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br Fipronil resistance associated with A S and A
2022-04-21

Fipronil resistance associated with A2′S and A2′G mutations Fipronil is a second-generation NCA (Fig. 1), and A2′S and A2′G mutations provide a low level of cross-resistance to fipronil (Cole et al., 1995, Gao et al., 2007). As shown in Table 1, the A2′S H-Lys(Ac)-OH.HCl confers high resistance
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The optimum parameter sets were detected by the
2022-04-21

The optimum parameter sets were detected by the highest J-statistic for the training set and applied to the test set for evaluation. J-statistics obtained from the test set is reported at Table 2 along with respective parameters. We also applied QP, G4H and PQSF methods, in order to compare the pre
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br Introduction Regulation of transcription is a critical ev
2022-04-21

Introduction Regulation of transcription is a critical event of the embryonic development and epigenetic mechanisms such as histone modifications and DNA methylation appear important in mediating temporal changes, and differences among cells/tissues, of temporary stabilized transcriptomes (Mas et
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br Heme oxygenase inhibitors Historically the first class of
2022-04-20

Heme oxygenase-1 inhibitors Historically, the first class of competitive HO-1 inhibitors was represented by MPs, heme analogs in which the central iron Dehydrocostus Lactone mg of heme is exchanged by another element, such as zinc, cobalt, tin, or chromium. These molecules compete with heme for b
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Cdk2/Cyclin Inhibitory Peptide I mg br Conclusion br Disclos
2022-04-20

Conclusion Disclosure of interest Acknowledgement Introduction Vitamin B6 has long been recognized as a cofactor for many enzymes, especially those involved in amino Cdk2/Cyclin Inhibitory Peptide I mg metabolism. Apart from its role as coenzyme, recent studies are unveiling a new role
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Our synthetic approach to GPR antagonists
2022-04-20

Our synthetic approach to GPR55 antagonists was designed so that many different structures could be accessed to rapidly explore initial SAR, along with validating or modifying our current model (). The synthesis begins with the coupling of a carboxylic STF-62247 to 4-piperidone by first forming th
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Both GPR A and GPR are
2022-04-20

Both GPR109A and GPR81 are located on chromosome 12q24 [3] and mediate anti-lipolytic effects through coupling to Gi-type G proteins [17]. It is important to note that with the recent deorphanization of these receptors, there has been a recommendation to the International Union of Basic and Clinical
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Based on these findings we set out
2022-04-20

Based on these findings, we set out to identify GPR109A agonists capable of biasing the receptor's signaling towards the functional anti-lipolytic and presumed therapeutic response, and away from the flushing side-effect pathways. Indeed, using recombinantly expressed GPR109A, two classes of compoun
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Our study has some limitations
2022-04-20

Our study has some limitations. While our study provides data from a diverse multi-country setting, we did not have a sufficient sample size to investigate whether the relationship of micronutrients and fbpase with CD4 recovery differed by country. We relied on measurement of deficiencies based on m
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877877 The unique ability of R
2022-04-20

The unique ability of R.PabI to specifically excise 877877 from a palindromic sequence is based on a novel structural architecture that is distinct not only from other DNA glycosylases but also from other proteins [88]. In the absence of DNA, R.PabI forms a dimer with a central, highly twisted β-she
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By contrast pentameric glycine receptors GlyR in
2022-04-20

By contrast, pentameric glycine receptors (GlyR) in humans have four functional subunits, α1− α3 and β (Lynch, 2004) whereas the retina of other mammals have an additional α4 subunit (Harvey et al., 2000), and in humans the α4 subunit is considered a pseudogene as it lacks the 4th transmembrane doma
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Cinchonidine Na K ATPase adenosine triphosphate ATP and astr
2022-04-20

Na+/K+-ATPase, Cinchonidine and astrocytic glutamate transporters act together to maintain sodium and potassium gradients and the proper activities of EAAT1 and EAAT2 (Rose et al., 2009; Sheean et al., 2013); nevertheless, in present study, Na+/K+-ATPase activity was shown to be increased as from 24
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A number of experimental data declare
2022-04-20

A number of experimental data declare a tight interdependence between the pathological changes of glutamate transport in AZD-3463 australia and consequent alterations in glutamate transport and activity/expression of glutamate metabolizing enzymes in platelets (Aliprandi et al., 2005, Behari and Sh
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br Acknowledgments This work was supported
2022-04-20

Acknowledgments This work was supported by a grant CIHR-NSFC China-Canada Joint Health Research from the National Science Foundation of China (Grant Number 81061120525) and the Canadian Institutes for Health Research (Grant number CCI-109605). The authors thank two anonymous reviewers for helpful
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br Acknowledgments The authors would
2022-04-19

Acknowledgments The authors would like to thank principal investigator Edward John Pratt, MD (Lilly-NUS Centre for Clinical Pharmacology, Singapore) and study investigator Martha Hernandez-Illas MD (QPS-MRA) along with site staff, and trial participants and their families. We thank Zvonko Milicev
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