Workshops are an important part of the IFPA annual meeting. At IFPA Meeting 2010 diverse topics were
discussed in twelve themed workshops, six of which are summarized in this report. 1. The placental
pathology workshop focused on clinical correlates of placenta accreta/percreta. 2. Mechanisms of
regulation of trophoblast invasion and spiral artery remodeling were discussed in the trophoblast
invasion workshop. 3. The fetal sex and intrauterine stress workshop explored recent work on placental
sex differences and discussed them in the context of whether boys live dangerously in the womb.4. The
workshop on parasites addressed inflammatory responses as a sign of interaction between placental
tissue and parasites. 5. The decidua and embryonic/fetal loss workshop focused on key regulatory
mediators in the decidua, embryo and fetus and how alterations in expression may contribute to
different diseases and adverse conditions of pregnancy. 6. The trophoblast differentiation and syncytialisation
workshop addressed the regulation of villous cytotrophoblast differentiation and how variations
may lead to placental dysfunction and pregnancy complications
Workshops are an important part of the IFPA annual meeting as they allow for discussion of specialized topics. At IFPA meeting 2012 there were twelve themed workshops, four of which are summarized in this report. These workshops related to various aspects of placental biology: 1) epigenetics and imprinting in the placenta; 2) growth factors and villous trophoblast differentiation; 3) role of the placenta in regulating fetal exposure to xenobiotics during pregnancy; 4) infection and the placenta.
Estradiol and LY117018 differentially regulate the expression of CFTR and ENaC in ovariectomized mouse uterus. This finding suggests that uterine fluid accumulation can be controlled mainly by targeting the ENaC.
Aim: In order to investigate the current status of prenatal testing for genetic disorders, we conducted a multicenter retrospective questionnaire survey. Methods: The questionnaire was sent to 105 facilities with genetic counseling systems. The questionnaire consisted of two parts: (i) the number of prenatal tests conducted for genetic disorders from January 2010 to December 2012, whether the laboratory was combined with the counseling facility or separate, the sampling procedure method, the testing results, and the outcomes of the affected fetus in addition to treatment; and (ii) a survey of personal comments regarding prenatal testing for genetic disorders. Results: We received responses from 69 of the 105 facilities (65.7%), and genetic testing was performed at 26 of these facilities. Nucleic acid sequential testing was performed on 45 disorders and 252 cases during a three-year period. There were 67 cases of affected fetuses. Six cases continued pregnancy and were treated. The comment survey highlighted difficulties in locating a laboratory to assess prenatal samples, as well as inadequate counseling and preparation for genetic disorders. Conclusions: Our study revealed that a number of prenatal testing for genetic disorders are conducted in Japan; however, it is difficult for counselors to locate a laboratory capable of testing for specific genetic disorders. Inadequate counseling and healthcare providers' lack of knowledge is a current problem. A well-established system of prenatal testing for genetic disorders and the further education of general physicians is required.
These results indicate that erythrocyte deformability may worsen with the decrease in the estrogen level because of the onset of menopause, and also suggest that ET and EPT may allow it to recover.
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