Date published: 2025-10-11

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TIA1 Aktivatoren

Chemical activators of TIA1 play a pivotal role in the activation of stress granule formation and the cellular stress response. Anisomycin, by inhibiting peptidyl transferase activity in eukaryotic ribosomes, directly leads to the formation of stress granules, a process in which TIA1 is a key component. Similarly, Arsenite and Sodium Selenite induce oxidative stress, which is a trigger for the assembly of stress granules that incorporate TIA1 to maintain cellular integrity during stressful conditions. Hippuristanol and Pateamine A disrupt the function of eukaryotic initiation factor 4A (eIF4A), a crucial player in translation initiation, thereby causing translational repression. This repression is a signal for TIA1 to participate in the formation of stress granules to mitigate the effects of inhibited protein synthesis.

Additionally, Epigallocatechin Gallate, known for its oxidative properties, can lead to the activation of TIA1 through the induction of a stress response that culminates in stress granule assembly. Lithium Chloride takes a different approach by inhibiting glycogen synthase kinase 3 (GSK-3), a kinase involved in numerous signaling pathways, including those related to stress responses that can activate TIA1. Thapsigargin and Tunicamycin induce endoplasmic reticulum stress, which is known to activate TIA1 as part of the unfolded protein response, essential for restoring normal function of the cell. MG132's inhibition of the proteasome results in an accumulation of misfolded proteins, a condition that necessitates the involvement of TIA1 in stress granule dynamics to protect the cell from proteotoxic stress. Chloroquine disrupts lysosomal acidification, leading to a form of cellular stress that signals for TIA1 activation in stress granule assembly. Lastly, Sodium Arsenate induces oxidative stress, a condition under which TIA1 activation is critical for the cellular stress response, marking its essential role in the maintenance of cellular homeostasis under adverse conditions.

Siehe auch...

ProduktCAS #Katalog #MengePreisReferenzenBewertung

Anisomycin

22862-76-6sc-3524
sc-3524A
5 mg
50 mg
$97.00
$254.00
36
(2)

Anisomycin aktiviert TIA1, indem es die Peptidyltransferase-Aktivität in eukaryotischen Ribosomen hemmt, was zur Bildung von Stressgranulaten führt, an denen TIA1 beteiligt ist.

Sodium (meta)arsenite

7784-46-5sc-250986
sc-250986A
100 g
1 kg
$106.00
$765.00
3
(2)

Arsenit induziert die Bildung von Stresskörnchen durch die Förderung von oxidativem Stress, ein Zustand, der bekanntermaßen zur Aktivierung von TIA1 und zur Bildung von Stresskörnchen führt.

Sodium selenite

10102-18-8sc-253595
sc-253595B
sc-253595C
sc-253595A
5 g
500 g
1 kg
100 g
$48.00
$179.00
$310.00
$96.00
3
(2)

Natriumselenit löst bei bestimmten Konzentrationen oxidativen Stress aus, der zur Bildung von Stresskörnchen führen kann, an denen TIA1 aktiv beteiligt ist.

(−)-Epigallocatechin Gallate

989-51-5sc-200802
sc-200802A
sc-200802B
sc-200802C
sc-200802D
sc-200802E
10 mg
50 mg
100 mg
500 mg
1 g
10 g
$42.00
$72.00
$124.00
$238.00
$520.00
$1234.00
11
(1)

Epigallocatechingallat induziert nachweislich oxidativen Stress, der zur Aktivierung von TIA1 und zur Bildung von Stressgranula führen kann.

Lithium

7439-93-2sc-252954
50 g
$214.00
(0)

Lithiumchlorid hemmt die Glykogensynthase-Kinase 3 (GSK-3), was indirekt zur Aktivierung von TIA1 über Stressreaktionswege führen kann.

Thapsigargin

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

Thapsigargin löst Stress im endoplasmatischen Retikulum aus, was zur Aktivierung von Stressreaktionswegen führt, an denen TIA1 beteiligt ist.

Tunicamycin

11089-65-9sc-3506A
sc-3506
5 mg
10 mg
$169.00
$299.00
66
(3)

Tunicamycin induziert Stress im endoplasmatischen Retikulum, indem es die N-gebundene Glykosylierung hemmt, die TIA1 als Teil der "unfolded protein response" aktivieren kann.

MG-132 [Z-Leu- Leu-Leu-CHO]

133407-82-6sc-201270
sc-201270A
sc-201270B
5 mg
25 mg
100 mg
$56.00
$260.00
$980.00
163
(3)

MG132 hemmt das Proteasom, was zu zellulärem Stress und der potenziellen Aktivierung von TIA1 durch seine Rolle in der Stressgranulat-Dynamik führt.