science (PLOS)

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PubMed Central

University of Melbourne Institutional Repository

Deciphering the molecular events necessary for synergistic tumor cell apoptosis mediated by the histone deacetylase inhibitor vorinostat and the BH3 mimetic ABT-737

Author: Alsop Amber E.
Banks Kellie-Marie
Bots Michael
Cluse Leonie A.
Frenzel Anna
Johnstone Ricky W.
Ralli Rachael
Scott Clare L.
Villunger Andreas
Wiegmans Adrian P.
Williams Steven P.
Publication venue: 'American Association for Cancer Research (AACR)'
Publication date: 01/01/2011
Field of study

The concept of personalized anticancer therapy is based on the use of targeted therapeutics through in-depth knowledge of the molecular mechanisms of action of these agents when used alone and in combination. We have identified the apoptotic proteins and pathways necessary for synergistic tumor cell apoptosis and in vivo antitumor responses seen when the HDAC inhibitor vorinostat is combined with the BH3-mimetic ABT-737 in lymphomas overexpressing Bcl-2. Vorinostat "primes" tumors overexpressing Bcl-2 for rapid ABT-737-mediated apoptosis by inducing expression of the BH3-only gene bmf. Moreover, these synergistic effects of vorinostat/ABT-737 were blunted in cells with an inactive p53 pathway or in cells lacking expression of the p53 target gene, noxa. These studies show the important and complex functional interaction between specific proapoptotic BH3-only proteins and the BH3-mimetic compound ABT-737 and provide the most comprehensive functional link between tumor genotype and the apoptotic and therapeutic effects of HDACi combined with ABT-73