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The TREAT NMD global registry has been focused on European countries and the Un

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 The TREAT NMD global registry has been focused on European countries and the Un Empty The TREAT NMD global registry has been focused on European countries and the Un

Сообщение  wangqian Ср Фев 19, 2014 1:23 pm

Therefore, inhibitors of tyrosine kinases can lead to the down regulation of CRKL and PXN, a fact that is being now taken into con sideration for the JNJ-7706621 Aurora Kinase inhibitor development of novel RA drugs, Indeed, a recent clinical trial shows promising results in the control of a specific tyrosine, based on clinical efficacy observed in mice where the small mol ecule R406 is used to target the spleen tyrosine kinase, which plays a crucial role in the signalling of acti vating Fc receptors and the B cell receptor, From our network analysis in human, we can suggest that the control of synovium degeneration illustrated above might be an additional reason to its efficacy, as Syk is directly linked to CRKL, Additionally, we can suggest an interpretation to one of the side effects of the therapy: neutropenia.<br><br> Due to the crucial role of CRKL in neutrophil adhesion, CRKL indirect down regulation via Syk for the LDN193189 1062368-24-4 control of synovium degeneration implies a reduc tion in neutrophils activity. The control of PXN was also pro posed as a novel therapeutic approach for RA, as PXN is up regulated in this disease via the triggering of the FAK family kinases signalling cascade, To our knowledge this path has not been pursued. In gen eral, the control of PXN can be achieved through a hier archy of interactions and therefore this represents a more subtle system that cannot be targeted by the golden bullet therapy approach. Interestingly insulin, via the tyrosine dephosphorylation of PXN, is able to control its activity in conjunction with Phos photyrosyne Phosphatase 1D, Phosphotyrosyne Phosphatase 1D is encoded by PTPN11 and controlled by echistatin, This is extremely signifi cant as a large amount of literature exists on insulin related to diabetes.<br><br> The overlap between RA and dia betes is an interesting one: in RA and diabetes, levels of inflammatory LY2157299 価格 markers, such as C reactive protein, TNF and interleukin 6 are typically increased and drugs used to treat RA by reducing in flammation through inhibition of TNF have shown promising results in the treatment of diabetes, Reducing inflammation with Remicade has also shown to improve insulin sensitivity in people who had inflam matory diseases and were insulin resistant, It there fore follows suite that some treatments for one inflammatory disease may be effective in the treatment of the other. In this direction, an on going clinical study is testing Pioglitazone on RA.<br><br> This trial is based on the rationale that recent studies have shown an increased prevalence of coronary artery atherosclerosis, metabolic syndrome and insulin resistance among people with RA. Furthermore, insulin resistance, which can lead to hyperinsulinemia too much insulin in the blood has been associated with RA disease activity and the severity of coronary artery atherosclerosis. These correlations corroborate the observation that inflammation and hyperinsulinemia somehow interact and facilitate one another. Interestingly, by joining all the above informa tion, thanks also to the systemic view that the map allowed us to have, we can recommend not to use Pioglitazone in conjunction with echistatin and therefore add this interaction as an unsuitable one.

wangqian

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