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Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines

Approximately 10–15% of the human prion disease is inherited and one of the important genetic mutations occurs in the octapeptide repeat region of prion protein gene. One of the variants, one octapeptide repeat deletion (1-OPRD), existed in several gastric cancer cell lines and its mutation frequenc...

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Autores principales: Liang, Jie, Wang, Jingbo, Luo, Guanhong, Pan, Yanglin, Wang, Xin, Guo, Changcun, Zhang, Dexin, Yin, Fang, Zhang, Xiaoyin, Liu, Jie, Wang, Jianhong, Guo, Xuegang, Wu, Kaichun, Fan, Daiming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Ltd 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4515061/
https://www.ncbi.nlm.nih.gov/pubmed/19210573
http://dx.doi.org/10.1111/j.1582-4934.2009.00687.x
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author Liang, Jie
Wang, Jingbo
Luo, Guanhong
Pan, Yanglin
Wang, Xin
Guo, Changcun
Zhang, Dexin
Yin, Fang
Zhang, Xiaoyin
Liu, Jie
Wang, Jianhong
Guo, Xuegang
Wu, Kaichun
Fan, Daiming
author_facet Liang, Jie
Wang, Jingbo
Luo, Guanhong
Pan, Yanglin
Wang, Xin
Guo, Changcun
Zhang, Dexin
Yin, Fang
Zhang, Xiaoyin
Liu, Jie
Wang, Jianhong
Guo, Xuegang
Wu, Kaichun
Fan, Daiming
author_sort Liang, Jie
collection PubMed
description Approximately 10–15% of the human prion disease is inherited and one of the important genetic mutations occurs in the octapeptide repeat region of prion protein gene. One of the variants, one octapeptide repeat deletion (1-OPRD), existed in several gastric cancer cell lines and its mutation frequency was higher in gastric cancer cases. However, the biological functions of it remain unknown. Wild-type and mutation forms of PrP(C) were cloned and transfected into gastric cancer cells. Cell apoptosis, adhesion, invasion, multidrug resistance (MDR) and proliferation were, respectively, investigated. Different expressed genes were screened by gene array and proved by PT-PCR. Further, luciferase report assay was used to explore the transcriptional activation of target genes. Forced overexpression PrP(C) (1-OPRD) could promote the gastric cancer cells SGC7901 growth through facilitating G1- to S-phase transition in the cell cycle. PrP(C) (1-OPRD) could also inhibit apoptosis, and promote adhesion, invasion and MDR in SGC7901. However, it exhibited no significant difference between wild-type PrP(C) (1-OPRD) and PrP(C) on apoptosis, invasion or MDR effects. Further experiments indicated that PrP(C) (1-OPRD) could trigger the transactivation of cyclinD3 besides cyclinD1 to promote cell transition and proliferation. Overexpression of PrP(C) (1-OPRD) might promote the proliferation of gastric cancer cells at least partially through transcriptional activation of cyclinD3 to accelerate the G1-/S-phase transition. The promoting proliferation effect of PrP(C) (1-OPRD) was more than that of wild-type PrP(C). However, they showed no difference on apoptosis, adhesion, invasion or MDR effects of gastric cancer cells.
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spelling pubmed-45150612015-07-27 Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines Liang, Jie Wang, Jingbo Luo, Guanhong Pan, Yanglin Wang, Xin Guo, Changcun Zhang, Dexin Yin, Fang Zhang, Xiaoyin Liu, Jie Wang, Jianhong Guo, Xuegang Wu, Kaichun Fan, Daiming J Cell Mol Med Articles Approximately 10–15% of the human prion disease is inherited and one of the important genetic mutations occurs in the octapeptide repeat region of prion protein gene. One of the variants, one octapeptide repeat deletion (1-OPRD), existed in several gastric cancer cell lines and its mutation frequency was higher in gastric cancer cases. However, the biological functions of it remain unknown. Wild-type and mutation forms of PrP(C) were cloned and transfected into gastric cancer cells. Cell apoptosis, adhesion, invasion, multidrug resistance (MDR) and proliferation were, respectively, investigated. Different expressed genes were screened by gene array and proved by PT-PCR. Further, luciferase report assay was used to explore the transcriptional activation of target genes. Forced overexpression PrP(C) (1-OPRD) could promote the gastric cancer cells SGC7901 growth through facilitating G1- to S-phase transition in the cell cycle. PrP(C) (1-OPRD) could also inhibit apoptosis, and promote adhesion, invasion and MDR in SGC7901. However, it exhibited no significant difference between wild-type PrP(C) (1-OPRD) and PrP(C) on apoptosis, invasion or MDR effects. Further experiments indicated that PrP(C) (1-OPRD) could trigger the transactivation of cyclinD3 besides cyclinD1 to promote cell transition and proliferation. Overexpression of PrP(C) (1-OPRD) might promote the proliferation of gastric cancer cells at least partially through transcriptional activation of cyclinD3 to accelerate the G1-/S-phase transition. The promoting proliferation effect of PrP(C) (1-OPRD) was more than that of wild-type PrP(C). However, they showed no difference on apoptosis, adhesion, invasion or MDR effects of gastric cancer cells. John Wiley & Sons, Ltd 2009 2009-02-04 /pmc/articles/PMC4515061/ /pubmed/19210573 http://dx.doi.org/10.1111/j.1582-4934.2009.00687.x Text en © 2009 The Authors Journal compilation © 2009 Foundation for Cellular and Molecular Medicine/Blackwell Publishing Ltd
spellingShingle Articles
Liang, Jie
Wang, Jingbo
Luo, Guanhong
Pan, Yanglin
Wang, Xin
Guo, Changcun
Zhang, Dexin
Yin, Fang
Zhang, Xiaoyin
Liu, Jie
Wang, Jianhong
Guo, Xuegang
Wu, Kaichun
Fan, Daiming
Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title_full Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title_fullStr Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title_full_unstemmed Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title_short Function of PrP(C) (1-OPRD) in biological activities of gastric cancer cell lines
title_sort function of prp(c) (1-oprd) in biological activities of gastric cancer cell lines
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4515061/
https://www.ncbi.nlm.nih.gov/pubmed/19210573
http://dx.doi.org/10.1111/j.1582-4934.2009.00687.x
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