Blood and/or breast milk have been used to assess human exposure to various
environmental contaminants. Few studies have been available to compare
the concentrations in one matrix with those in another. The goals
of this study were to determine the current levels of polybrominated
diphenyl ethers (PBDEs) and polychlorinated biphenyls (PCBs) in Japanese
women, with analysis of the effects of lifestyle and dietary habits
on these levels, and to develop a quantitative structure–activity
relationship (QSAR) with which to predict the ratio of serum concentration
to breast milk concentration. We measured PBDEs and PCBs in 89 paired
samples of serum and breast milk collected in four regions
of Japan in 2005. The geometric means of the total concentrations of PBDE (13 congeners) in
milk and serum were 1.56 and 2.89 ng/g lipid, respectively, whereas
those of total PCBs (15 congeners) were 63.9 and 37.5 ng/g
lipid, respectively. The major determinant of total PBDE concentration
in serum and milk was the geographic area within Japan, whereas
nursing duration was the major determinant of PCB concentration. BDE-209 was
the most predominant PBDE congener in serum but not in milk. The
excretion of BDE 209 in milk was lower than that of BDE 47 and BDE 153. QSAR
analysis revealed that two parameters, calculated octanol/water
partition and number of hydrogen-bond acceptors, were significant
descriptors. During the first weeks of lactation, the predicted partitioning
of PBDE and PCB congeners from serum to milk agreed with the
observed values. However, the prediction became weaker after 10 weeks
of nursing.
Following the death of one twin, morbidity in the surviving twin can be produced by hypotensive ischemia of the brain due to hemorrhage through placental vascular anastomoses.
To determine the relationship between premature ovarian failure (POF) and skewed X-chromosome inactivation (XCI), karyotype, and XCI status in 43 patients with POF (group I) and 43 age-matched control women with regular menstrual cycles (group II) were evaluated. Evaluation of XCI status was based on the CAG triplet repeat polymorphism assay in the androgen receptor gene after sodium bisulfite treatment of DNA samples, and XCI patterns were classified as random (XCI < 70% skewing) or skewed (> or =70%). Furthermore, skewed XCI was classified under three different thresholds (> or =70, > or =80, or > or =90%). Karyotyping by G-banding and fluorescence in situ hybridization (FISH) on peripheral blood lymphocytes showed that one patient in group I had a deletion of Xq22, and another was 47,XXX. The frequency of low-level 45,X/46,XX mosaicism was nearly equal in both groups. In women without any X-chromosomal aberrations, the incidence of skewed XCI in group I was significantly higher than in group II on all threshold levels. Furthermore, extremely skewed XCI (> or =90%) was observed only in group I. These results indicate that POF may be caused by some underlying genetic disorders, which may induce skewed XCI.
In order to evaluate the relation between pericentric inversion of chromosome 9 (inv (9)) and clinical problems, the characteristics of inv (9) were investigated on the basis of chromosomal analyses of fetuses and infertile couples. The incidence of such inversion in fetuses with parents having an offspring who suffered from various clinical problems was significantly higher than the basic incidence obtained in fetuses karyotyped by reason of advanced maternal age. In the chromosomal examination of the parents whose fetuses were diagnosed as inv (9), it was revealed that either parent might be the carrier. Furthermore, in the inv (9) carrying fetuses, the number of females was significantly greater than that of males. Analysis of infertile couples revealed that the incidence of such inversion in males was significantly higher than the basic incidence mentioned above. Moreover, infertile couples with an inv(9) carrier showed a significantly higher incidence of intrauterine fetal death, compared with infertile couples with a translocation carrier or those in which the etiology was unknown. These results indicate that inv(9) may often cause clinical problems in offspring of the carrier and infertility with unknown mechanisms related to sex. pericentric inversion of chromosome 9 ; prenatal diagnosis ; infertility ; repeated abortion ; sexual difference Pericentric inversion is one type of chromosomal rearrangement, the detection of which has been greatly facilitated by the development of banding techniques. The site of such inversion of chromosome 9 (inv (9)) is now well known to be heterochromatin.In comparison with pericentric inversion of other chromosomes, pericentric inversion of chromosome 9, the incidence of which has been reported to be about 1% in the general population (Ferguson-Smith 1974;Buckton et al. 1976;Mueller and Klinger 1976), has been categorized as a minor chromosomal rearrangement which does not correlate with abnormal phenotypes
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