TY - JOUR
T1 - Rescue of progeria in trichothiodystrophy by homozygous lethal Xpd alleles
AU - Andressoo, Jaan Olle
AU - Jans, Judith
AU - De Wit, Jan
AU - Coin, Frederic
AU - Hoogstraten, Deborah
AU - Van De Ven, Marieke
AU - Toussaint, Wendy
AU - Huijmans, Jan
AU - Thio, H. Bing
AU - Van Leeuwen, Wibeke J.
AU - De Boer, Jan
AU - Egly, Jean Marc
AU - Hoeijmakers, Jan H.J.
AU - Van Der Horst, Gijsbertus T.J.
AU - Mitchell, James R.
PY - 2006
Y1 - 2006
N2 - Although compound heterozygosity, or the presence of two different mutant alleles of the same gene, is common in human recessive disease, its potential to impact disease outcome has not been well documented. This is most likely because of the inherent difficulty in distinguishing specific biallelic effects from differences in environment or genetic background. We addressed the potential of different recessive alleles to contribute to the enigmatic pleiotropy associated with XPD recessive disorders in compound heterozygous mouse models. Alterations in this essential helicase, with functions in both DNA repair and basal transcription, result in diverse pathologies ranging from elevated UV sensitivity and cancer predisposition to accelerated segmental progeria. We report a variety of biallelic effects on organismal phenotype attributable to combinations of recessive Xpd alleles, including the following: (i) the ability of homozygous lethal Xpd alleles to ameliorate a variety of disease symptoms when their essential basal transcription function is supplied by a different disease-causing allele, (ii) differential developmental and tissue-specific functions of distinct Xpd allele products, and (iii) interallelic complementation, a phenomenon rarely reported at clinically relevant loci in mammals. Our data suggest a re-evaluation of the contribution of "null" alleles to XPD disorders and highlight the potential of combinations of recessive alleles to affect both normal and pathological phenotypic plasticity in mammals.
AB - Although compound heterozygosity, or the presence of two different mutant alleles of the same gene, is common in human recessive disease, its potential to impact disease outcome has not been well documented. This is most likely because of the inherent difficulty in distinguishing specific biallelic effects from differences in environment or genetic background. We addressed the potential of different recessive alleles to contribute to the enigmatic pleiotropy associated with XPD recessive disorders in compound heterozygous mouse models. Alterations in this essential helicase, with functions in both DNA repair and basal transcription, result in diverse pathologies ranging from elevated UV sensitivity and cancer predisposition to accelerated segmental progeria. We report a variety of biallelic effects on organismal phenotype attributable to combinations of recessive Xpd alleles, including the following: (i) the ability of homozygous lethal Xpd alleles to ameliorate a variety of disease symptoms when their essential basal transcription function is supplied by a different disease-causing allele, (ii) differential developmental and tissue-specific functions of distinct Xpd allele products, and (iii) interallelic complementation, a phenomenon rarely reported at clinically relevant loci in mammals. Our data suggest a re-evaluation of the contribution of "null" alleles to XPD disorders and highlight the potential of combinations of recessive alleles to affect both normal and pathological phenotypic plasticity in mammals.
UR - http://www.scopus.com/inward/record.url?scp=33750247815&partnerID=8YFLogxK
U2 - 10.1371/journal.pbio.0040322
DO - 10.1371/journal.pbio.0040322
M3 - Article
C2 - 17020410
AN - SCOPUS:33750247815
SN - 1544-9173
VL - 4
SP - 1821
EP - 1830
JO - PLoS Biology
JF - PLoS Biology
IS - 10
ER -