Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes

Mohamed H. Al-Sabri; Neha Behare; Ahmed M. Alsehli; Samuel Berkins; Aadeya Arora; Eirini Antoniou; Eleni I. Moysiadou; Sowmya Anantha-Krishnan; Patricia D. Cosmen; Johanna Vikner; Thiago C. Moulin; Nourhene Ammar; Hadi Boukhatmi; Laura E. Clemensson; Mathias Rask-Andersen; Jessica Mwinyi; Michael J. Williams; Robert Fredriksson; Helgi B. Schiöth

doi:10.3390/cells11223528

Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes

Mohamed H. Al-Sabri, Neha Behare, Ahmed M. Alsehli, Samuel Berkins, Aadeya Arora, Eirini Antoniou, Eleni I. Moysiadou, Sowmya Anantha-Krishnan, Patricia D. Cosmen, Johanna Vikner, Thiago C. Moulin, Nourhene Ammar, Hadi Boukhatmi, Laura E. Clemensson, Mathias Rask-Andersen, Jessica Mwinyi, Michael J. Williams, Robert Fredriksson, Helgi B. Schiöth

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Abstract

The underlying mechanisms for statin-induced myopathy (SIM) are still equivocal. In this study, we employ Drosophila melanogaster to dissect possible underlying mechanisms for SIM. We observe that chronic fluvastatin treatment causes reduced general locomotion activity and climbing ability. In addition, transmission microscopy of dissected skeletal muscles of fluvastatin-treated flies reveals strong myofibrillar damage, including increased sarcomere lengths and Z-line streaming, which are reminiscent of myopathy, along with fragmented mitochondria of larger sizes, most of which are round-like shapes. Furthermore, chronic fluvastatin treatment is associated with impaired lipid metabolism and insulin signalling. Mechanistically, knockdown of the statin-target Hmgcr in the skeletal muscles recapitulates fluvastatin-induced mitochondrial phenotypes and lowered general locomotion activity; however, it was not sufficient to alter sarcomere length or elicit myofibrillar damage compared to controls or fluvastatin treatment. Moreover, we found that fluvastatin treatment was associated with reduced expression of the skeletal muscle chloride channel, ClC-a (Drosophila homolog of CLCN1), while selective knockdown of skeletal muscle ClC-a also recapitulated fluvastatin-induced myofibril damage and increased sarcomere lengths. Surprisingly, exercising fluvastatin-treated flies restored ClC-a expression and normalized sarcomere lengths, suggesting that fluvastatin-induced myofibrillar phenotypes could be linked to lowered ClC-a expression. Taken together, these results may indicate the potential role of ClC-a inhibition in statin-associated muscular phenotypes. This study underlines the importance of Drosophila melanogaster as a powerful model system for elucidating the locomotion and muscular phenotypes, promoting a better understanding of the molecular mechanisms underlying SIM.

Original language	English
Article number	3528
Journal	Cells
Volume	11
Issue number	22
DOIs	https://doi.org/10.3390/cells11223528
Publication status	Published - 2022 Nov

Subject classification (UKÄ)

Neurosciences

Free keywords

chelerythrine
CLC-1
ClC-a
Drosophila melanogaster
fluvastatin
Hmgcr
lipotoxicity
locomotion
mitochondrial dysfunction
myopathy
Pkcdelta (Pkcδ)
PKCtheta (PKCθ)
sarcomere
skeletal muscle chloride channel
statin-induced myopathy
statins

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Al-Sabri, M. H., Behare, N., Alsehli, A. M., Berkins, S., Arora, A., Antoniou, E., Moysiadou, E. I., Anantha-Krishnan, S., Cosmen, P. D., Vikner, J., Moulin, T. C., Ammar, N., Boukhatmi, H., Clemensson, L. E., Rask-Andersen, M., Mwinyi, J., Williams, M. J., Fredriksson, R., & Schiöth, H. B. (2022). Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes. Cells, 11(22), Article 3528. https://doi.org/10.3390/cells11223528

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title = "Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes",

abstract = "The underlying mechanisms for statin-induced myopathy (SIM) are still equivocal. In this study, we employ Drosophila melanogaster to dissect possible underlying mechanisms for SIM. We observe that chronic fluvastatin treatment causes reduced general locomotion activity and climbing ability. In addition, transmission microscopy of dissected skeletal muscles of fluvastatin-treated flies reveals strong myofibrillar damage, including increased sarcomere lengths and Z-line streaming, which are reminiscent of myopathy, along with fragmented mitochondria of larger sizes, most of which are round-like shapes. Furthermore, chronic fluvastatin treatment is associated with impaired lipid metabolism and insulin signalling. Mechanistically, knockdown of the statin-target Hmgcr in the skeletal muscles recapitulates fluvastatin-induced mitochondrial phenotypes and lowered general locomotion activity; however, it was not sufficient to alter sarcomere length or elicit myofibrillar damage compared to controls or fluvastatin treatment. Moreover, we found that fluvastatin treatment was associated with reduced expression of the skeletal muscle chloride channel, ClC-a (Drosophila homolog of CLCN1), while selective knockdown of skeletal muscle ClC-a also recapitulated fluvastatin-induced myofibril damage and increased sarcomere lengths. Surprisingly, exercising fluvastatin-treated flies restored ClC-a expression and normalized sarcomere lengths, suggesting that fluvastatin-induced myofibrillar phenotypes could be linked to lowered ClC-a expression. Taken together, these results may indicate the potential role of ClC-a inhibition in statin-associated muscular phenotypes. This study underlines the importance of Drosophila melanogaster as a powerful model system for elucidating the locomotion and muscular phenotypes, promoting a better understanding of the molecular mechanisms underlying SIM.",

keywords = "chelerythrine, CLC-1, ClC-a, Drosophila melanogaster, fluvastatin, Hmgcr, lipotoxicity, locomotion, mitochondrial dysfunction, myopathy, Pkcdelta (Pkcδ), PKCtheta (PKCθ), sarcomere, skeletal muscle chloride channel, statin-induced myopathy, statins",

author = "Al-Sabri, {Mohamed H.} and Neha Behare and Alsehli, {Ahmed M.} and Samuel Berkins and Aadeya Arora and Eirini Antoniou and Moysiadou, {Eleni I.} and Sowmya Anantha-Krishnan and Cosmen, {Patricia D.} and Johanna Vikner and Moulin, {Thiago C.} and Nourhene Ammar and Hadi Boukhatmi and Clemensson, {Laura E.} and Mathias Rask-Andersen and Jessica Mwinyi and Williams, {Michael J.} and Robert Fredriksson and Schi{\"o}th, {Helgi B.}",

year = "2022",

month = nov,

doi = "10.3390/cells11223528",

language = "English",

volume = "11",

journal = "Cells",

issn = "2073-4409",

publisher = "MDPI AG",

number = "22",

}

Al-Sabri, MH, Behare, N, Alsehli, AM, Berkins, S, Arora, A, Antoniou, E, Moysiadou, EI, Anantha-Krishnan, S, Cosmen, PD, Vikner, J, Moulin, TC, Ammar, N, Boukhatmi, H, Clemensson, LE, Rask-Andersen, M, Mwinyi, J, Williams, MJ, Fredriksson, R & Schiöth, HB 2022, 'Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes', Cells, vol. 11, no. 22, 3528. https://doi.org/10.3390/cells11223528

Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes. / Al-Sabri, Mohamed H.; Behare, Neha; Alsehli, Ahmed M. et al.
In: Cells, Vol. 11, No. 22, 3528, 11.2022.

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

TY - JOUR

T1 - Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy

T2 - Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes

AU - Al-Sabri, Mohamed H.

AU - Behare, Neha

AU - Alsehli, Ahmed M.

AU - Berkins, Samuel

AU - Arora, Aadeya

AU - Antoniou, Eirini

AU - Moysiadou, Eleni I.

AU - Anantha-Krishnan, Sowmya

AU - Cosmen, Patricia D.

AU - Vikner, Johanna

AU - Moulin, Thiago C.

AU - Ammar, Nourhene

AU - Boukhatmi, Hadi

AU - Clemensson, Laura E.

AU - Rask-Andersen, Mathias

AU - Mwinyi, Jessica

AU - Williams, Michael J.

AU - Fredriksson, Robert

AU - Schiöth, Helgi B.

PY - 2022/11

Y1 - 2022/11

N2 - The underlying mechanisms for statin-induced myopathy (SIM) are still equivocal. In this study, we employ Drosophila melanogaster to dissect possible underlying mechanisms for SIM. We observe that chronic fluvastatin treatment causes reduced general locomotion activity and climbing ability. In addition, transmission microscopy of dissected skeletal muscles of fluvastatin-treated flies reveals strong myofibrillar damage, including increased sarcomere lengths and Z-line streaming, which are reminiscent of myopathy, along with fragmented mitochondria of larger sizes, most of which are round-like shapes. Furthermore, chronic fluvastatin treatment is associated with impaired lipid metabolism and insulin signalling. Mechanistically, knockdown of the statin-target Hmgcr in the skeletal muscles recapitulates fluvastatin-induced mitochondrial phenotypes and lowered general locomotion activity; however, it was not sufficient to alter sarcomere length or elicit myofibrillar damage compared to controls or fluvastatin treatment. Moreover, we found that fluvastatin treatment was associated with reduced expression of the skeletal muscle chloride channel, ClC-a (Drosophila homolog of CLCN1), while selective knockdown of skeletal muscle ClC-a also recapitulated fluvastatin-induced myofibril damage and increased sarcomere lengths. Surprisingly, exercising fluvastatin-treated flies restored ClC-a expression and normalized sarcomere lengths, suggesting that fluvastatin-induced myofibrillar phenotypes could be linked to lowered ClC-a expression. Taken together, these results may indicate the potential role of ClC-a inhibition in statin-associated muscular phenotypes. This study underlines the importance of Drosophila melanogaster as a powerful model system for elucidating the locomotion and muscular phenotypes, promoting a better understanding of the molecular mechanisms underlying SIM.

AB - The underlying mechanisms for statin-induced myopathy (SIM) are still equivocal. In this study, we employ Drosophila melanogaster to dissect possible underlying mechanisms for SIM. We observe that chronic fluvastatin treatment causes reduced general locomotion activity and climbing ability. In addition, transmission microscopy of dissected skeletal muscles of fluvastatin-treated flies reveals strong myofibrillar damage, including increased sarcomere lengths and Z-line streaming, which are reminiscent of myopathy, along with fragmented mitochondria of larger sizes, most of which are round-like shapes. Furthermore, chronic fluvastatin treatment is associated with impaired lipid metabolism and insulin signalling. Mechanistically, knockdown of the statin-target Hmgcr in the skeletal muscles recapitulates fluvastatin-induced mitochondrial phenotypes and lowered general locomotion activity; however, it was not sufficient to alter sarcomere length or elicit myofibrillar damage compared to controls or fluvastatin treatment. Moreover, we found that fluvastatin treatment was associated with reduced expression of the skeletal muscle chloride channel, ClC-a (Drosophila homolog of CLCN1), while selective knockdown of skeletal muscle ClC-a also recapitulated fluvastatin-induced myofibril damage and increased sarcomere lengths. Surprisingly, exercising fluvastatin-treated flies restored ClC-a expression and normalized sarcomere lengths, suggesting that fluvastatin-induced myofibrillar phenotypes could be linked to lowered ClC-a expression. Taken together, these results may indicate the potential role of ClC-a inhibition in statin-associated muscular phenotypes. This study underlines the importance of Drosophila melanogaster as a powerful model system for elucidating the locomotion and muscular phenotypes, promoting a better understanding of the molecular mechanisms underlying SIM.

KW - chelerythrine

KW - CLC-1

KW - ClC-a

KW - Drosophila melanogaster

KW - fluvastatin

KW - Hmgcr

KW - lipotoxicity

KW - locomotion

KW - mitochondrial dysfunction

KW - myopathy

KW - Pkcdelta (Pkcδ)

KW - PKCtheta (PKCθ)

KW - sarcomere

KW - skeletal muscle chloride channel

KW - statin-induced myopathy

KW - statins

U2 - 10.3390/cells11223528

DO - 10.3390/cells11223528

M3 - Article

C2 - 36428957

AN - SCOPUS:85142416234

SN - 2073-4409

VL - 11

JO - Cells

JF - Cells

IS - 22

M1 - 3528

ER -

Statins Induce Locomotion and Muscular Phenotypes in Drosophila melanogaster That Are Reminiscent of Human Myopathy: Evidence for the Role of the Chloride Channel Inhibition in the Muscular Phenotypes

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