Date published: 2025-10-15

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PLAC9 Inhibitors

Chemical inhibitors of PLAC9 can achieve functional inhibition through various biochemical and cellular pathways. GW4869 targets the enzymatic activity of sphingomyelinase, which is pivotal in ceramide production, a lipid that plays a regulatory role in the function of PLAC9. By inhibiting sphingomyelinase, GW4869 can reduce ceramide levels, thus influencing the regulation of PLAC9. MAFP and U73122 act on different phospholipases; MAFP inhibits phospholipase A2, which is instrumental in generating lipid signaling molecules that can regulate PLAC9, while U73122 inhibits phospholipase C, which is involved in signal transduction pathways that can regulate the activity of PLAC9. PD98059 is a specific inhibitor of MEK, an upstream component of the MAPK/ERK pathway. By inhibiting MEK, PD98059 can lead to a decrease in the phosphorylation and activity of PLAC9. Similarly, LY294002 and Wortmannin are PI3K inhibitors that prevent signal propagation, potentially preventing the activation of PLAC9.

In addition to these, SB203580 acts as an inhibitor of p38 MAPK and can reduce the phosphorylation of proteins within the pathway that includes PLAC9, leading to its functional inhibition. SP600125, a JNK inhibitor, can lead to decreased activity of transcription factors that are part of the regulatory mechanism for PLAC9's function. Calcium signaling is also critical for PLAC9, and the chelator BAPTA can inhibit these calcium-dependent pathways, thus influencing PLAC9. Y-27632 inhibits ROCK, which may affect cytoskeletal organization and associated signaling processes involving PLAC9. ML7's inhibition of myosin light chain kinase can alter cytoskeletal dynamics, potentially inhibiting signaling pathways that would otherwise enable PLAC9 function. Finally, Genistein inhibits tyrosine kinases that are responsible for phosphorylation of proteins interacting with or regulating PLAC9, thus providing a multi-angled approach to the functional inhibition of this protein through disruption of its regulatory mechanisms.

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Items 1 to 10 of 11 total

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Product NameCAS #Catalog #QUANTITYPriceCitationsRATING

GW4869

6823-69-4sc-218578
sc-218578A
5 mg
25 mg
$199.00
$599.00
24
(3)

GW4869 inhibits the enzymatic activity of sphingomyelinase, which could reduce ceramide production, a molecule involved in the regulation of PLAC9.

MAFP

188404-10-6sc-203440
5 mg
$215.00
4
(1)

MAFP inhibits phospholipase A2, which is crucial for generating lipid signaling molecules that may regulate the activity of PLAC9.

PD 98059

167869-21-8sc-3532
sc-3532A
1 mg
5 mg
$39.00
$90.00
212
(2)

PD98059 inhibits MEK, which is upstream in the MAPK/ERK pathway, potentially leading to decreased phosphorylation and activity of PLAC9.

LY 294002

154447-36-6sc-201426
sc-201426A
5 mg
25 mg
$121.00
$392.00
148
(1)

LY294002 is a PI3K inhibitor, which would prevent the propagation of signals that could activate PLAC9.

Wortmannin

19545-26-7sc-3505
sc-3505A
sc-3505B
1 mg
5 mg
20 mg
$66.00
$219.00
$417.00
97
(3)

Wortmannin inhibits PI3K like LY294002, preventing downstream signaling that could influence PLAC9 activation.

SB 203580

152121-47-6sc-3533
sc-3533A
1 mg
5 mg
$88.00
$342.00
284
(5)

SB203580 inhibits p38 MAPK, which could reduce the phosphorylation of proteins in the pathway that includes PLAC9, leading to its functional inhibition.

SP600125

129-56-6sc-200635
sc-200635A
10 mg
50 mg
$40.00
$150.00
257
(3)

SP600125 inhibits JNK, which could lead to decreased activity of transcription factors that regulate PLAC9's function.

BAPTA, Free Acid

85233-19-8sc-201508
sc-201508A
100 mg
500 mg
$67.00
$262.00
10
(1)

BAPTA chelates calcium ions, potentially inhibiting calcium-dependent signaling pathways that regulate PLAC9.

Y-27632, free base

146986-50-7sc-3536
sc-3536A
5 mg
50 mg
$182.00
$693.00
88
(1)

Y-27632 inhibits ROCK, which may disrupt cytoskeletal organization and signaling pathways involving PLAC9.

ML-7 hydrochloride

110448-33-4sc-200557
sc-200557A
10 mg
50 mg
$89.00
$262.00
13
(1)

ML7 inhibits myosin light chain kinase, potentially altering cytoskeletal dynamics and associated signaling pathways that could inhibit PLAC9.