A COL4A4-G394S Variant and Impaired Collagen IV Trimerization in a Patient with Mild Alport Syndrome

Jennefer Kohler; Kohei Omachi; Vivek Charu; Jeffrey H Miner; Vivek Bhalla

doi:10.34067/KID.0005472022

A COL4A4-G394S Variant and Impaired Collagen IV Trimerization in a Patient with Mild Alport Syndrome

Kidney360. 2022 Oct 26;3(11):1899-1908. doi: 10.34067/KID.0005472022. eCollection 2022 Nov 24.

Authors

Jennefer Kohler¹, Kohei Omachi², Vivek Charu³, Jeffrey H Miner², Vivek Bhalla⁴

Affiliations

¹ Division of Cardiovascular Medicine, Department of Medicine, Stanford University School of Medicine, Stanford, California.
² Division of Nephrology, Department of Medicine, Washington University School of Medicine, St. Louis, Missouri.
³ Department of Pathology, Stanford University School of Medicine, Stanford, California.
⁴ Division of Nephrology, Department of Medicine, Stanford School of Medicine, Stanford, California.

Abstract

Background: Missense variants in COL4A genes are often found in patients with an Alport syndrome-like presentation, but their pathogenicity is not always clear. We encountered a woman with microscopic hematuria and proteinuria at 33 years of age with a diagnosis of thin basement membrane disease who was approaching end stage kidney disease at 59 years of age. We hypothesized that this patient's kidney disease was within the spectrum of Alport syndrome.

Methods: We used histologic, genetic, and biochemical approaches to investigate the mechanisms of kidney disease. By immunofluorescence, we investigated collagen IV chain composition of the glomerular basement membrane (GBM). We employed targeted sequencing to search for pathogenic variants in COL4A and other relevant genes. We utilized N- and C-terminal split NanoLuciferase assays to determine the effect of a novel COL4A4 variant of uncertain significance (VUS) on collagen IV heterotrimer formation in vitro. We transfected COL4A4 expression constructs with split NanoLuciferase fragment-fused COL4A3 and COL4A5 constructs into human embryonic kidney 293T cells. To assay for α3α4α5(IV) heterotrimer formation and secretion, we measured luminescence in cell lysates and culture supernatants from transfected cells.

Results: Immunostaining suggested that the collagen α3α4α5(IV) network was present throughout the patient's GBMs. DNA sequencing revealed a novel homozygous VUS: COL4A4 c.1180G>A (p. Gly394Ser). In the C-terminal split luciferase-based α3α4α5(IV) heterotrimer formation assays, luminescence levels for G394S were comparable to WT, but in the N-terminal tag assays, the extracellular luminescence levels for G394S were decreased by approximately 50% compared with WT.

Conclusions: Our cell-based assay provides a platform to test COL4 VUS and shows that G394S impairs assembly of the α3α4α5(IV) N-terminus and subsequent trimer secretion. These data suggest that the COL4A4-G394S variant is pathogenic and causes an atypical mild form of autosomal recessive Alport syndrome.

Keywords: Alport syndrome; basic science; collagen; genetics; glomerular and tubulointerstitial diseases.

Publication types

Case Reports
Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Autoantigens / genetics
Collagen Type IV / genetics
Female
Glomerular Basement Membrane / metabolism
Hematuria / genetics
Humans
Middle Aged
Nephritis, Hereditary* / genetics

Substances

Autoantigens
COL4A4 protein, human
Collagen Type IV

Abstract

Publication types

MeSH terms

Substances

Grants and funding