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; Stanislav Kmoch

doi:10.1016/j.kint.2023.11.021

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 PayneHeidi 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, Stanislav Kmoch

Research output: Contribution to journal › Article › peer-review

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.

Original language	English (US)
Pages (from-to)	799-811
Number of pages	13
Journal	Kidney international
Volume	105
Issue number	4
DOIs	https://doi.org/10.1016/j.kint.2023.11.021
State	Published - Apr 2024

Keywords

AApoA-IV
ApoA4
autosomal dominant tubulointerstitial kidney disease
medullary amyloidosis

ASJC Scopus subject areas

Nephrology

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10.1016/j.kint.2023.11.021

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Kmochová, T., Kidd, K. O., Orr, A., Hnízda, A., Hartmannová, H., Hodaňová, K., Vyleťal, P., Naušová, K., Brinsa, V., Trešlová, H., Sovová, J., Barešová, V., Svojšová, K., Vrbacká, A., Stránecký, V., Robins, V. C., Taylor, A., Martin, L., Rivas-Chavez, A., ... Kmoch, S. (2024). Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis. Kidney international, 105(4), 799-811. https://doi.org/10.1016/j.kint.2023.11.021

Kmochová, T, Kidd, KO, Orr, A, Hnízda, A, Hartmannová, H, Hodaňová, K, Vyleťal, P, Naušová, K, Brinsa, V, Trešlová, H, Sovová, J, Barešová, V, Svojšová, K, Vrbacká, A, Stránecký, V, Robins, VC, Taylor, A, Martin, L, Rivas-Chavez, A, Payne, R, Bleyer, HA, Williams, A, Rennke, HG, Weins, A, Short, PJ, Agrawal, V, Storsley, LJ, Waikar, SS, McPhail, ED , Dasari, S, Leung, N, Hewlett, T, Yorke, J, Gaston, D, Geldenhuys, L, Samuels, M, Levine, AP, West, M, Hůlková, H, Pompach, P, Novák, P, Weinberg, RB, Bedard, K, Živná, M, Sikora, J, Bleyer, AJ & Kmoch, S 2024, 'Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis', Kidney international, vol. 105, no. 4, pp. 799-811. https://doi.org/10.1016/j.kint.2023.11.021

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title = "Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis",

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.",

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author = "Tereza Kmochov{\'a} and Kidd, {Kendrah O.} and Andrew Orr and Ale{\v s} Hn{\'i}zda and Hana Hartmannov{\'a} and Kate{\v r}ina Hoda{\v n}ov{\'a} and Petr Vyle{\v t}al and Karol{\'i}na Nau{\v s}ov{\'a} and V{\'i}t{\v e}zslav Brinsa and Helena Tre{\v s}lov{\'a} and Jana Sovov{\'a} and Veronika Bare{\v s}ov{\'a} and Kl{\'a}ra Svoj{\v s}ov{\'a} and Alena Vrback{\'a} and Viktor Str{\'a}neck{\'y} and Robins, {Victoria C.} and Abbigail Taylor and Lauren Martin and Ana Rivas-Chavez and Riley Payne and Bleyer, {Heidi A.} and Adrienne Williams and Rennke, {Helmut G.} and Astrid Weins and Short, {Patrick J.} and Varun Agrawal and Storsley, {Leroy J.} and Waikar, {Sushrut S.} and McPhail, {Ellen D.} and Surendra Dasari and Nelson Leung and Tom Hewlett and Jake Yorke and Daniel Gaston and Laurette Geldenhuys and Mark Samuels and Levine, {Adam P.} and Michael West and Helena Hůlkov{\'a} and Petr Pompach and Petr Nov{\'a}k and Weinberg, {Richard B.} and Karen Bedard and Martina {\v Z}ivn{\'a} and Jakub Sikora and Bleyer, {Anthony J.} and Stanislav Kmoch",

note = "Publisher Copyright: {\textcopyright} 2023 International Society of Nephrology",

year = "2024",

month = apr,

doi = "10.1016/j.kint.2023.11.021",

language = "English (US)",

volume = "105",

pages = "799--811",

journal = "Kidney international",

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T1 - Autosomal dominant ApoA4 mutations present as tubulointerstitial kidney disease with medullary amyloidosis

AU - Kmochová, Tereza

AU - Kidd, Kendrah O.

AU - Orr, Andrew

AU - Hnízda, Aleš

AU - Hartmannová, Hana

AU - Hodaňová, Kateřina

AU - Vyleťal, Petr

AU - Naušová, Karolína

AU - Brinsa, Vítězslav

AU - Trešlová, Helena

AU - Sovová, Jana

AU - Barešová, Veronika

AU - Svojšová, Klára

AU - Vrbacká, Alena

AU - Stránecký, Viktor

AU - Robins, Victoria C.

AU - Taylor, Abbigail

AU - Martin, Lauren

AU - Rivas-Chavez, Ana

AU - Payne, Riley

AU - Bleyer, Heidi A.

AU - Williams, Adrienne

AU - Rennke, Helmut G.

AU - Weins, Astrid

AU - Short, Patrick J.

AU - Agrawal, Varun

AU - Storsley, Leroy J.

AU - Waikar, Sushrut S.

AU - McPhail, Ellen D.

AU - Dasari, Surendra

AU - Leung, Nelson

AU - Hewlett, Tom

AU - Yorke, Jake

AU - Gaston, Daniel

AU - Geldenhuys, Laurette

AU - Samuels, Mark

AU - Levine, Adam P.

AU - West, Michael

AU - Hůlková, Helena

AU - Pompach, Petr

AU - Novák, Petr

AU - Weinberg, Richard B.

AU - Bedard, Karen

AU - Živná, Martina

AU - Sikora, Jakub

AU - Bleyer, Anthony J.

AU - Kmoch, Stanislav

PY - 2024/4

Y1 - 2024/4

N2 - 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.

AB - 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.

KW - AApoA-IV

KW - ApoA4

KW - autosomal dominant tubulointerstitial kidney disease

KW - medullary amyloidosis

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SN - 0085-2538

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JO - Kidney international

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

Abstract

Keywords

ASJC Scopus subject areas

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