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排序方式: 共有486条查询结果,搜索用时 0 毫秒
91.
Aaron W. Bradshaw Riccardo Autorino Giuseppe Simone Bo Yang Robert G. Uzzo Francesco Porpiglia Umberto Capitanio James Porter Riccardo Bertolo Andrea Minervini Clayton Lau Kenneth Jacobsohn Akbar Ashrafi Daniel Eun Alexandre Mottrie Wesley M. White Luigi Schips Benjamin J. Challacombe Ottavio De Cobelli Carmen M. Mir Alessandro Veccia Alessandro Larcher Alexander Kutikov Monish Aron Prokar Dasgupta Francesco Montorsi Inderbir S. Gill Chandru P. Sundaram Jihad Kaouk Ithaar H. Derweesh 《BJU international》2020,126(1):114-123
92.
We investigated whether cigarette smoking, measured by follicular fluid
concentrations of cotinine (a major metabolite of nicotine), affects the
maturity of oocytes from women undergoing in-vitro fertilization (IVF) and
embryo transfer. In 234 women, follicular fluid samples were assessed for
cotinine and their 2020 oocytes were assessed for maturity stage. Data on
individual proportions of oocytes which were mature (OM) and were
fertilized (OF) were analysed by regression in relation to age and
follicular fluid cotinine. OF gave an independent assessment of oocyte
maturity. Both age and follicular fluid cotinine entered the OM and OF
regressions and were significant. The age-adjusted regression coefficients
for log cotinine were positive; greater cotinine concentrations usually
accompanied greater OM and OF. The cotinine effect on OM was positive in
younger women, but it became negative (decreased OM with increasing
cotinine concentrations) in older women (> or = 40 years). We further
found in older women an average reduction of approximately 50% in the
number of mature oocytes; this reduced number was lower than the number of
embryos usually transferred. Smoking can reduce the number of mature
oocytes even further, therefore risking a negative IVF-embryo transfer
outcome. This may be the reason why the negative effects of smoking become
clinically detectable in older women.
相似文献
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Eduard Roussel Giovanni Tasso Riccardo Campi Maximilian C. Kriegmair Önder Kara Tobias Klatte Umberto Capitanio Riccardo Bertolo Alexandre Ingels Selcuk Erdem Loïc Baekelandt Maria C. Mir Idir Ouzaid Nicola Pavan Benoit Beuselinck Mauro Gacci Andrea Minervini Alessandro Volpe Maarten Albersen 《European urology》2021,79(1):133-140
96.
97.
To quantitatively map and compare patterns of regional cardiac metabolism with greater spatial resolution than is possible with positron emission tomography (PET), the authors developed autoradiographic techniques for use with combinations of radiolabeled fluorodeoxyglucose (FDG), glucose (GLU), and acetate (ACE) and applied the techniques to normal rats. Kinetic models were developed to compare GLU-based oxidative glucose metabolism with FDG-based total glucose metabolism (oxidative plus anaerobic) and to compare ACE-based overall oxidative metabolism with FDG-based total glucose metabolism. GLU-based metabolism generally paralleled FDG-based metabolism, but divergence occurred in certain structures such as the papillary muscles, where FDG-based metabolism was much greater. ACE-based metabolism also generally paralleled FDG-based metabolism, but again, the papillary muscles had relatively greater FDG-based metabolism. These discrepancies between FDG-based metabolism and GLU- or ACE-based metabolism suggest the presence of high levels of anaerobic glycolysis. Thus, the study indicates that anaerobic glycolysis, in addition to occurring in ischemic or "stunned" myocardium (as has been shown in recent PET studies), occurs normally in specific cardiac regions, despite the presence of abundant oxygen. 相似文献
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100.
Cloning and characterization of DXS6673E, a candidate gene for X-linked mental retardation in Xq13.1 总被引:3,自引:0,他引:3
van der Maarel SM; Scholten IH; Huber I; Philippe C; Suijkerbuijk RF; Gilgenkrantz S; Kere J; Cremers FP; Ropers HH 《Human molecular genetics》1996,5(7):887-897
In several families with non-specific X-linked mental retardation (XLMR)
linkage analyses have assigned the underlying gene defect to the
pericentromeric region of the X chromosome, but none of these genes have
been isolated so far. Here, we report on the cloning and characterization
of a novel gene, DXS6673E, that maps to Xq13.1, is subject to
X-inactivation and is disrupted in the 5' untranslated region by a balanced
X;13 translocation in a mentally retarded female. The DXS6673E gene is
highly conserved among vertebrates and its expression is most abundant in
brain. It encodes a hydrophilic protein of 1358 amino acids (aa) that does
not show sequence homology to other known proteins. A segment of this
protein consisting of neutral and hydrophobic aa with a proline residue in
every second position may represent a transmembrane domain. Almost complete
sequence identity was found between the 3' end of the DXS6673E gene and two
expressed sequence tags (ESTs) and between the 5' end of the DXS6673E gene
and a third EST. Moreover, weaker sequence similarity was observed between
coding regions and two other ESTs.
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