VLX1570CAS号1431280-51-1
VLX1570CAS号1431280-51-1

VLX1570

¥514.90 ~¥8,960.90
100mg / 10mg / 25mg / 2mg / 50mg / 5mg
100mg
上海
阿拉丁
2025-04-25
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产品详情
中文名称:VLX1570中文别名:VLX1570
英文名称:VLX1570CAS:1431280-51-1
产品分类:合成有机化合物配体纯度:≥99%
产品编号品牌纯度规格库存价格
V413963阿拉丁≥99%100mg现货8,960.90 元
V413963阿拉丁≥99%10mg现货1,750.90 元
V413963阿拉丁≥99%25mg现货3,501.90 元
V413963阿拉丁≥99%2mg现货514.90 元
V413963阿拉丁≥99%50mg现货5,664.90 元
V413963阿拉丁≥99%5mg现货1,029.90 元
标准名称:VLX1570英文名称:VLX1570
CAS:1431280-51-1分子式:C23H17F2N3O6
分子量:469.394392728806颜色与性状:
密度:沸点:
熔点:水溶性:

中文名:VLX1570

英文名:VLX1570

纯度:Moligand™,≥99%

货号:V413963

Cas号:1431280-51-1

存储温度:-20°C储存

运输条件:超低温冰袋运输

产品介绍:

Information

VLX1570 VLX1570 is a competitive inhibitor of proteasome DUB activity, with an IC50 of ~10 μM in vitro.


Targets

DUB (Cell-free assay) ~10 μM


In vitro

VLX1570 is an analogue of b-AP15 that shows higher potency and improved solubility. VLX1570 preferentially inhibits proteasomal DUB activity while not inhibiting the activities of a panel of non-proteasomal DUBs. VLX1570 binds to and inhibits the activity of ubiquitin-specific protease-14 (USP14) with comparatively weaker inhibitory activity towards UCHL5 (ubiquitin-C-terminal hydrolase-5). Treatment of multiple myeloma cells with VLX1570 induces the accumulation of proteasome-bound high molecular weight polyubiquitin conjugates and an apoptotic response. VLX1570 induces the expression of the chaperone HSP70B′, the oxidative stress marker Hmox-1, and the ER stress marker XBP-1s. VLX1570 is retained in cells after removal of drug and that USP14 was engaged by drug 17\u2009hours after wash-out, as evidenced by thermal stabilization and persistent enzyme inhibition.


In vivo

VLX1570 is an inhibitor of proteasome DUB activity currently in clinical trials for relapsed multiple myeloma. Treatment with VLX1570 is found to lead to extended survival in xenograft models of multiple myeloma. The in vivo IC50 for inhibition of proteasome DUB activity and induction of apoptosis is <1\u2009μM, with multiple myeloma cells showing greater levels of sensitivity compared to other tumor types. The lower IC50 for activity in vivo is presumably due to rapid drug uptake and enrichment in cells.


Cell Research(from reference)

Cell lines:OPM-2\u2009MM cells

Concentrations:0.5 μM

Incubation Time:3 h


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