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Alport Syndrome: Clinical Spectrum and Therapeutic Advances

Vanessa De Gregorio, Emine Bilge Çaparali, Azadeh Shojaei, Samantha Ricardo, Moumita Barua

2023Kidney Medicine45 citationsDOIOpen Access PDF

Abstract

(chromosome Xq22), encoding the α3, α4, and α5 chains of type IV collagen, as the responsible genes. Subsequent studies suggested that autosomal recessive Alport syndrome and males with X-linked Alport syndrome have more severe disease, whereas autosomal dominant Alport syndrome and females with X-linked Alport syndrome have more variability. Variant type is also influential-protein-truncating variants in autosomal recessive Alport syndrome or males with X-linked Alport syndrome often present with severe symptoms, characterized by kidney failure, extrarenal manifestations, and lack of the α3-α4-α5(IV) network. By contrast, mild-moderate forms from missense variants display α3-α4-α5(IV) in the glomerular basement membrane and are associated with protracted kidney involvement without extrarenal manifestations. Regardless of type, therapeutic intervention for kidney involvement is focused on early initiation of angiotensin-converting enzyme inhibitors. There are several therapies under investigation including sodium/glucose cotransporter 2 inhibitors, aminoglycoside analogs, endothelin type A antagonists, lipid-modifying drugs, and hydroxychloroquine, although targeting the underlying defect through gene therapy remains in preclinical stages.

Topics & Concepts

Alport syndromeType IV collagenX chromosomeSensorineural hearing lossHearing lossMedicineGlomerular basement membraneGlomerulonephritisGeneticsKidneyInternal medicineEndocrinologyBiologyPathologyLamininGeneCellAudiologyCell Adhesion Molecules ResearchCoagulation, Bradykinin, Polyphosphates, and AngioedemaBlood Coagulation and Thrombosis Mechanisms
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