Mutations in KEOPS-complex genes cause nephrotic syndrome with primary microcephaly.
Daniela A BraunJia RaoGeraldine MolletDavid SchapiroMarie-Claire DaugeronWeizhen TanOlivier GribouvalOlivia BoyerPatrick RevyTilman Jobst-SchwanJohanna Magdalena SchmidtJennifer A LawsonDenny SchanzeShazia AshrafJeremy F P UllmannCharlotte A HoogstratenNathalie BoddaertBruno CollinetGaëlle MartinDominique LigerSvjetlana LovricMonica FurlanoI Chiara GuerreraOraly Sanchez-FerrasJennifer F HuAnne-Claire BoschatSylvia SanquerBjörn MentenSarah VergultNina De RockerMerlin AirikTobias HermleShirlee ShrilEugen WidmeierHeon Yung GeeWon-Il ChoiCarolin E SadowskiWerner L PabstJillian K WarejkoAnkana DagaTamara BastaVerena MatejasKarin ScharmannSandra D KienastBabak BehnamBrendan BeesonAmber BegtrupMalcolm BruceGaik-Siew Ch'ngShuan-Pei LinJui-Hsing ChangChao-Huei ChenMegan T ChoPatrick M GaffneyPatrick E GipsonChyong-Hsin HsuJameela A KariYu-Yuan KeCathy Kiraly-BorriWai-Ming LaiEmmanuelle LemyreRebecca Okashah LittlejohnAmira MasriMastaneh MoghtaderiKazuyuki NakamuraFatih OzaltinMarleen PraetChitra PrasadAgnieszka PrytułaElizabeth R RoederPatrick RumpRhonda E SchnurTakashi ShiiharaManish D SinhaNeveen A SolimanKenza SoulamiDavid A SweetserWen-Hui TsaiJeng-Daw TsaiRezan TopalogluUdo VesterDavid H ViskochilNithiwat VatanavicharnJessica L WaxlerKlaas J WierengaMatthias T F WolfSik-Nin WongSebastian A LeidelGessica TruglioPeter C DedonAnnapurna PoduriShrikant ManeRichard P LiftonMaxime BouchardPeter KannuDavid ChitayatDaniella MagenBert CallewaertHerman van TilbeurghMartin ZenkerCorinne AntignacFriedhelm HildebrandtPublished in: Nature genetics (2017)
Galloway-Mowat syndrome (GAMOS) is an autosomal-recessive disease characterized by the combination of early-onset nephrotic syndrome (SRNS) and microcephaly with brain anomalies. Here we identified recessive mutations in OSGEP, TP53RK, TPRKB, and LAGE3, genes encoding the four subunits of the KEOPS complex, in 37 individuals from 32 families with GAMOS. CRISPR-Cas9 knockout in zebrafish and mice recapitulated the human phenotype of primary microcephaly and resulted in early lethality. Knockdown of OSGEP, TP53RK, or TPRKB inhibited cell proliferation, which human mutations did not rescue. Furthermore, knockdown of these genes impaired protein translation, caused endoplasmic reticulum stress, activated DNA-damage-response signaling, and ultimately induced apoptosis. Knockdown of OSGEP or TP53RK induced defects in the actin cytoskeleton and decreased the migration rate of human podocytes, an established intermediate phenotype of SRNS. We thus identified four new monogenic causes of GAMOS, describe a link between KEOPS function and human disease, and delineate potential pathogenic mechanisms.
Keyphrases
- endoplasmic reticulum stress
- endothelial cells
- induced apoptosis
- early onset
- zika virus
- intellectual disability
- cell proliferation
- crispr cas
- high glucose
- dna damage response
- pluripotent stem cells
- genome wide
- late onset
- signaling pathway
- cell cycle
- insulin resistance
- white matter
- brain injury
- climate change
- subarachnoid hemorrhage
- protein protein
- genome wide identification
- risk assessment
- high fat diet induced