Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis

Tereza Kmochová; Kendrah O Kidd; Andrew Orr; Aleš Hnízda; Hana Hartmannová; Kateřina Hodaňová; Petr Vyleťal; Karolína Naušová; Vítězslav Brinsa; Helena Trešlová; Jana Sovová; Veronika Barešová; Klára Svojšová; Alena Vrbacká; Viktor Stránecký; Victoria C Robins; Abbigail Taylor; Lauren Martin; Ana Rivas-Chavez; Riley Payne; Heidi A Bleyer; Adrienne Williams; Helmut G Rennke; Astrid Weins; Patrick J Short; Varun Agrawal; Leroy J Storsley; Sushrut S Waikar; Ellen D McPhail; Surendra Dasari; Nelson Leung; Tom Hewlett; Jake Yorke; Daniel Gaston; Laurette Geldenhuys; Mark Samuels; Adam P Levine; Michael West; Helena Hůlková; Petr Pompach; Petr Novák; Richard B Weinberg; Karen Bedard; Martina Živná; Jakub Sikora; Anthony J Bleyer Sr; Stanislav Kmoch

doi:10.1016/j.kint.2023.11.021

Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis

Kidney Int. 2024 Apr;105(4):799-811. doi: 10.1016/j.kint.2023.11.021. Epub 2023 Dec 12.

Authors

Tereza Kmochová¹, Kendrah O Kidd², Andrew Orr³, Aleš Hnízda¹, Hana Hartmannová¹, Kateřina Hodaňová¹, Petr Vyleťal¹, Karolína Naušová¹, Vítězslav Brinsa¹, Helena Trešlová¹, Jana Sovová¹, Veronika Barešová¹, Klára Svojšová¹, Alena Vrbacká¹, Viktor Stránecký¹, Victoria C Robins⁴, Abbigail Taylor⁴, Lauren Martin⁴, Ana Rivas-Chavez⁴, Riley Payne⁴, Heidi A Bleyer⁴, Adrienne Williams⁴, Helmut G Rennke⁵, Astrid Weins⁵, Patrick J Short⁶, Varun Agrawal⁷, Leroy J Storsley⁸, Sushrut S Waikar⁹, Ellen D McPhail¹⁰, Surendra Dasari¹¹, Nelson Leung¹², Tom Hewlett¹³, Jake Yorke¹⁴, Daniel Gaston¹⁴, Laurette Geldenhuys¹⁴, Mark Samuels¹⁵, Adam P Levine¹⁶, Michael West¹³, Helena Hůlková¹⁷, Petr Pompach¹⁸, Petr Novák¹⁸, Richard B Weinberg¹⁹, Karen Bedard²⁰, Martina Živná², Jakub Sikora¹⁷, Anthony J Bleyer Sr²¹, Stanislav Kmoch²

Affiliations

¹ Research Unit for Rare Diseases, Department of Pediatrics and Inherited Metabolic Disorders, First Faculty of Medicine, Charles University, Prague, Czech Republic.
² Research Unit for Rare Diseases, Department of Pediatrics and Inherited Metabolic Disorders, First Faculty of Medicine, Charles University, Prague, Czech Republic; Section on Nephrology, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.
³ Department of Ophthalmology and Visual Sciences, Dalhousie University, Halifax, Nova Scotia, Canada; Department of Pathology, Faculty of Medicine, Dalhousie University, Halifax, Nova Scotia, Canada.
⁴ Section on Nephrology, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.
⁵ Pathology Department, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, USA.
⁶ Sano Genetics Limited, London, UK.
⁷ Division of Nephrology and Hypertension, Larner College of Medicine, University of Vermont, Burlington, Vermont, USA.
⁸ Department of Medicine, University of Manitoba, Winnipeg, Manitoba, Canada.
⁹ Section of Nephrology, Boston University Chobanian and Avedisian School of Medicine, Boston, Massachusetts, USA.
¹⁰ Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota, USA.
¹¹ Department of Quantitative Health Sciences, Mayo Clinic, Rochester, Minnesota, USA.
¹² Division of Nephrology and Hypertension, Division of Hematology, Mayo Clinic, Rochester, Minnesota, USA.
¹³ Division of Nephrology, Department of Medicine, Faculty of Medicine, Dalhousie University, Halifax, Nova Scotia, Canada.
¹⁴ Department of Pathology, Faculty of Medicine, Dalhousie University, Halifax, Nova Scotia, Canada.
¹⁵ Department of Medicine Université de Montréal, Montreal, Quebec, Canada; Department of Biochemistry, Université de Montréal, Montreal, Quebec, Canada; Centre de Recherche du CHU Ste-Justine, Montreal, Quebec, Canada.
¹⁶ Research Department of Pathology, University College London, London, UK.
¹⁷ Research Unit for Rare Diseases, Department of Pediatrics and Inherited Metabolic Disorders, First Faculty of Medicine, Charles University, Prague, Czech Republic; Institute of Pathology, First Faculty of Medicine, Charles University, Prague, Czech Republic.
¹⁸ Institute of Microbiology of the Czech Academy of Sciences, Vestec, Czech Republic.
¹⁹ Section on Gastroenterology, Department of Internal Medicine, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA; Department of Physiology and Pharmacology, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.
²⁰ Department of Pathology and Laboratory Medicine, Izaak Walton Killam Hospital, Halifax Nova Scotia, Canada.
²¹ Research Unit for Rare Diseases, Department of Pediatrics and Inherited Metabolic Disorders, First Faculty of Medicine, Charles University, Prague, Czech Republic; Section on Nephrology, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA. Electronic address: ableyer@wakehealth.edu.

PMID: 38096951
DOI: 10.1016/j.kint.2023.11.021

Abstract

Sporadic cases of apolipoprotein A-IV medullary amyloidosis have been reported. Here we describe five families found to have autosomal dominant medullary amyloidosis due to two different pathogenic APOA4 variants. A large family with autosomal dominant chronic kidney disease (CKD) and bland urinary sediment underwent whole genome sequencing with identification of a chr11:116692578 G>C (hg19) variant encoding the missense mutation p.L66V of the ApoA4 protein. We identified two other distantly related families from our registry with the same variant and two other distantly related families with a chr11:116693454 C>T (hg19) variant encoding the missense mutation p.D33N. Both mutations are unique to affected families, evolutionarily conserved and predicted to expand the amyloidogenic hotspot in the ApoA4 structure. Clinically affected individuals suffered from CKD with a bland urinary sediment and a mean age for kidney failure of 64.5 years. Genotyping identified 48 genetically affected individuals; 44 individuals had an estimated glomerular filtration rate (eGFR) under 60 ml/min/1.73 m², including all 25 individuals with kidney failure. Significantly, 11 of 14 genetically unaffected individuals had an eGFR over 60 ml/min/1.73 m². Fifteen genetically affected individuals presented with higher plasma ApoA4 concentrations. Kidney pathologic specimens from four individuals revealed amyloid deposits limited to the medulla, with the mutated ApoA4 identified by mass-spectrometry as the predominant amyloid constituent in all three available biopsies. Thus, ApoA4 mutations can cause autosomal dominant medullary amyloidosis, with marked amyloid deposition limited to the kidney medulla and presenting with autosomal dominant CKD with a bland urinary sediment. Diagnosis relies on a careful family history, APOA4 sequencing and pathologic studies.

Keywords: AApoA-IV; ApoA4; autosomal dominant tubulointerstitial kidney disease; medullary amyloidosis.

MeSH terms

Amyloidosis*
Apolipoproteins A*
Humans
Middle Aged
Mutation
Nephritis, Interstitial* / complications
Nephritis, Interstitial* / diagnosis
Nephritis, Interstitial* / genetics
Renal Insufficiency, Chronic* / complications
Renal Insufficiency, Chronic* / diagnosis
Renal Insufficiency, Chronic* / genetics

Substances

apolipoprotein A-IV
Apolipoproteins A