In vitro demonstration of intra-locus compensation using the ornithine transcarbamylase protein as model

doi:10.1093/hmg/ddm172

Human Molecular Genetics Advance Access originally published online on July 5, 2007
Human Molecular Genetics 2007 16(18):2209-2214; doi:10.1093/hmg/ddm172

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In vitro demonstration of intra-locus compensation using the ornithine transcarbamylase protein as model

Gianpaolo Suriano¹^,2^,*, Luisa Azevedo¹, Marta Novais¹, Barbara Boscolo³, Raquel Seruca¹^,2, Antonio Amorim¹ and Elena Maria Ghibaudi³

¹ Institute of Molecular Pathology and Immunology of the University of Porto (IPATIMUP), Porto, Portugal, ² Faculty of Medicine, University of Porto, Porto, Portugal and ³ Department of Inorganic, Physical and Material Chemistry, University of Torino, Torino, Italy

^* To whom correspondence should be addressed at: Institute of Molecular Pathology and Immunology of the University of Porto (IPATIMUP), rua Dr Roberto Frias, s/n 4200-465 Porto, Portugal. Tel: +351 225570730; Fax: +351 225570799; Email: gsuriano{at}ipatimup.pt

Received May 16, 2007; Accepted July 2, 2007

Ornithine transcarbamylase deficiency (OTCD) is an X-linkedinborn defect of metabolism of the urea cycle, which causeshyperamonemia. Mutations of the OTC gene have been recognizedas the genetic cause underlying the OTC deficiency. The severityof the disease is associated with the type of mutation, leadingeither to neonatal onset of hyperammonemia or to a later appearanceof the disease. The mutation Thr125Met is associated with neonatalhyperammonemia. Recently, the disease-causing Thr125Met mutationin humans was reported as wild-type neutral allele in chimpanzees.Further analysis confirmed the presence of Met125 fixed in chimpanzeestogether with Thr135, representing the only two divergent positionsbetween human and chimpanzee OTCs. Thr125 and Thr135 were identifiedas ancestral mammalian combination, so the Thr135Ala substitutionoccurred as human-specific event, whereas the substitution ofThr125Met was characteristic of the chimpanzee linage. Onlywhen Met125 emerges in a background with the human-specificAla135, a highly deleterious effect is observed, suggestingamong other hypotheses the existence of a compensatory effectin chimpanzee. To explore this hypothesis, we built an in vitrocell model system to study the effect of the three distinctgenetic backgrounds (Ala135–Thr125; Ala135–Met125and Thr135–Met125) on the OTC protein function. We observedthat the human Thr125Met mutant is inactive, whereas the chimpOTC shows an enzymatic activity comparable with the wild-typehuman OTC. We concluded that the presence of a threonine atposition 135 in chimps rescues the deleterious effect of themethionine at position 125, in a mechanism of intra-locus compensation.

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