Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity

Jonathan A. Stiber; Zhu Shan Zhang; Jarrett Burch; Jerry P. Eu; Sarah Zhang; George A. Truskey; Malini Seth; Naohiro Yamaguchi; Gerhard Meissner; Ripai Shah; Paul F. Worley; R. Sanders Williams; Paul B. Rosenberg

doi:10.1128/MCB.01601-07

Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity

Jonathan A. Stiber, Zhu Shan Zhang, Jarrett Burch, Jerry P. Eu, Sarah Zhang, George A. Truskey, Malini Seth, Naohiro Yamaguchi, Gerhard Meissner, Ripai Shah, Paul F. Worley, R. Sanders Williams, Paul B. Rosenberg

School of Medicine

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

79 Scopus citations

Abstract

Transient receptor potential (TRP) channels are nonselective cation channels, several of which are expressed in striated muscle. Because the scaffolding protein Homer 1 has been implicated in TRP channel regulation, we hypothesized that Homer proteins play a significant role in skeletal muscle function. Mice lacking Homer 1 exhibited a myopathy characterized by decreased muscle fiber cross-sectional area and decreased skeletal muscle force generation. Homer 1 knockout myotubes displayed increased basal current density and spontaneous cation influx. This spontaneous cation influx in Homer 1 knockout myotubes was blocked by reexpression of Homer 1b, but not Homer 1a, and by gene silencing of TRPC1. Moreover, diminished Homer 1 expression in mouse models of Duchenne's muscular dystrophy suggests that loss of Homer 1 scaffolding of TRP channels may contribute to the increased stretch-activated channel activity observed in mdx myofibers. These findings provide direct evidence that Homer 1 functions as an important scaffold for TRP channels and regulates mechanotransduction in skeletal muscle.

Original language	English (US)
Pages (from-to)	2637-2647
Number of pages	11
Journal	Molecular and cellular biology
Volume	28
Issue number	8
DOIs	https://doi.org/10.1128/MCB.01601-07
State	Published - Apr 2008

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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Stiber, J. A., Zhang, Z. S., Burch, J., Eu, J. P., Zhang, S., Truskey, G. A., Seth, M., Yamaguchi, N., Meissner, G., Shah, R., Worley, P. F., Williams, R. S., & Rosenberg, P. B. (2008). Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity. Molecular and cellular biology, 28(8), 2637-2647. https://doi.org/10.1128/MCB.01601-07

Stiber, JA, Zhang, ZS, Burch, J, Eu, JP, Zhang, S, Truskey, GA, Seth, M, Yamaguchi, N, Meissner, G, Shah, R, Worley, PF, Williams, RS & Rosenberg, PB 2008, 'Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity', Molecular and cellular biology, vol. 28, no. 8, pp. 2637-2647. https://doi.org/10.1128/MCB.01601-07

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title = "Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity",

abstract = "Transient receptor potential (TRP) channels are nonselective cation channels, several of which are expressed in striated muscle. Because the scaffolding protein Homer 1 has been implicated in TRP channel regulation, we hypothesized that Homer proteins play a significant role in skeletal muscle function. Mice lacking Homer 1 exhibited a myopathy characterized by decreased muscle fiber cross-sectional area and decreased skeletal muscle force generation. Homer 1 knockout myotubes displayed increased basal current density and spontaneous cation influx. This spontaneous cation influx in Homer 1 knockout myotubes was blocked by reexpression of Homer 1b, but not Homer 1a, and by gene silencing of TRPC1. Moreover, diminished Homer 1 expression in mouse models of Duchenne's muscular dystrophy suggests that loss of Homer 1 scaffolding of TRP channels may contribute to the increased stretch-activated channel activity observed in mdx myofibers. These findings provide direct evidence that Homer 1 functions as an important scaffold for TRP channels and regulates mechanotransduction in skeletal muscle.",

author = "Stiber, {Jonathan A.} and Zhang, {Zhu Shan} and Jarrett Burch and Eu, {Jerry P.} and Sarah Zhang and Truskey, {George A.} and Malini Seth and Naohiro Yamaguchi and Gerhard Meissner and Ripai Shah and Worley, {Paul F.} and Williams, {R. Sanders} and Rosenberg, {Paul B.}",

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doi = "10.1128/MCB.01601-07",

language = "English (US)",

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AU - Eu, Jerry P.

AU - Zhang, Sarah

AU - Truskey, George A.

AU - Seth, Malini

AU - Yamaguchi, Naohiro

AU - Meissner, Gerhard

AU - Shah, Ripai

AU - Worley, Paul F.

AU - Williams, R. Sanders

AU - Rosenberg, Paul B.

PY - 2008/4

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N2 - Transient receptor potential (TRP) channels are nonselective cation channels, several of which are expressed in striated muscle. Because the scaffolding protein Homer 1 has been implicated in TRP channel regulation, we hypothesized that Homer proteins play a significant role in skeletal muscle function. Mice lacking Homer 1 exhibited a myopathy characterized by decreased muscle fiber cross-sectional area and decreased skeletal muscle force generation. Homer 1 knockout myotubes displayed increased basal current density and spontaneous cation influx. This spontaneous cation influx in Homer 1 knockout myotubes was blocked by reexpression of Homer 1b, but not Homer 1a, and by gene silencing of TRPC1. Moreover, diminished Homer 1 expression in mouse models of Duchenne's muscular dystrophy suggests that loss of Homer 1 scaffolding of TRP channels may contribute to the increased stretch-activated channel activity observed in mdx myofibers. These findings provide direct evidence that Homer 1 functions as an important scaffold for TRP channels and regulates mechanotransduction in skeletal muscle.

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Mice lacking homer 1 exhibit a skeletal myopathy characterized by abnormal transient receptor potential channel activity

Abstract

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