KLHL40 deficiency destabilizes thin filament proteins and promotes nemaline myopathy
Ankit Garg, … , Rhonda Bassel-Duby, Eric N. Olson
Ankit Garg, … , Rhonda Bassel-Duby, Eric N. Olson
Published June 24, 2014
Citation Information: J Clin Invest. 2014;124(8):3529-3539. https://doi.org/10.1172/JCI74994.
View: Text | PDF
Research Article

KLHL40 deficiency destabilizes thin filament proteins and promotes nemaline myopathy

Abstract

Nemaline myopathy (NM) is a congenital myopathy that can result in lethal muscle dysfunction and is thought to be a disease of the sarcomere thin filament. Recently, several proteins of unknown function have been implicated in NM, but the mechanistic basis of their contribution to disease remains unresolved. Here, we demonstrated that loss of a muscle-specific protein, kelch-like family member 40 (KLHL40), results in a nemaline-like myopathy in mice that closely phenocopies muscle abnormalities observed in KLHL40-deficient patients. We determined that KLHL40 localizes to the sarcomere I band and A band and binds to nebulin (NEB), a protein frequently implicated in NM, as well as a putative thin filament protein, leiomodin 3 (LMOD3). KLHL40 belongs to the BTB-BACK-kelch (BBK) family of proteins, some of which have been shown to promote degradation of their substrates. In contrast, we found that KLHL40 promotes stability of NEB and LMOD3 and blocks LMOD3 ubiquitination. Accordingly, NEB and LMOD3 were reduced in skeletal muscle of both Klhl40–/– mice and KLHL40-deficient patients. Loss of sarcomere thin filament proteins is a frequent cause of NM; therefore, our data that KLHL40 stabilizes NEB and LMOD3 provide a potential basis for the development of NM in KLHL40-deficient patients.

Authors

Ankit Garg, Jason O’Rourke, Chengzu Long, Jonathan Doering, Gianina Ravenscroft, Svetlana Bezprozvannaya, Benjamin R. Nelson, Nadine Beetz, Lin Li, She Chen, Nigel G. Laing, Robert W. Grange, Rhonda Bassel-Duby, Eric N. Olson

×

Figure 1

Klhl40 is expressed specifically in skeletal muscle and heart, and deletion of Klhl40 causes neonatal lethality.

Options: View larger image (or click on image) Download as PowerPoint
Klhl40 is expressed specifically in skeletal muscle and heart, and delet...
(A) Sagittal sections of E15 mouse embryos were probed for Klhl40 mRNA using antisense radioisotopic probes. Signal for Klhl40 (pseudocolored red) only appears in developing muscle. Black arrows point to representative developing intercostal and back muscles from rostral to caudal, respectively. The black arrowhead denotes heart. Scale bar: 1 mm. (B) Northern blot of adult mouse tissues for Klhl40 and Gapdh (loading control) shows Klhl40 expression in skeletal muscle and heart. Numbers on right indicate size of transcripts in kilobases. SK Muscle, skeletal muscle. (C) qPCR analysis of Klhl40 transcript in P8 quadriceps in mice of the indicated genotypes. Values are normalized to 18S ribosomal RNA (n = 3 for both genotypes). #P < 0.05. (D) Representative image of surviving P8 KO pups with WT littermates. (E) Survival curve of WT versus KO mice shows early neonatal lethality in KO mice (WT, n = 21, and KO, n = 17).