A Short Form of the PRL Receptor is Able to Rescue Mammopoiesis in Heterozygous PRL Receptor Mice

doi:10.1210/me.2002-0181

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A Short Form of the PRL Receptor is Able to Rescue Mammopoiesis in Heterozygous PRL Receptor Mice

NADINE BINART¹^*, PRUNE IMBERT-BOLLORÉ¹, NATHALIE BARAN¹, CÉLINE VIGLIETTA¹, and PAUL A. KELLY¹

¹ Molecular Endocrinology, INSERM Unit 344, Faculté de Médecine Necker-Enfants Malades Paris, France (N. B., P. I. B., N. B., P. A. K.), Unité de Différenciation Cellulaire, INRA, Jouy en Josas, France (C. V.)

^* To whom correspondence should be addressed. E-mail: binart{at}necker.fr.

The heterozygous PRL receptor (PRLR +/-) mouse fails to developa fully functional mammary gland at the end of the first pregnancyand shows markedly impaired lobuloalveolar development and milksecretion in young females. The PRL receptor is expressed ubiquitously,with various proportions of long and short isoforms in differenttissues. Conflicting data have appeared on the putative roleof the receptor short forms with both agonist and antagonisticactions proposed. To assess whether the mouse PR-1 short isoformof the PRL receptor is potentially able to transduce a signal,we overexpressed it in heterozygous mice and investigated itseffect on the rescue of mammary development. PRLR+/- mice werenot able to develop a functional mammary gland, but restorationof mammary alveolar development and an increase in the expressionsof casein and WAP genes were observed in transgenic PRLR+/-mice expressing the short form of the PRLR, leading to a completerescue of mammary gland development and function in young females.These results demonstrate that PR-1 the short form of the PRLRcan improve mammary development in PRLR+/- mice compensatingthe haploinsufficiency of the receptor long form, the effectprobably being due to accelerated proliferation and an activationof the PRLR signaling cascade, resulting in activation of targetgenes involved in mammary development and milk synthesis.

Key words: PRL • mammary gland • receptor isoform

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