Scientists have found that a protein shown to function in the liver has a key role in human menstrual cycle and may also play a crucial role in pregnancy.
According to researchers at the University of Montreal in Canada, mice that were genetically engineered not to produce the liver receptor homolog-1 (Lrh-1) molecule were unable to create the uterine conditions necessary for establishing and sustaining pregnancy, resulting in the formation of defective placentas.
The researchers then showed that Lhr-1 was present in the human uterus and the essential processes related to the success of early gestation.
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"We worked with mice before looking at human tissues. I believe it premature to propose determination of Lrh-1 in uterine biopsies as a diagnostic tool, but we are working on determining the receptor's pattern of expression across the menstrual cycle," Murphy said.
The researchers also looked at whether hormone replacement therapy might restore normal uterine functions in the mice.
"Progesterone did not make a difference. Although hormone therapy allowed for the embryos to implant, we saw problems with the lining in the uterus, compromised formation of the placenta, foetal growth retardation and foetal death," Murphy said.
"However, there are new Lrh-1 agonists and antagonists, currently in clinical trials to treat hepatic consequences of type II diabetes, and thus therapeutic intervention might be possible," he said.
The study was published in journal Nature Medicine.