HDAC6 differentially regulates autophagy in stem-like versus differentiated cancer cells

Tanveer Sharif; Emma Martell; Cathleen Dai; Mohammad Saleh Ghassemi-Rad; Mark Robert Hanes; Patrick J. Murphy; Nandini N. Margam; Hirendrasinh B. Parmar; Carman A. Giacomantonio; Roy Duncan; Patrick W.K. Lee; Shashi Gujar

doi:10.1080/15548627.2018.1548547

HDAC6 differentially regulates autophagy in stem-like versus differentiated cancer cells

Tanveer Sharif, Emma Martell, Cathleen Dai, Mohammad Saleh Ghassemi-Rad, Mark Robert Hanes, Patrick J. Murphy, Nandini N. Margam, Hirendrasinh B. Parmar, Carman A. Giacomantonio, Roy Duncan, Patrick W.K. Lee, Shashi Gujar

Résultat de recherche: Article › examen par les pairs

33 Citations (Scopus)

Résumé

Cancer stem-like cells (CSCs), a small population of pluripotent cells residing within heterogeneous tumor mass, remain highly resistant to various chemotherapies as compared to the differentiated cancer cells. It is being postulated that CSCs possess unique molecular mechanisms, such as autophagic homeostasis, that allow CSCs to withstand the therapeutic assaults. Here we demonstrate that HDAC6 inhibition differentially modulates macroautophagy/autophagy in CSCs as compared to that of differentiated cancer cells. Using human and murine CSC models and differentiated cells, we show that the inhibition or knockdown (KD) of HDAC6 decreases CSC pluripotency by downregulating major pluripotency factors POU5F1, NANOG and SOX2. This decreased HDAC6 expression increases ACTB, TUBB3 and CSN2 expression and promotes differentiation in CSCs in an apoptosis-independent manner. Mechanistically, HDAC6 KD in CSCs decreases pluripotency by promoting autophagy, whereas the inhibition of pluripotency via retinoic acid treatment, POU5F1 or autophagy-related gene (ATG7 and ATG12) KD in CSCs decreases HDAC6 expression and promotes differentiation. Interestingly, HDAC6 KD-mediated CSC growth inhibition is further enhanced in the presence of autophagy inducers Tat-Beclin 1 peptide and rapamycin. In contrast to the results observed in CSCs, HDAC6 KD in differentiated breast cancer cells downregulates autophagy and increases apoptosis. Furthermore, the autophagy regulator p-MTOR, upstream negative regulators of p-MTOR (TSC1 and TSC2) and downstream effectors of p-MTOR (p-RPS6KB and p-EIF4EBP1) are differentially regulated in CSCs versus differentiated cancer cells following HDAC6 KD. Overall these data identify the differential regulation of autophagy as a molecular link behind the differing chemo-susceptibility of CSCs and differentiated cancer cells.

Langue d'origine	English
Pages (de-à)	686-706
Nombre de pages	21
Journal	Autophagy
Volume	15
Numéro de publication	4
DOI	https://doi.org/10.1080/15548627.2018.1548547
Statut de publication	Published - avr. 3 2019

Note bibliographique

Funding Information:
This work was supported by the Government of Canada | Canadian Institutes of Health Research (CIHR);Breast Cancer Society;Canadian Breast Cancer Foundation (CBCF). This work was supported by grants from the Canadian Institute of Health Research (CIHR), from the Canadian Breast Cancer Foundation–Atlantic (CBCF), and Breast Cancer Society of Canada (BCSC)/QEII Foundation Awards for Breast Cancer Research through Beatrice Hunter Cancer Research Institute (BHCRI) to SAG and PWKL. TS is supported by the CIHR. PJM is supported through the post-doctoral fellowship from Cancer Research Training Program (CRTP) of BHCRI. MH is a trainee in the CRTP of BHCRI, with funds provided by a CIBC Graduate Scholarship in Medical Research. EM and CD were recipients of the BHCRI studentship award from BHCRI. SAG is supported by Dalhousie Medical Research Foundation (DMRF).

Publisher Copyright:
© 2018, © 2018 Informa UK Limited, trading as Taylor & Francis Group.

ASJC Scopus Subject Areas

Molecular Biology
Cell Biology

ODD de l’ONU

Cette action contribue à la réalisation des objectifs de développement durable suivants

Accès au document

10.1080/15548627.2018.1548547

Autres fichiers et liens

Citer

@article{f4676209f16e4440ad24a262e6fdbb0f,

title = "HDAC6 differentially regulates autophagy in stem-like versus differentiated cancer cells",

abstract = "Cancer stem-like cells (CSCs), a small population of pluripotent cells residing within heterogeneous tumor mass, remain highly resistant to various chemotherapies as compared to the differentiated cancer cells. It is being postulated that CSCs possess unique molecular mechanisms, such as autophagic homeostasis, that allow CSCs to withstand the therapeutic assaults. Here we demonstrate that HDAC6 inhibition differentially modulates macroautophagy/autophagy in CSCs as compared to that of differentiated cancer cells. Using human and murine CSC models and differentiated cells, we show that the inhibition or knockdown (KD) of HDAC6 decreases CSC pluripotency by downregulating major pluripotency factors POU5F1, NANOG and SOX2. This decreased HDAC6 expression increases ACTB, TUBB3 and CSN2 expression and promotes differentiation in CSCs in an apoptosis-independent manner. Mechanistically, HDAC6 KD in CSCs decreases pluripotency by promoting autophagy, whereas the inhibition of pluripotency via retinoic acid treatment, POU5F1 or autophagy-related gene (ATG7 and ATG12) KD in CSCs decreases HDAC6 expression and promotes differentiation. Interestingly, HDAC6 KD-mediated CSC growth inhibition is further enhanced in the presence of autophagy inducers Tat-Beclin 1 peptide and rapamycin. In contrast to the results observed in CSCs, HDAC6 KD in differentiated breast cancer cells downregulates autophagy and increases apoptosis. Furthermore, the autophagy regulator p-MTOR, upstream negative regulators of p-MTOR (TSC1 and TSC2) and downstream effectors of p-MTOR (p-RPS6KB and p-EIF4EBP1) are differentially regulated in CSCs versus differentiated cancer cells following HDAC6 KD. Overall these data identify the differential regulation of autophagy as a molecular link behind the differing chemo-susceptibility of CSCs and differentiated cancer cells.",

author = "Tanveer Sharif and Emma Martell and Cathleen Dai and Ghassemi-Rad, {Mohammad Saleh} and Hanes, {Mark Robert} and Murphy, {Patrick J.} and Margam, {Nandini N.} and Parmar, {Hirendrasinh B.} and Giacomantonio, {Carman A.} and Roy Duncan and Lee, {Patrick W.K.} and Shashi Gujar",

note = "Funding Information: This work was supported by the Government of Canada | Canadian Institutes of Health Research (CIHR);Breast Cancer Society;Canadian Breast Cancer Foundation (CBCF). This work was supported by grants from the Canadian Institute of Health Research (CIHR), from the Canadian Breast Cancer Foundation–Atlantic (CBCF), and Breast Cancer Society of Canada (BCSC)/QEII Foundation Awards for Breast Cancer Research through Beatrice Hunter Cancer Research Institute (BHCRI) to SAG and PWKL. TS is supported by the CIHR. PJM is supported through the post-doctoral fellowship from Cancer Research Training Program (CRTP) of BHCRI. MH is a trainee in the CRTP of BHCRI, with funds provided by a CIBC Graduate Scholarship in Medical Research. EM and CD were recipients of the BHCRI studentship award from BHCRI. SAG is supported by Dalhousie Medical Research Foundation (DMRF). Publisher Copyright: {\textcopyright} 2018, {\textcopyright} 2018 Informa UK Limited, trading as Taylor & Francis Group.",

year = "2019",

month = apr,

day = "3",

doi = "10.1080/15548627.2018.1548547",

language = "English",

volume = "15",

pages = "686--706",

journal = "Autophagy",

issn = "1554-8627",

publisher = "Landes Bioscience",

number = "4",

}

TY - JOUR

T1 - HDAC6 differentially regulates autophagy in stem-like versus differentiated cancer cells

AU - Sharif, Tanveer

AU - Martell, Emma

AU - Dai, Cathleen

AU - Ghassemi-Rad, Mohammad Saleh

AU - Hanes, Mark Robert

AU - Murphy, Patrick J.

AU - Margam, Nandini N.

AU - Parmar, Hirendrasinh B.

AU - Giacomantonio, Carman A.

AU - Duncan, Roy

AU - Lee, Patrick W.K.

AU - Gujar, Shashi

N1 - Funding Information: This work was supported by the Government of Canada | Canadian Institutes of Health Research (CIHR);Breast Cancer Society;Canadian Breast Cancer Foundation (CBCF). This work was supported by grants from the Canadian Institute of Health Research (CIHR), from the Canadian Breast Cancer Foundation–Atlantic (CBCF), and Breast Cancer Society of Canada (BCSC)/QEII Foundation Awards for Breast Cancer Research through Beatrice Hunter Cancer Research Institute (BHCRI) to SAG and PWKL. TS is supported by the CIHR. PJM is supported through the post-doctoral fellowship from Cancer Research Training Program (CRTP) of BHCRI. MH is a trainee in the CRTP of BHCRI, with funds provided by a CIBC Graduate Scholarship in Medical Research. EM and CD were recipients of the BHCRI studentship award from BHCRI. SAG is supported by Dalhousie Medical Research Foundation (DMRF). Publisher Copyright: © 2018, © 2018 Informa UK Limited, trading as Taylor & Francis Group.

PY - 2019/4/3

Y1 - 2019/4/3

N2 - Cancer stem-like cells (CSCs), a small population of pluripotent cells residing within heterogeneous tumor mass, remain highly resistant to various chemotherapies as compared to the differentiated cancer cells. It is being postulated that CSCs possess unique molecular mechanisms, such as autophagic homeostasis, that allow CSCs to withstand the therapeutic assaults. Here we demonstrate that HDAC6 inhibition differentially modulates macroautophagy/autophagy in CSCs as compared to that of differentiated cancer cells. Using human and murine CSC models and differentiated cells, we show that the inhibition or knockdown (KD) of HDAC6 decreases CSC pluripotency by downregulating major pluripotency factors POU5F1, NANOG and SOX2. This decreased HDAC6 expression increases ACTB, TUBB3 and CSN2 expression and promotes differentiation in CSCs in an apoptosis-independent manner. Mechanistically, HDAC6 KD in CSCs decreases pluripotency by promoting autophagy, whereas the inhibition of pluripotency via retinoic acid treatment, POU5F1 or autophagy-related gene (ATG7 and ATG12) KD in CSCs decreases HDAC6 expression and promotes differentiation. Interestingly, HDAC6 KD-mediated CSC growth inhibition is further enhanced in the presence of autophagy inducers Tat-Beclin 1 peptide and rapamycin. In contrast to the results observed in CSCs, HDAC6 KD in differentiated breast cancer cells downregulates autophagy and increases apoptosis. Furthermore, the autophagy regulator p-MTOR, upstream negative regulators of p-MTOR (TSC1 and TSC2) and downstream effectors of p-MTOR (p-RPS6KB and p-EIF4EBP1) are differentially regulated in CSCs versus differentiated cancer cells following HDAC6 KD. Overall these data identify the differential regulation of autophagy as a molecular link behind the differing chemo-susceptibility of CSCs and differentiated cancer cells.

AB - Cancer stem-like cells (CSCs), a small population of pluripotent cells residing within heterogeneous tumor mass, remain highly resistant to various chemotherapies as compared to the differentiated cancer cells. It is being postulated that CSCs possess unique molecular mechanisms, such as autophagic homeostasis, that allow CSCs to withstand the therapeutic assaults. Here we demonstrate that HDAC6 inhibition differentially modulates macroautophagy/autophagy in CSCs as compared to that of differentiated cancer cells. Using human and murine CSC models and differentiated cells, we show that the inhibition or knockdown (KD) of HDAC6 decreases CSC pluripotency by downregulating major pluripotency factors POU5F1, NANOG and SOX2. This decreased HDAC6 expression increases ACTB, TUBB3 and CSN2 expression and promotes differentiation in CSCs in an apoptosis-independent manner. Mechanistically, HDAC6 KD in CSCs decreases pluripotency by promoting autophagy, whereas the inhibition of pluripotency via retinoic acid treatment, POU5F1 or autophagy-related gene (ATG7 and ATG12) KD in CSCs decreases HDAC6 expression and promotes differentiation. Interestingly, HDAC6 KD-mediated CSC growth inhibition is further enhanced in the presence of autophagy inducers Tat-Beclin 1 peptide and rapamycin. In contrast to the results observed in CSCs, HDAC6 KD in differentiated breast cancer cells downregulates autophagy and increases apoptosis. Furthermore, the autophagy regulator p-MTOR, upstream negative regulators of p-MTOR (TSC1 and TSC2) and downstream effectors of p-MTOR (p-RPS6KB and p-EIF4EBP1) are differentially regulated in CSCs versus differentiated cancer cells following HDAC6 KD. Overall these data identify the differential regulation of autophagy as a molecular link behind the differing chemo-susceptibility of CSCs and differentiated cancer cells.

UR - http://www.scopus.com/inward/record.url?scp=85057769746&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85057769746&partnerID=8YFLogxK

U2 - 10.1080/15548627.2018.1548547

DO - 10.1080/15548627.2018.1548547

M3 - Article

C2 - 30444165

AN - SCOPUS:85057769746

SN - 1554-8627

VL - 15

SP - 686

EP - 706

JO - Autophagy

JF - Autophagy

IS - 4

ER -

HDAC6 differentially regulates autophagy in stem-like versus differentiated cancer cells

Résumé

Note bibliographique

ASJC Scopus Subject Areas

ODD de l’ONU

Accès au document

Autres fichiers et liens

Empreinte numérique

Citer