Date published: 2025-11-28

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Aut7 Activators

Aut7 Activators are a diverse collection of chemical compounds that, through their distinct mechanisms, enhance the autophagic process wherein Aut7 plays a critical enzymatic role. Phosphatidylinositol 3-phosphate (PI3P), by recruiting effector proteins to autophagic structures, directly facilitates the localization and activity of Aut7 in vesicle nucleation. Similarly, trehalose, by inducing protein aggregation, necessitates Aut7's conjugation activity for autophagosome formation, while rapamycin, by inhibAut7 Activators encompass a variety of chemical compounds that enhance the functional activity of Aut7 through their interaction with specific signaling pathways and biological processes essential to autophagy. Phosphatidylinositol 3-phosphate (PI3P), as a pivotal signaling lipid, recruits proteins that are critical for early autophagic structures, thereby facilitating the vesicle nucleation step that is heavily dependent on Aut7 activity. Trehalose, a disaccharide, promotes autophagy by triggering the aggregation of misfolded proteins targeted for degradation, a process that requires the conjugation activity of Aut7 for autophagosome formation. Rapamycin and Perifosine both function as autophagy inducers by inhibiting the mTOR pathway, leading to the activation of downstream processes where Aut7's E1-like enzyme activity is vital for expanding and closing the autophagosome. Lithium, Carbamazepine, and Metformin, through different routes, all converge to enhance autophagosome formation, with Lithium acting via inositol monophosphatase inhibition, Carbamazepine through modulating inositol and cAMP signaling, and Metformin activating AMPK, which subsequently inhibits mTOR signaling.

Aut7 activator landscape, Nicotinamide, by inhibiting SIRT1, leads to the deacetylation of proteins crucial for autophagosome maturation, a step wherein Aut7 is indispensable. Verapamil, a calcium channel blocker, indirectly induces autophagy by modulating intracellular calcium levels, thus facilitating Aut7's role in phagophore formation. Spautin-1, by inhibiting specific ubiquitin-specific peptidases, leads to an increase in PI3P levels, which is conducive to Aut7-mediated autophagosome formation. Spermidine and Resveratrol, each through unique mechanisms involving the modulation of protein acetylation states, promote autophagy, thereby enhancing the essential conjugation reactions mediated by Aut7. Spermidine achieves this by inhibiting histone acetyltransferases, while Resveratrol activates SIRT1, both leading to a hypoacetylated state that favors Aut7's function in the autophagic flux. Collectively, these Aut7 Activators demonstrate the intricate regulation of autophagy and the pivotal role of Aut7 within this essential cellular process.

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Items 1 to 10 of 11 total

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Product NameCAS #Catalog #QUANTITYPriceCitationsRATING

D-(+)-Trehalose Anhydrous

99-20-7sc-294151
sc-294151A
sc-294151B
1 g
25 g
100 g
$29.00
$164.00
$255.00
2
(0)

Trehalose is a disaccharide that promotes autophagy by inducing the aggregation of misfolded proteins, which are subsequently targeted for degradation. This process necessitates the conjugation activity of Aut7 to form the autophagosome.

Rapamycin

53123-88-9sc-3504
sc-3504A
sc-3504B
1 mg
5 mg
25 mg
$62.00
$155.00
$320.00
233
(4)

Rapamycin is a well-known activator of autophagy by inhibiting the mammalian target of rapamycin (mTOR) pathway, which in turn activates the ULK1 complex. This complex initiates the formation of the phagophore, where Aut7 is essential for the expansion and closure of the autophagosome.

Lithium

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

Lithium induces autophagy independently of the mTOR pathway by inhibiting inositol monophosphatase, leading to depletion of free inositol and a decrease in phosphatidylinositol (4,5)-bisphosphate levels. This inositol depletion promotes autophagosome formation, which requires the E1-like enzyme activity of Aut7.

Nicotinamide

98-92-0sc-208096
sc-208096A
sc-208096B
sc-208096C
100 g
250 g
1 kg
5 kg
$43.00
$65.00
$200.00
$815.00
6
(1)

Nicotinamide, a form of vitamin B3, inhibits the deacetylase activity of SIRT1, leading to the deacetylation of essential autophagy proteins. Deacetylated proteins are necessary for autophagosome maturation, which is mediated by Aut7.

Carbamazepine

298-46-4sc-202518
sc-202518A
1 g
5 g
$32.00
$70.00
5
(0)

Carbamazepine stimulates autophagy by modulating the inositol and cAMP signaling pathways. This modulation leads to enhanced autophagosome formation, where Aut7’s ubiquitin-like conjugation system is critical for autophagosome elongation.

Verapamil

52-53-9sc-507373
1 g
$367.00
(0)

Verapamil, a calcium channel blocker, indirectly induces autophagy by reducing intracellular calcium levels, which are known to inhibit autophagy. Lower calcium concentrations facilitate the phagophore formation process in which Aut7 is involved.

Spautin-1

1262888-28-7sc-507306
10 mg
$165.00
(0)

Spautin-1 promotes autophagy by inhibiting the ubiquitin-specific peptidase 10 (USP10) and USP13, leading to the degradation of Vps34 PI3 kinase complexes. The resulting increase in PI3P levels enhances Aut7's role in autophagosome formation.

Perifosine

157716-52-4sc-364571
sc-364571A
5 mg
10 mg
$184.00
$321.00
1
(2)

Perifosine, an alkylphospholipid, activates autophagy by inhibiting the Akt/mTOR signaling pathway. This inhibition triggers downstream autophagy processes that involve the lipidation activity of Aut7.

Metformin

657-24-9sc-507370
10 mg
$77.00
2
(0)

Metformin activates AMP-activated protein kinase (AMPK), which in turn inhibits mTOR signaling, leading to the induction of autophagy. Aut7 functions as an E1-like enzyme are vital for the expansion of the autophagic membrane in this context.

Spermidine

124-20-9sc-215900
sc-215900B
sc-215900A
1 g
25 g
5 g
$56.00
$595.00
$173.00
(2)

Spermidine promotes autophagy through the inhibition of histone acetyltransferases, favoring a hypoacetylated state of autophagy-related proteins. This promotes the autophagic process, where Aut7 is essential for the conjugation of ATG12 to ATG5 and the lipidation of ATG8-family proteins.