Loss of Myh14 Increases Susceptibility to Noise-Induced Hearing Loss in CBA/CaJ Mice

Fu, Xiaolong; Zhang, Linqing; Jin, Yecheng; Sun, Xiaoyang; Zhang, Aizhen; Wen, Zongzhuang; Zhou, Yisu; Xia, Mengna; Gao, Jiangang

doi:10.1155/2016/6720420

Cited by 36 publications

(28 citation statements)

References 44 publications

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“…Disruption of the pathway by mutation of R788 to a glutamate causes the loss of its enzymatic signatures and results in a high duty ratio motor. Importantly, several key residues involved in the allosteric communication pathway are implicated in the onset and progression of debilitating human diseases ( Fu et al, 2016 ; Donaudy et al, 2004 ; Kim et al, 2017 ). Missense mutation G376C is in proximity to residues C324 of helix J and R328 of the JK-loop ( Figure 4—figure supplement 1F ).…”

Section: Discussionmentioning

confidence: 99%

Mechanistic insights into the active site and allosteric communication pathways in human nonmuscle myosin-2C

Chinthalapudi

Heissler

Preller

et al. 2017

eLife

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Despite a generic, highly conserved motor domain, ATP turnover kinetics and their activation by F-actin vary greatly between myosin-2 isoforms. Here, we present a 2.25 Å pre-powerstroke state (ADP⋅VO4) crystal structure of the human nonmuscle myosin-2C motor domain, one of the slowest myosins characterized. In combination with integrated mutagenesis, ensemble-solution kinetics, and molecular dynamics simulation approaches, the structure reveals an allosteric communication pathway that connects the distal end of the motor domain with the active site. Disruption of this pathway by mutation of hub residue R788, which forms the center of a cluster of interactions connecting the converter, the SH1-SH2 helix, the relay helix, and the lever, abolishes nonmuscle myosin-2 specific kinetic signatures. Our results provide insights into structural changes in the myosin motor domain that are triggered upon F-actin binding and contribute critically to the mechanochemical behavior of stress fibers, actin arcs, and cortical actin-based structures.

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Section: Discussionmentioning

confidence: 99%

Mechanistic insights into the active site and allosteric communication pathways in human nonmuscle myosin-2C

Chinthalapudi

Heissler

Preller

et al. 2017

eLife

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“…Auditory brainstem responses (ABRs) and distortion product otoacoustic emissions (DPOAEs) were measured as described previously (ref. 62; and see Supplemental Methods).…”

Section: Author Contributionsmentioning

confidence: 99%

Tuberous sclerosis complex–mediated mTORC1 overactivation promotes age-related hearing loss

Fu¹,

Sun²,

Zhang³

et al. 2018

Journal of Clinical Investigation

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“…NM2C exhibits specific expression to pituitary gland and glial cells, as well as inner ear sensory, intestinal, and kidney epithelia (32). Mutations in MYH14 have been linked to hearing loss, peripheral neuropathies, and developmental defects in the lower gastrointestinal tract (33)(34)(35)(36)(37)(38)(39)(40)(41). The parallel perturbation of both inner ear and intestinal epithelial systems by mutations in MYH14 is intriguing, as actin bundled-supported stereocilia found on the apical surface of hair cells are closely related to microvilli found on solute transporting epithelia, and may share mechanisms of assembly and maintenance (42,43).…”

Section: Introductionmentioning

confidence: 99%

Non-muscle myosin-2 contractility-dependent actin turnover limits the length of epithelial microvilli

Chinowsky

Pinette

Meenderink

et al. 2020

Preprint

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Epithelial brush borders are large arrays of microvilli that enable efficient solute uptake from luminal spaces. In the context of the intestinal tract, brush border microvilli drive functions that are critical for physiological homeostasis, including nutrient uptake and host defense. However, cytoskeletal mechanisms that regulate the assembly and morphology of these protrusions are poorly understood. The parallel actin bundles that support microvilli have their pointed-end rootlets anchored in a highly crosslinked filamentous meshwork referred to as the "terminal web".Although classic EM studies revealed complex ultrastructure, the composition, organization, and function of the terminal web remains unclear. Here, we identify non-muscle myosin-2C (NM2C) as a major component of the brush border terminal web. NM2C is found in a dense, isotropic layer of puncta across the sub-apical domain, which transects the rootlets of microvillar actin bundles.Puncta in this network are separated by ~210 nm, dimensions that are comparable to the expected size of filaments formed by NM2C. In primary intestinal organoid cultures, the terminal web NM2C network is highly dynamic and exhibits continuous remodeling. Using pharmacological and genetic perturbations to disrupt NM2C activity in cultured intestinal epithelial cells, we found that this motor controls the length of growing microvilli by regulating actin turnover in a manner that requires a fully active motor domain. Our findings answer a decades old question on the function of terminal web myosin and hold broad implications for understanding apical morphogenesis in diverse epithelial systems.

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Loss of Myh14 Increases Susceptibility to Noise-Induced Hearing Loss in CBA/CaJ Mice

Cited by 36 publications

References 44 publications

Mechanistic insights into the active site and allosteric communication pathways in human nonmuscle myosin-2C

Mechanistic insights into the active site and allosteric communication pathways in human nonmuscle myosin-2C

Tuberous sclerosis complex–mediated mTORC1 overactivation promotes age-related hearing loss

Non-muscle myosin-2 contractility-dependent actin turnover limits the length of epithelial microvilli

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