# MYH9 Variant p.(Arg424Gly) Alters Nonmuscle Myosin IIA Contraction, Causing Atypical MYH9-related Disease

**Authors:** Lena Pollinger, Johannes N. Greve, Melanie Grosch, Sara Kaliman, Shada Abuhattum, Martin Kräter, Ina Brauer, Jan T. Schaefer, Francesca Pasutto, Antje Wiesener, Florian J. Wopperer, Cathiana Kolb, Christian H.K. Lehmann, André Hoerning, Christoph Daniel, Kerstin Amann, Jochen Guck, Mario Schiffer, Dietmar J. Manstein, Michael S. Wiesener, Tilman Jobst-Schwan

PMC · DOI: 10.1016/j.ekir.2026.106343 · 2026-02-03

## TL;DR

A new MYH9 gene variant causes a rare disease by increasing the activity of a muscle-related protein, leading to kidney and liver issues.

## Contribution

This study identifies a novel gain-of-function MYH9 variant causing atypical MYH9-related disease.

## Key findings

- The p.(Arg424Gly) variant increases ATP turnover and motor activity of nonmuscle myosin IIA.
- The variant is fully segregating in a family and causes proteinuric kidney disease and elevated liver enzymes.
- The disease mechanism is linked to enhanced intrinsic motor activity of the variant protein.

## Abstract

Pathogenic variants in myosin heavy chain 9 (MYH9), encoding the heavy chain of nonmuscle myosin IIA (NMMIIA), cause autosomal-dominant MYH9-related disease that may include proteinuric kidney disease, macrothrombocytopenia, cataract, sensorineural deafness, and elevated liver enzymes.

Whole exome sequencing and segregation analysis were performed in a patient with end-stage renal disease. Histology of kidney and liver biopsies was assessed and blood smears were examined for the presence of Döhle-like bodies. Deformability cytometry and monocyte migration assays were performed. Immortalized podocytes and primary skin fibroblasts of 1 patient were transfected with plasmids containing MYH9 wild type (WT) or the p.(Arg424Gly) variant. Biochemical studies using recombinantly produced proteins were conducted to assess the variant’s impact on adenosine triphosphate (ATP) turnover and motor function.

We identified the likely pathogenic heterozygous MYH9 variant c.1270C>G, p.(Arg424Gly) in all affected members of a nonconsanguineous family. Typical microscopic findings, such as Döhle-like bodies or NMMIIA conglomerates were absent. Nonetheless, all patients presented with proteinuric kidney disease, elevated liver enzymes, and intermittent thrombocytopenia. The altered protein showed increased ATP turnover in the presence of actin and enhanced motor activity under both unloaded and loaded conditions.

We identified a novel fully segregating MYH9 variant causing MYH9-related disease. Based on biochemical findings, we report the first gain-of-function variant of MYH9. We propose that the enhanced intrinsic motor activity of the p.(Arg424Gly) variant is a key contributor to the disease mechanism. Incorporation of the p.(Arg424Gly) variant into nonmuscle myosin IIA filaments and higher-order actomyosin assemblies may, in principle, affect actomyosin dynamics.

## Linked entities

- **Genes:** MYH9 (myosin heavy chain 9) [NCBI Gene 4627]
- **Chemicals:** adenosine triphosphate (PubChem CID 5957), ATP (PubChem CID 5957)
- **Diseases:** MYH9-related disease (MONDO:0015912), end-stage renal disease (MONDO:0004375)

## Full-text entities

- **Genes:** MYH9 (myosin heavy chain 9) [NCBI Gene 4627] {aka BDPLT6, DFNA17, EPSTS, FTNS, MATINS, MHA}, TMEM11 (transmembrane protein 11) [NCBI Gene 8834] {aka C17orf35, PM1, PMI}, POTEF (POTE ankyrin domain family member F) [NCBI Gene 728378] {aka A26C1B, POTE2alpha, POTEACTIN}, NPY4R (neuropeptide Y receptor Y4) [NCBI Gene 5540] {aka NPY4-R, PP1, PPYR1, Y4}, ACTN1 (actinin alpha 1) [NCBI Gene 87] {aka BDPLT15}, GGT1 (gamma-glutamyltransferase 1) [NCBI Gene 2678] {aka CD224, D22S672, D22S732, GGT, GGT 1, GGTD}, VCL (vinculin) [NCBI Gene 7414] {aka CMD1W, CMH15, HEL114, MV, MVCL, VINC}, MYH14 (myosin heavy chain 14) [NCBI Gene 79784] {aka DFNA4, DFNA4A, FP17425, MHC16, MYH17, NMHC II-C}, MYH2 (myosin heavy chain 2) [NCBI Gene 4620] {aka CMYO6, CMYP6, IBM3, MYH2A, MYHSA2, MYHas8}, DNAH8 (dynein axonemal heavy chain 8) [NCBI Gene 1769] {aka ATPase, SPGF46, hdhc9}, MAP1LC3B (microtubule associated protein 1 light chain 3 beta) [NCBI Gene 81631] {aka ATG8F, LC3B, MAP1A/1BLC3, MAP1LC3B-a}, ATP1B1 (ATPase Na+/K+ transporting subunit beta 1) [NCBI Gene 481] {aka ATP1B}
- **Diseases:** monogenic disorder (MESH:D009358), proteinuria (MESH:D011507), sensorineural deafness (MESH:D006319), MYH9-RD (MESH:D006362), bleeding (MESH:D006470), autoimmune diseases (MESH:D001327), focal segmental glomerulosclerosis (MESH:D005923), macrothrombocytopenia (OMIM:616737), chronic kidney disease (MESH:D051436), -dominant (MESH:C566739), impaired liver function (MESH:D008107), Epstein-Fechtner syndrome (MESH:C535507), NMMIIA (MESH:C564253), kidney disease (MESH:D007674), congenital platelet macrocytosis (MESH:C564004), cataract (MESH:D002386), renal involvement (MESH:C565423), primary (MESH:D010538), thrombocytopenia (MESH:D013921), MPGN (MESH:D015432), ESRD (MESH:D007676), infections (MESH:D007239), rare (MESH:D035583), Alport syndrome (MESH:D009394)
- **Chemicals:** Ponceau (MESH:C032756), nucleotide (MESH:D009711), BafA (MESH:C057620), methylcellulose (MESH:D008747), ADP (MESH:D000244), Ni (MESH:D009532), TRITC-phalloidin (MESH:C041085), osmium tetroxide (MESH:D009993), phalloidin (MESH:D010590), paraffin (MESH:D010232), Periodic Acid (MESH:D010504), dimethylsulfoxide (MESH:D004121), 4',6-diamidino-2-phenylindole (MESH:C007293), formalin (MESH:D005557), PVDF (MESH:C024865), reduced nicotinamide adenine dinucleotide (MESH:D009243), Lipopolysaccharide (MESH:D008070), ATP (MESH:D000255), TRITC (MESH:C009434), uranyl acetate (MESH:C005460), Hoechst (-)
- **Species:** Spodoptera frugiperda (fall armyworm, species) [taxon 7108], Gallus gallus (bantam, species) [taxon 9031], Oryctolagus cuniculus (domestic rabbit, species) [taxon 9986], Homo sapiens (human, species) [taxon 9606]
- **Mutations:** Arg424Gly, E334Q, ATG9A, c.1270C>G, p.Asn93Lys, Arg424Gly, E1841K, p.Arg705His, p.Arg1162Ser, R702
- **Cell lines:** Sf9 — Spodoptera frugiperda (Fall armyworm), Spontaneously immortalized cell line (CVCL_0549), NMMIIA-2R — Mus musculus (Mouse), Mouse reticulum cell sarcoma, Cancer cell line (CVCL_0J27), Madin-Darby canine kidney — Canis lupus familiaris (Dog), Spontaneously immortalized cell line (CVCL_0422)

## Figures

6 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12966671/full.md

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Source: https://tomesphere.com/paper/PMC12966671