Date published: 2025-10-15

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PSR Activators

In the realm of cellular homeostasis, the phosphatidylserine receptor (PSR) plays a crucial role in identifying and facilitating the clearance of apoptotic cells. The activation of PSR is inherently linked to the presence of apoptotic cells; thus, compounds that induce apoptosis indirectly augment the number of targets for PSR, leading to its theoretical activation. Chemicals like Sanguinarine and Piperlongumine increase intracellular reactive oxygen species, triggering cell death pathways and enhancing PSR-mediated phagocytosis by increasing the 'eat-me' signal through phosphatidylserine exposure. Similarly, Arsenic trioxide and Withaferin A can promote apoptosis in certain cell lines, which could lead to an upsurge in PSR activity due to a higher availability of apoptotic cells.

Betulinic acid, Ursolic acid, and Capsaicin are additional examples that induce apoptosis through various intracellular mechanisms, including the mitochondrial pathway and DNA damage, leading to PSR activation. Paclitaxel, through its action on microtubules, and Thapsigargin, via calcium dysregulation, also result in apoptosis, subsequently increasing the substrates for PSR engagement. Camptothecin's inhibition of DNA topoisomerase I, Curcumin's multi-targeted apoptotic induction, and Resveratrol's pro-apoptotic effects in specific cell lines, all contribute to the heightened activation of PSR. These compounds, by amplifying the apoptotic process, could serve as indirect activators of PSR, enhancing its critical function in maintaining cellular equilibrium. The exploration of such indirect activators is predicated on the intricate balance of cell death and clearance, where PSR serves as a sentinel for phagocytic signaling.

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Items 1 to 10 of 11 total

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Product NameCAS #Catalog #QUANTITYPriceCitationsRATING

Arsenic(III) oxide

1327-53-3sc-210837
sc-210837A
250 g
1 kg
$87.00
$224.00
(0)

Promotes apoptosis in certain types of cells, which could indirectly increase the activity of PSR by presenting more 'eat-me' signals.

Betulinic Acid

472-15-1sc-200132
sc-200132A
25 mg
100 mg
$115.00
$337.00
3
(1)

A pentacyclic triterpenoid that induces apoptosis through the mitochondrial pathway, potentially enhancing PSR-mediated phagocytosis.

Piperlongumine

20069-09-4sc-364128
10 mg
$107.00
(1)

Increases ROS levels leading to apoptosis, potentially raising the number of apoptotic cells for PSR to recognize.

Withaferin A

5119-48-2sc-200381
sc-200381A
sc-200381B
sc-200381C
1 mg
10 mg
100 mg
1 g
$127.00
$572.00
$4090.00
$20104.00
20
(1)

A steroidal lactone that induces apoptosis by generating ROS and modulating apoptosis-related proteins, which may increase PSR activity.

Ursolic Acid

77-52-1sc-200383
sc-200383A
50 mg
250 mg
$55.00
$176.00
8
(1)

Induces apoptosis and inhibits proliferation, which could indirectly lead to increased PSR activity.

Capsaicin

404-86-4sc-3577
sc-3577C
sc-3577D
sc-3577A
50 mg
250 mg
500 mg
1 g
$94.00
$173.00
$255.00
$423.00
26
(1)

Can induce apoptosis in various cell lines, potentially leading to increased activity of PSR.

Taxol

33069-62-4sc-201439D
sc-201439
sc-201439A
sc-201439E
sc-201439B
sc-201439C
1 mg
5 mg
25 mg
100 mg
250 mg
1 g
$40.00
$73.00
$217.00
$242.00
$724.00
$1196.00
39
(2)

Stabilizes microtubules and can induce apoptosis, which might enhance the externalization of phosphatidylserine and PSR activation.

Thapsigargin

67526-95-8sc-24017
sc-24017A
1 mg
5 mg
$94.00
$349.00
114
(2)

A SERCA pump inhibitor that causes calcium dysregulation and apoptosis, potentially leading to increased PSR activity.

Camptothecin

7689-03-4sc-200871
sc-200871A
sc-200871B
50 mg
250 mg
100 mg
$57.00
$182.00
$92.00
21
(2)

Inhibits DNA topoisomerase I, leading to DNA damage and apoptosis, indirectly affecting PSR activity.

Curcumin

458-37-7sc-200509
sc-200509A
sc-200509B
sc-200509C
sc-200509D
sc-200509F
sc-200509E
1 g
5 g
25 g
100 g
250 g
1 kg
2.5 kg
$36.00
$68.00
$107.00
$214.00
$234.00
$862.00
$1968.00
47
(1)

Has multiple cellular targets and can induce apoptosis in a variety of cell types, potentially increasing PSR-mediated phagocytosis.