Loss of polycystin-1 causes centrosome amplification and genomic instability

doi:10.1093/hmg/ddn180

Human Molecular Genetics Advance Access originally published online on June 19, 2008
Human Molecular Genetics 2008 17(18):2819-2833; doi:10.1093/hmg/ddn180

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Loss of polycystin-1 causes centrosome amplification and genomic instability

Lorenzo Battini¹, Salvador Macip², Elena Fedorova¹, Steven Dikman³, Stefan Somlo⁴, Cristina Montagna⁵ and G. Luca Gusella¹^,*

¹ Division of Renal Medicine ² Department of Oncological Sciences ³ Department of Pathology, Mount Sinai School of Medicine, One Gustave Levy Place, Box 1243 New York, NY 10029, USA ⁴ Department of Internal Medicine and Genetics, Yale University School of Medicine, New Haven, CT, USA ⁵ Department of Pathology, Albert Einstein College of Medicine, Bronx, NY, USA

^* To whom correspondence should be addressed. Tel: +1 212 241 9597; Fax: +1 212 987 0389; Email: luca.gusella{at}mssm.edu

Received April 27, 2008; Accepted June 16, 2008

Autosomal dominant polycystic kidney disease (ADPKD) is themost common monogenetic disease predominantly caused by alterationor dysregulation of the PKD1 gene, which encodes polycystin-1(PC1). The disease is characterized by the progressive expansionof bilateral fluid-filled renal cysts that ultimately lead torenal failure. Individual cysts, even within patients with germlinemutations, are genetically heterogeneous, displaying diversechromosomal abnormalities. To date, the molecular mechanismsresponsible for this genetic heterogeneity remain unknown. Usinga lentiviral-mediated siRNA expression model of Pkd1 hypomorphism,we show that loss of PC1 function is sufficient to produce centrosomeamplification and multipolar spindle formation. These eventslead to genomic instability characterized by gross polyploidismand mitotic catastrophe. Following these dramatic early changes,the cell population rapidly converges toward a stable ploidyin which centrosome amplification is significantly decreased,though cytological abnormalities such as micronucleation, chromatinbridges and aneuploidy remain common. In agreement with ourin vitro findings, we provide the first in vivo evidence thatsignificant centrosome amplification occurs in kidneys fromconditional Pkd1 knockout mice at early and late time duringthe disease progression as well as in human ADPKD patients.These findings establish a novel function of PC1 in ADPKD pathogenesisand a genetic mechanism that may underlie the intrafamilialvariability of ADPKD progression.

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