PUBLICATION

Individuals with mutations in XPNPEP3, which encodes a mitochondrial protein, develop a nephronophthisis-like nephropathy

Authors

O'Toole, J.F., Liu, Y., Davis, E.E., Westlake, C.J., Attanasio, M., Otto, E.A., Seelow, D., Nurnberg, G., Becker, C., Nuutinen, M., Kärppä, M., Ignatius, J., Uusimaa, J., Pakanen, S., Jaakkola, E., van den Heuvel, L.P., Fehrenbach, H., Wiggins, R., Goyal, M., Zhou, W., Wolf, M.T., Wise, E., Helou, J., Allen, S.J., Murga-Zamalloa, C.A., Ashraf, S., Chaki, M., Heeringa, S., Chernin, G., Hoskins, B.E., Chaib, H., Gleeson, J., Kusakabe, T., Suzuki, T., Isaac, R.E., Quarmby, L.M., Tennant, B., Fujioka, H., Tuominen, H., Hassinen, I., Lohi, H., van Houten, J.L., Rotig, A., Sayer, J.A., Rolinski, B., Freisinger, P., Madhavan, S.M., Herzer, M., Madignier, F., Prokisch, H., Nurnberg, P., Jackson, P., Khanna, H., Katsanis, N., and Hildebrandt, F.

ID

ZDB-PUB-100302-5

Date

2010

Source

J. Clin. Invest. 120(3): 791-802 (Journal)

Registered Authors

Davis, Erica, Katsanis, Nicholas, Khanna, Hemant, Zhou, Weibin

Keywords

none

MeSH Terms

Aminopeptidases/genetics
Aminopeptidases/metabolism*
Animals
Centrosome/enzymology
Centrosome/pathology
Chromosome Mapping/methods
Cilia/enzymology
Cilia/genetics
Cilia/pathology
Family
Female
Genetic Diseases, Inborn/enzymology*
Genetic Diseases, Inborn/genetics
Genetic Diseases, Inborn/pathology
Genome-Wide Association Study/methods
Humans
Kidney/enzymology*
Kidney/pathology
Male
Mitochondria/enzymology*
Mitochondria/pathology
Mitochondrial Proteins/genetics
Mitochondrial Proteins/metabolism*
Rats
Rats, Sprague-Dawley
Renal Insufficiency/enzymology*
Renal Insufficiency/genetics
Renal Insufficiency/pathology
Zebrafish/embryology
Zebrafish/genetics
Zebrafish/metabolism

PubMed

20179356 Full text @ J. Clin. Invest.

Abstract

The autosomal recessive kidney disease nephronophthisis (NPHP) constitutes the most frequent genetic cause of terminal renal failure in the first 3 decades of life. Ten causative genes (NPHP1-NPHP9 and NPHP11), whose products localize to the primary cilia-centrosome complex, support the unifying concept that cystic kidney diseases are "ciliopathies". Using genome-wide homozygosity mapping, we report here what we believe to be a new locus (NPHP-like 1 [NPHPL1]) for an NPHP-like nephropathy. In 2 families with an NPHP-like phenotype, we detected homozygous frameshift and splice-site mutations, respectively, in the X-prolyl aminopeptidase 3 (XPNPEP3) gene. In contrast to all known NPHP proteins, XPNPEP3 localizes to mitochondria of renal cells. However, in vivo analyses also revealed a likely cilia-related function; suppression of zebrafish xpnpep3 phenocopied the developmental phenotypes of ciliopathy morphants, and this effect was rescued by human XPNPEP3 that was devoid of a mitochondrial localization signal. Consistent with a role for XPNPEP3 in ciliary function, several ciliary cystogenic proteins were found to be XPNPEP3 substrates, for which resistance to N-terminal proline cleavage resulted in attenuated protein function in vivo in zebrafish. Our data highlight an emerging link between mitochondria and ciliary dysfunction, and suggest that further understanding the enzymatic activity and substrates of XPNPEP3 will illuminate novel cystogenic pathways.

Genes / Markers

Figures

Show all Figures

Expression

Phenotype

Mutations / Transgenics

Human Disease / Model

Sequence Targeting Reagents

Fish

Antibodies

Orthology

Engineered Foreign Genes

Mapping

O'Toole et al., 2010 ZDB-PUB-100302-5 PMID:20179356

Individuals with mutations in XPNPEP3, which encodes a mitochondrial protein, develop a nephronophthisis-like nephropathy

O'Toole et al., 2010

ZDB-PUB-100302-5
PMID:20179356