CHC1-L Inhibitors
Chemical inhibitors of CHC1-L target various signaling pathways and molecular processes to impede its function. Staurosporine, a potent kinase inhibitor, can disrupt the phosphorylation events essential for CHC1-L's activity, as many proteins require specific phosphorylation patterns to function correctly. Wortmannin and LY294002 both act upon phosphoinositide 3-kinases (PI3K), with the former being a steroidal metabolite and the latter a specific chemical inhibitor. Their inhibition of PI3K leads to a cascade effect, disrupting downstream pathways crucial for CHC1-L's role in cellular processes. Rapamycin directly inhibits mTOR, another key kinase in the regulation of protein synthesis, which can exert a downstream effect on the activity of CHC1-L due to its reliance on protein synthesis machinery and associated signaling networks.
Moreover, U0126 and PD98059, both MEK inhibitors, can impede the MAPK/ERK pathway, which is often essential for the regulation of proteins like CHC1-L. Similarly, SB203580 and SP600125, targeting p38 MAP kinase and c-JUN N-terminal kinase (JNK) respectively, can inhibit signaling paths that CHC1-L might utilize for its regulation. LFM-A13's selective inhibition of Bruton's tyrosine kinase and PP2's inhibition of Src family kinases can also lead to reduced CHC1-L activity due to the disruption of signaling networks. Finally, dasatinib and AZD0530, both tyrosine kinase inhibitors, can impede multiple kinases that CHC1-L may depend on for its functional state, thereby inhibiting the protein's activity through a broad interference with tyrosine kinase-dependent signaling.
SEE ALSO...
Items 1 to 10 of 12 total
Display:
| Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
|---|---|---|---|---|---|---|
Staurosporine | 62996-74-1 | sc-3510 sc-3510A sc-3510B | 100 µg 1 mg 5 mg | $82.00 $153.00 $396.00 | 113 | |
This alkaloid inhibits protein kinases, which can reduce the activity of CHC1-L by inhibiting phosphorylation events that are necessary for its function. | ||||||
Wortmannin | 19545-26-7 | sc-3505 sc-3505A sc-3505B | 1 mg 5 mg 20 mg | $67.00 $223.00 $425.00 | 97 | |
A steroidal metabolite that specifically inhibits phosphoinositide 3-kinases, which could lead to the inhibition of downstream pathways necessary for CHC1-L activity. | ||||||
LY 294002 | 154447-36-6 | sc-201426 sc-201426A | 5 mg 25 mg | $123.00 $400.00 | 148 | |
A chemical inhibitor of PI3K, LY294002 can inhibit the kinase activity, potentially disrupting signaling pathways that are crucial for CHC1-L function. | ||||||
Rapamycin | 53123-88-9 | sc-3504 sc-3504A sc-3504B | 1 mg 5 mg 25 mg | $63.00 $158.00 $326.00 | 233 | |
By inhibiting mTOR, rapamycin can disrupt signaling required for protein synthesis and other cellular processes related to CHC1-L function. | ||||||
U-0126 | 109511-58-2 | sc-222395 sc-222395A | 1 mg 5 mg | $64.00 $246.00 | 136 | |
As an inhibitor of MEK1/2, U0126 can inhibit the MAPK/ERK pathway, which could lead to a decrease in CHC1-L activity that relies on this signaling for its function. | ||||||
SB 203580 | 152121-47-6 | sc-3533 sc-3533A | 1 mg 5 mg | $90.00 $349.00 | 284 | |
This compound inhibits p38 MAP kinase, potentially inhibiting pathways that regulate CHC1-L function. | ||||||
SP600125 | 129-56-6 | sc-200635 sc-200635A | 10 mg 50 mg | $40.00 $150.00 | 257 | |
An inhibitor of c-JUN N-terminal kinase (JNK), which could block signaling pathways that contribute to CHC1-L activity. | ||||||
PD 98059 | 167869-21-8 | sc-3532 sc-3532A | 1 mg 5 mg | $40.00 $92.00 | 212 | |
A MEK inhibitor that could prevent the activation of the MAPK/ERK pathway, thereby potentially inhibiting CHC1-L function. | ||||||
LFM-A13 | 62004-35-7 | sc-203623 sc-203623A | 10 mg 50 mg | $119.00 $670.00 | ||
A selective inhibitor of Bruton's tyrosine kinase which could disrupt signaling pathways involving CHC1-L, leading to its functional inhibition. | ||||||
PP 2 | 172889-27-9 | sc-202769 sc-202769A | 1 mg 5 mg | $94.00 $227.00 | 30 | |
This Src family kinase inhibitor can disrupt multiple signaling pathways, potentially leading to the inhibition of CHC1-L that relies on Src signaling. | ||||||