Details der Publikation - Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission

Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission : = Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission

OBJECTIVE To elucidate the molecular mechanism and the anti-breast cancer effect of polyphyllinⅠ,which is a natural compound extracted from Rhizoma of Paris polyphyllin.METHODS Human breast cancer cells were treated with polyphyllinⅠ,after which DRP1-dependent mitochondrial fission and apoptosis,mitophagy and PINK1/PARK2 pathway were evaluated.A genetic approach was employed to determine how knockdown of PINK1 with sh RNA regulates polyphyllinⅠ-induced mitophagy and apoptosis.The inhibitory effect of polyphyllinⅠon tumor growth in a breast cancer cell xenograft mouse model was also examined.RESULTS PolyphyllinⅠenhanced the stabilization of full-length PINK1at the mitochondrial surface,leading to PARK2 recruitment to mitochondria,and culminating in mitophagy.PolyphyllinⅠalso induced dephosphorylation of DRP1 at Ser637 and mitochondrial translocation of DRP1,leading to mitochondrial fission and apoptosis.Knockdown of PINK1 evidently suppressed mitophagy stimulated by polyphyllinⅠ,and markedly enhanced DRP1-dependent mitochondrial fission and apoptosis induced by polyphyl inⅠ.Furthermore,suppression of DRP1 by mdivi-1 or sh RNA inhibits PINK1 knockdown-mediated mitochondrial fragmentation and apoptosis in response to polyphyllinⅠtreatment,suggesting that depletion of PINK1 lead to mitochondrial fragmentation due to excessive fission.Our in vivo study also showed that knockdown of PINK1potentiated polyphyllinⅠ-mediated inhibition of tumor growth in a breast cancer cell xenograft mouse model.CONCLUSION Our study provides a mechanism to support the role of PINK1 in the regulation of polyphyl inⅠ-induced mitophagy and apoptosis,and suggest polyphylinⅠas a potential drug for treatment of breast cancer..

Medienart:	E-Artikel

Erscheinungsjahr:	2016-10-30 2016
Erschienen:	2016-10-30

Enthalten in:	Zur Gesamtaufnahme - year:2016
Enthalten in:	Zhong guo yao li xue yu du li xue za zhi - (2016), 10 vom: 30. Okt., Seite 1074 Original Letters: Enthalten in 中国药理学与毒理学杂志 (DE-600)2989809-2 (DE-600)2989809-2 北京市

Reihe:	China Academic Journals (CAJ), E, 医药卫生科技 = Medicine & Public Health

Sprache:	Chinesisch

Weiterer Titel:	Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission

Beteiligte Personen:	LI Guo-bing [VerfasserIn] FU Ruo-qiu [Sonstige Person] SHEN Han-ming [Sonstige Person] ZHOU Jing [Sonstige Person] HU Xiao-ye [Sonstige Person] LIU Yan-xia [Sonstige Person] LI Yu-nong [Sonstige Person] ZHANG Hong-wei [Sonstige Person] LIU Xin [Sonstige Person] ZHANG Yan-hao [Sonstige Person] HUANG Cheng [Sonstige Person] ZHANG Rong [Sonstige Person] GAO Ning [Sonstige Person]

Links:	oversea.cnki.net [lizenzpflichtig]

Themen:	医药、卫生医药卫生科技药学药理学 College of Pharmacy,3rd Military Medical University Department of Pharmacy,The Second Affiliated Hospital of Third Military Medical University Department of Physiology,Yong Loo Lin School of Medicine,National University of Singapore Drug Discovery Lab,School of Pharmacy,Shanghai University of Traditional Chinese Medicine Medicine & Public Health Pharmaceutics

Anmerkungen:	Author info:LI Guo-bing;FU Ruo-qiu;SHEN Han-ming;ZHOU Jing;HU Xiao-ye;LIU Yan-xia;LI Yu-nong;ZHANG Hong-wei;LIU Xin;ZHANG Yan-hao;HUANG Cheng;ZHANG Rong;GAO Ning;College of Pharmacy,3rd Military Medical University;Department of Pharmacy,The Second Affiliated Hospital of Third Military Medical University;Department of Physiology,Yong Loo Lin School of Medicine,National University of Singapore;Drug Discovery Lab,School of Pharmacy,Shanghai University of Traditional Chinese Medicine

Förderinstitution / Projekttitel:

PPN (Katalog-ID):	CAJ518720837

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245	1	0	\|a Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission \|b = Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission
246	3	1	\|a Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission
264		1	\|c 2016-10-30
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500			\|a Author info:LI Guo-bing;FU Ruo-qiu;SHEN Han-ming;ZHOU Jing;HU Xiao-ye;LIU Yan-xia;LI Yu-nong;ZHANG Hong-wei;LIU Xin;ZHANG Yan-hao;HUANG Cheng;ZHANG Rong;GAO Ning;College of Pharmacy,3rd Military Medical University;Department of Pharmacy,The Second Affiliated Hospital of Third Military Medical University;Department of Physiology,Yong Loo Lin School of Medicine,National University of Singapore;Drug Discovery Lab,School of Pharmacy,Shanghai University of Traditional Chinese Medicine
520			\|a OBJECTIVE To elucidate the molecular mechanism and the anti-breast cancer effect of polyphyllinⅠ,which is a natural compound extracted from Rhizoma of Paris polyphyllin.METHODS Human breast cancer cells were treated with polyphyllinⅠ,after which DRP1-dependent mitochondrial fission and apoptosis,mitophagy and PINK1/PARK2 pathway were evaluated.A genetic approach was employed to determine how knockdown of PINK1 with sh RNA regulates polyphyllinⅠ-induced mitophagy and apoptosis.The inhibitory effect of polyphyllinⅠon tumor growth in a breast cancer cell xenograft mouse model was also examined.RESULTS PolyphyllinⅠenhanced the stabilization of full-length PINK1at the mitochondrial surface,leading to PARK2 recruitment to mitochondria,and culminating in mitophagy.PolyphyllinⅠalso induced dephosphorylation of DRP1 at Ser637 and mitochondrial translocation of DRP1,leading to mitochondrial fission and apoptosis.Knockdown of PINK1 evidently suppressed mitophagy stimulated by polyphyllinⅠ,and markedly enhanced DRP1-dependent mitochondrial fission and apoptosis induced by polyphyl inⅠ.Furthermore,suppression of DRP1 by mdivi-1 or sh RNA inhibits PINK1 knockdown-mediated mitochondrial fragmentation and apoptosis in response to polyphyllinⅠtreatment,suggesting that depletion of PINK1 lead to mitochondrial fragmentation due to excessive fission.Our in vivo study also showed that knockdown of PINK1potentiated polyphyllinⅠ-mediated inhibition of tumor growth in a breast cancer cell xenograft mouse model.CONCLUSION Our study provides a mechanism to support the role of PINK1 in the regulation of polyphyl inⅠ-induced mitophagy and apoptosis,and suggest polyphylinⅠas a potential drug for treatment of breast cancer.
610	2	4	\|a College of Pharmacy,3rd Military Medical University
610	2	4	\|a Department of Pharmacy,The Second Affiliated Hospital of Third Military Medical University
610	2	4	\|a Department of Physiology,Yong Loo Lin School of Medicine,National University of Singapore
610	2	4	\|a Drug Discovery Lab,School of Pharmacy,Shanghai University of Traditional Chinese Medicine
650		4	\|a 药理学
650		4	\|a 药学
650		4	\|a 医药、卫生
650		4	\|a Pharmaceutics
650		4	\|a 医药卫生科技
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700	0		\|a LIU Xin \|4 oth
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Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission : = Depletion of PINK1 sensitizes breast cancer cells to polyphyllin Ⅰ via mitophagy suppression and DRP1-mediated mitochondrial fission

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