The chemical class denoted as SH-PTP2 Activators are a set of compounds orchestrated to intricately modulate and amplify the functional activity of Src homology 2 domain-containing protein tyrosine phosphatase 2 (SH-PTP2). Within this ensemble, Erlotinib and Dasatinib emerge as architects of sustained SH-PTP2 activation, disrupting negative feedback loops that might otherwise curtail its activity. Their mechanisms intricately navigate cellular signaling, ensuring the perpetuation of SH-PTP2's catalytic prowess. In a parallel modulatory vein, Calyculin A and PP2 navigate indirect routes, influencing SH-PTP2 by targeting protein phosphatases and Src kinases, respectively. These compounds engage in a nuanced interplay with the intricate network of cellular signaling, indirectly sculpting the landscape for heightened SH-PTP2 activity. ATRA, on the other hand, emerges as a regulator of SH-PTP2 expression. By elevating SH-PTP2 levels, ATRA orchestrates a cascade effect, amplifying the phosphatase's activity and subsequently impacting downstream cellular processes.
The interplay extends further to Forskolin and Wortmannin, which orchestrate their effects through the cAMP and PI3K pathways, respectively. These compounds, with precision akin to molecular conductors, indirectly bolster SH-PTP2 activation, highlighting the complexity of signaling cascades interwoven in the modulation of SH-PTP2. The ensemble reaches its zenith with Bisindolylmaleimide I and NSC 87877, which directly engage with SH-PTP2's phosphatase activity. These compounds act as direct facilitators, ensuring enhanced access to substrates for SH-PTP2, thereby directly influencing its catalytic function. Expanding the repertoire, Staurosporine and SB203580 broaden their scope, impacting broader cellular signaling pathways.
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