MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca2+ Stress

Neeharika Nemani; Edmund Carvalho; Dhanendra Tomar; Zhiwei Dong; Andrea Ketschek; Sarah L. Breves; Fabián Jaña; Alison M. Worth; Julie Heffler; Palaniappan Palaniappan; Aparna Tripathi; Ramasamy Subbiah; Massimo F. Riitano; Ajay Seelam; Thomas Manfred; Kie Itoh; Shuxia Meng; Hiromi Sesaki; William J. Craigen; Sudarsan Rajan; Santhanam Shanmughapriya; Jeffrey Caplan; Benjamin L. Prosser; Donald L. Gill; Peter B. Stathopulos; Gianluca Gallo; David C. Chan; Prashant Mishra; Muniswamy Madesh

doi:10.1016/j.celrep.2018.03.098

MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca²⁺ Stress

Neeharika Nemani, Edmund Carvalho, Dhanendra Tomar, Zhiwei Dong, Andrea Ketschek, Sarah L. Breves, Fabián Jaña, Alison M. Worth, Julie Heffler, Palaniappan Palaniappan, Aparna Tripathi, Ramasamy Subbiah, Massimo F. Riitano, Ajay Seelam, Thomas Manfred, Kie Itoh, Shuxia Meng, Hiromi Sesaki, William J. Craigen, Sudarsan RajanSanthanam Shanmughapriya, Jeffrey Caplan, Benjamin L. Prosser, Donald L. Gill, Peter B. Stathopulos, Gianluca Gallo, David C. Chan, Prashant Mishra, Muniswamy Madesh

School of Medicine

Research output: Contribution to journal › Article › peer-review

36 Scopus citations

Abstract

Mitochondria shape cytosolic calcium ([Ca²⁺]_c) transients and utilize the mitochondrial Ca²⁺ ([Ca²⁺]_m) in exchange for bioenergetics output. Conversely, dysregulated [Ca²⁺]_c causes [Ca²⁺]_m overload and induces permeability transition pore and cell death. Ablation of MCU-mediated Ca²⁺ uptake exhibited elevated [Ca²⁺]_c and failed to prevent stress-induced cell death. The mechanisms for these effects remain elusive. Here, we report that mitochondria undergo a cytosolic Ca²⁺-induced shape change that is distinct from mitochondrial fission and swelling. [Ca²⁺]_c elevation, but not MCU-mediated Ca²⁺ uptake, appears to be essential for the process we term mitochondrial shape transition (MiST). MiST is mediated by the mitochondrial protein Miro1 through its EF-hand domain 1 in multiple cell types. Moreover, Ca²⁺-dependent disruption of Miro1/KIF5B/tubulin complex is determined by Miro1 EF1 domain. Functionally, Miro1-dependent MiST is essential for autophagy/mitophagy that is attenuated in Miro1 EF1 mutants. Thus, Miro1 is a cytosolic Ca²⁺ sensor that decodes metazoan Ca²⁺ signals as MiST. Metazoan Ca²⁺ signal determines mitochondrial shape transition (MiST) and cellular quality control. Nemani et al. find that mitochondria undergo shape changes upon Ca²⁺ stress. MiST is distinct from matrix Ca²⁺-induced swelling and mitochondrial dynamics. The conserved Ca²⁺ sensor Miro1 enables MiST and promotes autophagy/mitophagy.

Original language	English (US)
Pages (from-to)	1005-1019
Number of pages	15
Journal	Cell Reports
Volume	23
Issue number	4
DOIs	https://doi.org/10.1016/j.celrep.2018.03.098
State	Published - Apr 24 2018

Keywords

EF hand
MCU
MiST
Miro
PTP
autophagy
calcium
mitochondrial dynamics
mitochondrial shape
mitophagy

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.1016/j.celrep.2018.03.098

Cite this

Nemani, N., Carvalho, E., Tomar, D., Dong, Z., Ketschek, A., Breves, S. L., Jaña, F., Worth, A. M., Heffler, J., Palaniappan, P., Tripathi, A., Subbiah, R., Riitano, M. F., Seelam, A., Manfred, T., Itoh, K., Meng, S., Sesaki, H., Craigen, W. J., ... Madesh, M. (2018). MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca²⁺ Stress. Cell Reports, 23(4), 1005-1019. https://doi.org/10.1016/j.celrep.2018.03.098

Nemani, N, Carvalho, E, Tomar, D, Dong, Z, Ketschek, A, Breves, SL, Jaña, F, Worth, AM, Heffler, J, Palaniappan, P, Tripathi, A, Subbiah, R, Riitano, MF, Seelam, A, Manfred, T, Itoh, K, Meng, S, Sesaki, H, Craigen, WJ, Rajan, S, Shanmughapriya, S, Caplan, J, Prosser, BL, Gill, DL, Stathopulos, PB, Gallo, G, Chan, DC, Mishra, P & Madesh, M 2018, 'MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca²⁺ Stress', Cell Reports, vol. 23, no. 4, pp. 1005-1019. https://doi.org/10.1016/j.celrep.2018.03.098

@article{53494f12c571466d9c0c76078472c966,

title = "MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca2+ Stress",

abstract = "Mitochondria shape cytosolic calcium ([Ca2+]c) transients and utilize the mitochondrial Ca2+ ([Ca2+]m) in exchange for bioenergetics output. Conversely, dysregulated [Ca2+]c causes [Ca2+]m overload and induces permeability transition pore and cell death. Ablation of MCU-mediated Ca2+ uptake exhibited elevated [Ca2+]c and failed to prevent stress-induced cell death. The mechanisms for these effects remain elusive. Here, we report that mitochondria undergo a cytosolic Ca2+-induced shape change that is distinct from mitochondrial fission and swelling. [Ca2+]c elevation, but not MCU-mediated Ca2+ uptake, appears to be essential for the process we term mitochondrial shape transition (MiST). MiST is mediated by the mitochondrial protein Miro1 through its EF-hand domain 1 in multiple cell types. Moreover, Ca2+-dependent disruption of Miro1/KIF5B/tubulin complex is determined by Miro1 EF1 domain. Functionally, Miro1-dependent MiST is essential for autophagy/mitophagy that is attenuated in Miro1 EF1 mutants. Thus, Miro1 is a cytosolic Ca2+ sensor that decodes metazoan Ca2+ signals as MiST. Metazoan Ca2+ signal determines mitochondrial shape transition (MiST) and cellular quality control. Nemani et al. find that mitochondria undergo shape changes upon Ca2+ stress. MiST is distinct from matrix Ca2+-induced swelling and mitochondrial dynamics. The conserved Ca2+ sensor Miro1 enables MiST and promotes autophagy/mitophagy.",

keywords = "EF hand, MCU, MiST, Miro, PTP, autophagy, calcium, mitochondrial dynamics, mitochondrial shape, mitophagy",

author = "Neeharika Nemani and Edmund Carvalho and Dhanendra Tomar and Zhiwei Dong and Andrea Ketschek and Breves, {Sarah L.} and Fabi{\'a}n Ja{\~n}a and Worth, {Alison M.} and Julie Heffler and Palaniappan Palaniappan and Aparna Tripathi and Ramasamy Subbiah and Riitano, {Massimo F.} and Ajay Seelam and Thomas Manfred and Kie Itoh and Shuxia Meng and Hiromi Sesaki and Craigen, {William J.} and Sudarsan Rajan and Santhanam Shanmughapriya and Jeffrey Caplan and Prosser, {Benjamin L.} and Gill, {Donald L.} and Stathopulos, {Peter B.} and Gianluca Gallo and Chan, {David C.} and Prashant Mishra and Muniswamy Madesh",

note = "Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax −/− Bak −/− MEFs, mito-Keima, mito-BFP, sec61-β, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH ( R01GM109882 , R01HL086699 , R01HL119306 , and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships ( 17PRE33660720 , 17POST33660251 ). S.S. is supported by a NIH K99/R00 grant ( 1K99HL138268-01 ). Z.D. is supported by China Scholarship Council (No. 201403170252 ). F.J. is supported by FONDECYT postdoctoral fellowship # 3140458 . Access to the electron microscope was supported by NIH-NIGMS ( P20 GM103446 ) and NSF ( IIA-1301765 ). Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax?/?Bak?/? MEFs, mito-Keima, mito-BFP, sec61-?, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH (R01GM109882, R01HL086699, R01HL119306, and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships (17PRE33660720, 17POST33660251). S.S. is supported by a NIH K99/R00 grant (1K99HL138268-01). Z.D. is supported by China Scholarship Council (No. 201403170252). F.J. is supported by FONDECYT postdoctoral fellowship #3140458. Access to the electron microscope was supported by NIH-NIGMS (P20 GM103446) and NSF (IIA-1301765). Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax−/−Bak−/− MEFs, mito-Keima, mito-BFP, sec61-β, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH (R01GM109882, R01HL086699, R01HL119306, and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships (17PRE33660720, 17POST33660251). S.S. is supported by a NIH K99/R00 grant (1K99HL138268-01). Z.D. is supported by China Scholarship Council (No. 201403170252). F.J. is supported by FONDECYT postdoctoral fellowship #3140458. Access to the electron microscope was supported by NIH-NIGMS (P20 GM103446) and NSF (IIA-1301765). Publisher Copyright: {\textcopyright} 2018 The Author(s)",

year = "2018",

month = apr,

day = "24",

doi = "10.1016/j.celrep.2018.03.098",

language = "English (US)",

volume = "23",

pages = "1005--1019",

journal = "Cell Reports",

issn = "2211-1247",

publisher = "Cell Press",

number = "4",

}

TY - JOUR

T1 - MIRO-1 Determines Mitochondrial Shape Transition upon GPCR Activation and Ca2+ Stress

AU - Nemani, Neeharika

AU - Carvalho, Edmund

AU - Tomar, Dhanendra

AU - Dong, Zhiwei

AU - Ketschek, Andrea

AU - Breves, Sarah L.

AU - Jaña, Fabián

AU - Worth, Alison M.

AU - Heffler, Julie

AU - Palaniappan, Palaniappan

AU - Tripathi, Aparna

AU - Subbiah, Ramasamy

AU - Riitano, Massimo F.

AU - Seelam, Ajay

AU - Manfred, Thomas

AU - Itoh, Kie

AU - Meng, Shuxia

AU - Sesaki, Hiromi

AU - Craigen, William J.

AU - Rajan, Sudarsan

AU - Shanmughapriya, Santhanam

AU - Caplan, Jeffrey

AU - Prosser, Benjamin L.

AU - Gill, Donald L.

AU - Stathopulos, Peter B.

AU - Gallo, Gianluca

AU - Chan, David C.

AU - Mishra, Prashant

AU - Madesh, Muniswamy

N1 - Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax −/− Bak −/− MEFs, mito-Keima, mito-BFP, sec61-β, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH ( R01GM109882 , R01HL086699 , R01HL119306 , and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships ( 17PRE33660720 , 17POST33660251 ). S.S. is supported by a NIH K99/R00 grant ( 1K99HL138268-01 ). Z.D. is supported by China Scholarship Council (No. 201403170252 ). F.J. is supported by FONDECYT postdoctoral fellowship # 3140458 . Access to the electron microscope was supported by NIH-NIGMS ( P20 GM103446 ) and NSF ( IIA-1301765 ). Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax?/?Bak?/? MEFs, mito-Keima, mito-BFP, sec61-?, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH (R01GM109882, R01HL086699, R01HL119306, and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships (17PRE33660720, 17POST33660251). S.S. is supported by a NIH K99/R00 grant (1K99HL138268-01). Z.D. is supported by China Scholarship Council (No. 201403170252). F.J. is supported by FONDECYT postdoctoral fellowship #3140458. Access to the electron microscope was supported by NIH-NIGMS (P20 GM103446) and NSF (IIA-1301765). Funding Information: We thank Craig B. Thompson, Richard Youle, Gia Voeltz, Tom Rapoport, and Gary Yellen for sharing Bax−/−Bak−/− MEFs, mito-Keima, mito-BFP, sec61-β, and Peredox plasmid constructs, respectively. We thank John Elrod for sharing the CypD KO MEFs. The authors also thank Shannon Modla for EM sample processing and image acquisition. This research was funded by the NIH (R01GM109882, R01HL086699, R01HL119306, and 1S10RR027327 to M.M. and R01 NS095471 to G.G.). N.N. and D.T. are supported by the AHA fellowships (17PRE33660720, 17POST33660251). S.S. is supported by a NIH K99/R00 grant (1K99HL138268-01). Z.D. is supported by China Scholarship Council (No. 201403170252). F.J. is supported by FONDECYT postdoctoral fellowship #3140458. Access to the electron microscope was supported by NIH-NIGMS (P20 GM103446) and NSF (IIA-1301765). Publisher Copyright: © 2018 The Author(s)

PY - 2018/4/24

Y1 - 2018/4/24

N2 - Mitochondria shape cytosolic calcium ([Ca2+]c) transients and utilize the mitochondrial Ca2+ ([Ca2+]m) in exchange for bioenergetics output. Conversely, dysregulated [Ca2+]c causes [Ca2+]m overload and induces permeability transition pore and cell death. Ablation of MCU-mediated Ca2+ uptake exhibited elevated [Ca2+]c and failed to prevent stress-induced cell death. The mechanisms for these effects remain elusive. Here, we report that mitochondria undergo a cytosolic Ca2+-induced shape change that is distinct from mitochondrial fission and swelling. [Ca2+]c elevation, but not MCU-mediated Ca2+ uptake, appears to be essential for the process we term mitochondrial shape transition (MiST). MiST is mediated by the mitochondrial protein Miro1 through its EF-hand domain 1 in multiple cell types. Moreover, Ca2+-dependent disruption of Miro1/KIF5B/tubulin complex is determined by Miro1 EF1 domain. Functionally, Miro1-dependent MiST is essential for autophagy/mitophagy that is attenuated in Miro1 EF1 mutants. Thus, Miro1 is a cytosolic Ca2+ sensor that decodes metazoan Ca2+ signals as MiST. Metazoan Ca2+ signal determines mitochondrial shape transition (MiST) and cellular quality control. Nemani et al. find that mitochondria undergo shape changes upon Ca2+ stress. MiST is distinct from matrix Ca2+-induced swelling and mitochondrial dynamics. The conserved Ca2+ sensor Miro1 enables MiST and promotes autophagy/mitophagy.

AB - Mitochondria shape cytosolic calcium ([Ca2+]c) transients and utilize the mitochondrial Ca2+ ([Ca2+]m) in exchange for bioenergetics output. Conversely, dysregulated [Ca2+]c causes [Ca2+]m overload and induces permeability transition pore and cell death. Ablation of MCU-mediated Ca2+ uptake exhibited elevated [Ca2+]c and failed to prevent stress-induced cell death. The mechanisms for these effects remain elusive. Here, we report that mitochondria undergo a cytosolic Ca2+-induced shape change that is distinct from mitochondrial fission and swelling. [Ca2+]c elevation, but not MCU-mediated Ca2+ uptake, appears to be essential for the process we term mitochondrial shape transition (MiST). MiST is mediated by the mitochondrial protein Miro1 through its EF-hand domain 1 in multiple cell types. Moreover, Ca2+-dependent disruption of Miro1/KIF5B/tubulin complex is determined by Miro1 EF1 domain. Functionally, Miro1-dependent MiST is essential for autophagy/mitophagy that is attenuated in Miro1 EF1 mutants. Thus, Miro1 is a cytosolic Ca2+ sensor that decodes metazoan Ca2+ signals as MiST. Metazoan Ca2+ signal determines mitochondrial shape transition (MiST) and cellular quality control. Nemani et al. find that mitochondria undergo shape changes upon Ca2+ stress. MiST is distinct from matrix Ca2+-induced swelling and mitochondrial dynamics. The conserved Ca2+ sensor Miro1 enables MiST and promotes autophagy/mitophagy.

KW - EF hand

KW - MCU

KW - MiST

KW - Miro

KW - PTP

KW - autophagy

KW - calcium

KW - mitochondrial dynamics

KW - mitochondrial shape

KW - mitophagy

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