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- xy-C422Ra01
- 2025年08月21日
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- 详细信息
- 文献和实验
- 技术资料
- 保存条件:
-20℃
- 保质期:
12个月
- 英文名:
Recombinant Constitutive Androstane Receptor (CAR)
- 库存:
1000
- 供应商:
上海信裕
| Organism species | Rattus norvegicus (Rat) |
| Product No. | |
| Source | Prokaryotic expression |
| Host | E.coli |
| Purity | > 90% |
| UOM | 50ug |
| Predicted Molecular Mass | 31.8kDa |
| Concentration | n/a |
| Applications | SDS-PAGE; WB; ELISA; IP. |
| Endotoxin Level | <1.0EU per 1µg (determined by the LAL method) |
| Residues | Met1~Glu247 with two N-terminal Tags, His-tag and T7-tag |
| Formulation | Supplied as lyophilized form in 20mM Tris, 150mM NaCl, pH8.0, containing 1mM EDTA, 1mM DTT, 0.01% sarcosyl, 5% trehalose, and preservative. |
MTATLTLETM TSEEEYGPRN CVVCGDRATG YHFHALTCEG CKGFFRRTVS KTIGPICPFA GRCEVSKAQR RHCPACRLQK CLNVGMRKDM ILSAEALALR RARQARRRAQ KASLQLSQQQ KELIQTLLGA HTRHVGPMFD QFVQFRPPAY LFSHHRPFQP LAPVLPLLTH FADINTFMVQ QIIKFTKDLP LFRSLTMEDQ ISLLKGAAVE ILHISLNTTF CLQTQNFFCG PLCYKMEDAV HVGFQYE
Stability Test: The thermal stability is described by the loss rate of the target protein. The loss rate was determined by accelerated thermal degradation test, that is, incubate the protein at 37oC for 48h, and no obvious degradation and precipitation were observed. (Referring from China Biological Products Standard, which was calculated by the Arrhenius equation.) The loss of this protein is less than 5% within the expiration date under appropriate storage condition.
Protein bands: 10kDa, 14kDa, 18kDa, 22kDa, 26kDa, 33kDa, 44kDa and 70kDa.
Double intensity bands: The 26kDa, 18kDa, 10kDa bands are at double intensity to make location and size approximation of proteins of interest quick and easy.
Ready-to-use: No need to heat, dilute or add reducing agents before use.
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文献和实验「CAR-T 之父」Carl June 引领抗癌风向标!挑战
导读当前,嵌合抗原受体 (CAR)-T 细胞在白血病的治疗中已经取得了显著的进展,但是该疗法在大多数实体肿瘤中的疗效仍然受限。有学者认为,导致实体肿瘤疗效差的因素主要在于肿瘤微环境(TME)中免疫细胞的「捣乱」,这促使人们努力改善 CAR-T 细胞的内在功能,使其能够克服 TME 带来的抵抗,然而目前仍然没有突破性进展。损伤相关分子模式(Damage-associated molecular patterns, DAMPs)作为模式识别受体(Patter recognition
Science | 破除抑制性肿瘤微环境,改良 CAR-T 可靶向实体瘤
细胞上构建肿瘤特异合成性 Notch 受体(synNotch),可以在识别癌细胞后诱导产生 IL-2 促进 T 细胞活性,在胰腺肿瘤和黑色素瘤模型中可以有效增强 CAR-T 细胞或 TCR-T 细胞的肿瘤浸润,实验鼠体内的肿瘤清除能力以及其存活率均有显著提升,此类改良给 CAR / TCR-T 细胞在免疫抑制性实体瘤治疗领域带来新突破。 图:论文截图 目前 CAR-T 细胞治疗血液恶性肿瘤也仍面对四个主要挑战: 肿瘤异质性以及目的抗原丢失 免疫抑制性的肿瘤微环境 CAR-T 细胞耗竭 输注
嵌合抗原受体T细胞免疫疗法,CAR-T疗法。目前已在血液系统恶性肿瘤的治疗中取得了重大成功,但也存在严重的可能致命的副作用,例如细胞因子风暴CRS和神经毒性。同时,CAR-T疗法目前对实体瘤治疗效果非常有限,且肿瘤相关抗原在很多重要且关键的正常组织都有表达,这也增加了“On target off tumor”的毒性。 针对CAR-T疗法的局限性,研究人员采取了许多策略试图克服这些局限性,例如增强T细胞的扩增和降低T细胞的耗竭、敲除抑制基因、提高T细胞识别抗原的灵敏度。本期陈老湿
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