Literature DB >> 7640048

Programmed cell death in response to chemotherapeutic agents in human germ cell tumour lines.

R A Huddart1, J Titley, D Robertson, G T Williams, A Horwich, C S Cooper.   

Abstract

Testicular germ cell tumours are amongst the most chemosensitive neoplasms both in vivo and in vitro. In the present study we demonstrate that following exposure to drugs used in chemotherapeutic treatment of testicular germ cell cancer tumour cells undergo death by apoptosis. Thus, after exposure of the GCT27 embryonal carcinoma cell line to cisplatin, we observed the degradation of DNA into oligonucleosomal fragments, which is a hallmark of apoptosis. Furthermore, light, fluorescence and electron microscopy reveal the presence of condensed abnormal shaped nuclear chromatin which is characteristic of apoptosis. Changes diagnostic of apoptosis were also observed following (a) cisplatin treatment of the GCT48 and Susa embryonal carcinoma cell lines and the GCT44 yolk sac tumour cell line and (b) etoposide treatment of the GCT27 and Susa cell lines. When the GCT27 cell line was treated with 15 microns cisplatin, apoptosis was first observed at 6-9 h and greater than 90% of cells were dead within 24 h. Apoptosis was not blocked when cisplatin-treated cells were incubated in the presence of cycloheximide, although this agent did cause a 4-6 h delay in the onset of cell death. In addition, we demonstrated that the GCT27 cell line can be induced to undergo apoptosis by exposure to low concentrations of the calcium ionophore, ionomycin. These observations show that germ cell tumours are remarkably sensitive to a range of agents that act by different mechanisms. They are triggered to undergo apoptosis rapidly by a mechanism that is not blocked by inhibitors of protein synthesis.

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Year:  1995        PMID: 7640048     DOI: 10.1016/0959-8049(95)00047-m

Source DB:  PubMed          Journal:  Eur J Cancer        ISSN: 0959-8049            Impact factor:   9.162


  9 in total

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4.  Acute respiratory distress syndrome after chemotherapy for lung metastases from non-seminomatous germ-cell tumors.

Authors:  C Kirch; F Blot; K Fizazi; B Raynard; C Theodore; G Nitenberg
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5.  A histopathological study of nephrotoxicity, hepatoxicity or testicular toxicity: Which one is the first observation as side effect of Cisplatin-induced toxicity in animal model?

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6.  p53 hypersensitivity is the predominant mechanism of the unique responsiveness of testicular germ cell tumor (TGCT) cells to cisplatin.

Authors:  Matthias Gutekunst; Moshe Oren; Andrea Weilbacher; Michael A Dengler; Christiane Markwardt; Jürgen Thomale; Walter E Aulitzky; Heiko van der Kuip
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7.  Identification and validation of a five apoptosis-related genes signature for prediction of disease-free survival for testicular germ cell tumors.

Authors:  Tengyue Zeng; Liangyu Yao; Kai Zhao; Rong Cong; Xianghu Meng; Ninghong Song
Journal:  Transl Androl Urol       Date:  2021-03

8.  Expression of p53, Bcl-2 and Bax in cisplatin-induced apoptosis in testicular germ cell tumour cell lines.

Authors:  H Burger; K Nooter; A W Boersma; C J Kortland; G Stoter
Journal:  Br J Cancer       Date:  1998-05       Impact factor: 7.640

9.  Intensive chemotherapy as salvage treatment for solid tumors: focus on germ cell cancer.

Authors:  F Selle; J Gligorov; S Richard; A Khalil; I Alexandre; D Avenin; S Provent; D G Soares; J P Lotz
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  9 in total

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