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武汉纽拜尔医药科技有限公司(NEWBIO PHARM-TECH)成立于2015年,位于武汉国家生物产业基地-光谷生物城,是一家专业从事新药研发、生产、销售的充满活力和高效率的药物研发团队。        新药研究技术水平是企业核心竞争力。纽拜尔新药主要研究方向有:新药开发研究(工艺、质量标准等)、化学合成及化学药品新药的开发。在化药方面,我们积极寻找新的项目,开发新的合成路线,在原有的技术上减少反应步骤及反应条件,减少合成项目的投入并积极引进国外品种。          纽拜尔新药拥有强大的研发团队30余人,其中武汉大学、华中科技大学博士5人、硕士10人。另外特聘知名专家教授3人指导科研生产。依托光谷生物城的集群资源,公司拥有先进的生产工艺、齐全的检测手段,本着“专注新药研发、延续人类健康”的发展理念,奉行“低价高纯、诚信经营”的企业服务宗旨,可以高效快捷地为客户提供新药技术研发、技术转让、抗肿瘤新药的合成、化学与生物领域的科研服务、新产品开发到产品上市全过程的工艺研发、产品注册和生产服务。

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产品名称:卡博替尼苹果酸盐

产品别名:Cabozantinib malate (XL184)

CAS.NO:1140909-48-3

分子式:C28H24FN3O5.C4H6O5

分子量:635.59

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Cabozantinib malate (XL184)是Cabozantinib的苹果酸盐,是有效的VEGFR2抑制剂,IC50为0.035 nM,也抑制c-Met, Ret, Kit, Flt-1/3/4, Tie2和AXL,无细胞试验中IC50分别为1.3 nM, 4 nM, 4.6 nM, 12 nM/11.3 nM/6 nM, 14.3 nM和7 nM。

靶点:VEGFR2/KDR [1] c-Met [1] Kit [1] VEGFR3/FLT4 [1] Axl [1]

体外研究:Cabozantinib has weak inhibitory activity against RON and PDGFRβ with IC50 of 124 nM and 234 nM, respectivey, and has low activity against FGFR1 with IC50 of 5.294 μM. [1] Cabozantinib at low concentration (0.1-0.5 μM) is sufficient to induce marked inhibition of constitutive and inducible Met phosphorylation and its resultant downstream signaling in MPNST cells, and inhibit HGF-induced MPNST cell migration and invasion. Cabozantinib also induces marked inhibition of Met and VEGFR2 phosphorylation in cytokine-stimulated human umbilical vein endothelial cells (HUVECs). Although Cabozantinib has no significant effect on MPNST cell growth at 0.1 μM, Cabozantinib at 5-10 μM significantly inhibits the MPNST cell growth. [2]

体内研究:Cabozantinib treatment at 30 mg/kg in RIP-Tag2 mice with spontaneous pancreatic islet tumors disrupts 83% of the tumor vasculature, reduces pericytes and empty basement membrane sleeves, causes widespread intratumoral hypoxia and extensive tumor cell apoptosis, and slows regrowth of the tumor vasculature after drug withdrawal, more significantly compared with XL999 that blocks VEGFR but not c-Met, leading to only 43% reduction in vascularity, suggesting that concurrent inhibition of VEGFR and other functionally relevant receptor tyrosine kinases (RTK) amplifies angiogenesis inhibition. Cabozantinib also decreases invasiveness of primary tumors and reduces metastasis. [1] Cabozantinib at 30 mg/kg/day significantly abrogates human MPNST xenografts growth and metastasis in SCID mice. [2] Administration of Cabozantinib induces dose-dependent inhibition of tumor growth in breast, lung, and glioma tumor models, in association with decreased tumor and endothelial cell proliferation as well as increased apoptosis. A single oral dose of Cabozantinib is sufficient to induce sustained tumor growth inhibition in MDA-MB-231 tumor-bearing mice and C6 tumor-bearing rats at 100 mg/kg and 10 mg/kg, respectively. [3]

特征:


询价

产品名称:阿西替尼

产品别名:Axitinib

CAS.NO:319460-85-0

分子式:C22H18N4OS

分子量:386.47

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Axitinib是一种多靶点抑制剂,作用于 VEGFR1,VEGFR2,VEGFR3,PDGFRβ和c-Kit,在猪主动脉内皮细胞中IC50分别为0.1 nM,0.2 nM,0.1-0.3 nM,1.6 nM和1.7 nM。

靶点:VEGFR1/FLT1 [1] VEGFR2/Flk1 [1] VEGFR2/KDR [1] VEGFR3 [1] PDGFRβ [1]

体外研究:Axitinib是受体激酶抑制剂,作用于VEGFR-1, VEGFR-2,VEGFR-3, PDGFR-β和c-KIT时IC50分别为0.1 , 0.2, 0.1-0.3, 1.6 和1.7 nM 。[1]Axitinib可以阻断VEGFR的自磷酸化作用,VEGF调节的内皮细胞活力,微管形成,及下游信号。Axitinib抑制多种细胞系的增殖,如作用于IGR-N91, IGR-NB8, SH-SY5Y ,无VEGF刺激的HUVEC时IC50分别为>1000 nM, 849 nM, 274 nM和573 nM。[2]

体内研究:Axitinib抑制常位移植模型,如M24met (黑色素瘤), HCT-116 (结肠直肠癌), 和SN12C (肾细胞癌)。[1]活体研究显示,按动物体重,每千克口服处理30mg Axitinib,与没有Axitinib处理的对照组相比,实验组推迟肿瘤生长达到11.4天;且用于IGR-N91侧腹移植瘤时,与对照组(密度为49)相比实验组(密度降为21)降低血管密度。[2]Axitinib在多种肿瘤包括肾细胞癌,甲状腺癌,非小细胞肺癌,黑色素瘤中显示出单一药效活性。

询价

产品名称:阿法替尼双马来酸盐

产品别名:Afatinib (BIBW2992) Dimaleate

CAS.NO:850140-73-7

分子式:C24H25ClFN5O3.2C4H4O4

分子量:717.18

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Afatinib (BIBW2992) Dimaleate 不可逆地抑制 EGFR/HER2,包括 EGFR(wt),EGFR(L858R),EGFR(L858R/T790M) 和 HER2,IC50 分别为0.5 nM,0.4 nM,10 nM 和 14 nM;活性比对Gefitinib抵抗型L858R-T790M EGFR突变体高100倍。

靶点:EGFR (L858R);EGFR (wt);EGFR (L858R/T790M);HER2 

体外研究:在表达野生型(H1666)或L858R/T790M (NCI-H1975) EGFR的肺癌细胞系中,Afatinib比erlotinib、gefitinib和lapatinib能够更有效的抑制细胞生长。Afatinib同样对表达HER2 776insV (NCI-H1781) 或EGFR E746_A750del (HCC827)的NSCLC细胞系有效,但对表达野生型EGFR 和HER2的A549细胞无效。[1] Afatinib可增强topotecan和mitoxantrone对SP细胞的细胞毒性,并增强topotecan和mitoxantrone对SP细胞的诱导凋亡作用。[1]

体内研究:在MDA-MB-453移植瘤模型中,Afatinib(20 mg/kg,口服给药)可显著诱导肿瘤衰退,累积治疗/对照肿瘤体积比(T/C比)为2%,并下调EGFR和AKT磷酸化水平。[1] 在A7、A431、FaDu、UT-SCC-14和UT-SCC-15移植瘤模型中,Afatinib(30 mg/kg,口服给药)可显著延长肿瘤生长时间。[3] 在HER2扩增移植瘤模型中,Afatinib(30 mg/kg,口服给药)可显著抑制肿瘤生长,并显著延长生存期。[4] 在HER2阳性胃癌NCI-N87移植瘤模型中,Afatinib(25 mg/kg)口服给药4天可显著减小肿瘤体积,给药21天几乎完全治愈肿瘤。[5]

特征:


询价

最新供应

更多

产品名称:阿西替尼

产品别名:Axitinib

CAS.NO:319460-85-0

分子式:C22H18N4OS

分子量:386.47

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Axitinib是一种多靶点抑制剂,作用于 VEGFR1,VEGFR2,VEGFR3,PDGFRβ和c-Kit,在猪主动脉内皮细胞中IC50分别为0.1 nM,0.2 nM,0.1-0.3 nM,1.6 nM和1.7 nM。

靶点:VEGFR1/FLT1 [1] VEGFR2/Flk1 [1] VEGFR2/KDR [1] VEGFR3 [1] PDGFRβ [1]

体外研究:Axitinib是受体激酶抑制剂,作用于VEGFR-1, VEGFR-2,VEGFR-3, PDGFR-β和c-KIT时IC50分别为0.1 , 0.2, 0.1-0.3, 1.6 和1.7 nM 。[1]Axitinib可以阻断VEGFR的自磷酸化作用,VEGF调节的内皮细胞活力,微管形成,及下游信号。Axitinib抑制多种细胞系的增殖,如作用于IGR-N91, IGR-NB8, SH-SY5Y ,无VEGF刺激的HUVEC时IC50分别为>1000 nM, 849 nM, 274 nM和573 nM。[2]

体内研究:Axitinib抑制常位移植模型,如M24met (黑色素瘤), HCT-116 (结肠直肠癌), 和SN12C (肾细胞癌)。[1]活体研究显示,按动物体重,每千克口服处理30mg Axitinib,与没有Axitinib处理的对照组相比,实验组推迟肿瘤生长达到11.4天;且用于IGR-N91侧腹移植瘤时,与对照组(密度为49)相比实验组(密度降为21)降低血管密度。[2]Axitinib在多种肿瘤包括肾细胞癌,甲状腺癌,非小细胞肺癌,黑色素瘤中显示出单一药效活性。

产品名称:阿法替尼双马来酸盐

产品别名:Afatinib (BIBW2992) Dimaleate

CAS.NO:850140-73-7

分子式:C24H25ClFN5O3.2C4H4O4

分子量:717.18

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Afatinib (BIBW2992) Dimaleate 不可逆地抑制 EGFR/HER2,包括 EGFR(wt),EGFR(L858R),EGFR(L858R/T790M) 和 HER2,IC50 分别为0.5 nM,0.4 nM,10 nM 和 14 nM;活性比对Gefitinib抵抗型L858R-T790M EGFR突变体高100倍。

靶点:EGFR (L858R);EGFR (wt);EGFR (L858R/T790M);HER2 

体外研究:在表达野生型(H1666)或L858R/T790M (NCI-H1975) EGFR的肺癌细胞系中,Afatinib比erlotinib、gefitinib和lapatinib能够更有效的抑制细胞生长。Afatinib同样对表达HER2 776insV (NCI-H1781) 或EGFR E746_A750del (HCC827)的NSCLC细胞系有效,但对表达野生型EGFR 和HER2的A549细胞无效。[1] Afatinib可增强topotecan和mitoxantrone对SP细胞的细胞毒性,并增强topotecan和mitoxantrone对SP细胞的诱导凋亡作用。[1]

体内研究:在MDA-MB-453移植瘤模型中,Afatinib(20 mg/kg,口服给药)可显著诱导肿瘤衰退,累积治疗/对照肿瘤体积比(T/C比)为2%,并下调EGFR和AKT磷酸化水平。[1] 在A7、A431、FaDu、UT-SCC-14和UT-SCC-15移植瘤模型中,Afatinib(30 mg/kg,口服给药)可显著延长肿瘤生长时间。[3] 在HER2扩增移植瘤模型中,Afatinib(30 mg/kg,口服给药)可显著抑制肿瘤生长,并显著延长生存期。[4] 在HER2阳性胃癌NCI-N87移植瘤模型中,Afatinib(25 mg/kg)口服给药4天可显著减小肿瘤体积,给药21天几乎完全治愈肿瘤。[5]

特征:


产品名称:卡博替尼苹果酸盐

产品别名:Cabozantinib malate (XL184)

CAS.NO:1140909-48-3

分子式:C28H24FN3O5.C4H6O5

分子量:635.59

稳定性:3年 -20℃粉状 6个月-80℃溶于溶剂

产品描述:Cabozantinib malate (XL184)是Cabozantinib的苹果酸盐,是有效的VEGFR2抑制剂,IC50为0.035 nM,也抑制c-Met, Ret, Kit, Flt-1/3/4, Tie2和AXL,无细胞试验中IC50分别为1.3 nM, 4 nM, 4.6 nM, 12 nM/11.3 nM/6 nM, 14.3 nM和7 nM。

靶点:VEGFR2/KDR [1] c-Met [1] Kit [1] VEGFR3/FLT4 [1] Axl [1]

体外研究:Cabozantinib has weak inhibitory activity against RON and PDGFRβ with IC50 of 124 nM and 234 nM, respectivey, and has low activity against FGFR1 with IC50 of 5.294 μM. [1] Cabozantinib at low concentration (0.1-0.5 μM) is sufficient to induce marked inhibition of constitutive and inducible Met phosphorylation and its resultant downstream signaling in MPNST cells, and inhibit HGF-induced MPNST cell migration and invasion. Cabozantinib also induces marked inhibition of Met and VEGFR2 phosphorylation in cytokine-stimulated human umbilical vein endothelial cells (HUVECs). Although Cabozantinib has no significant effect on MPNST cell growth at 0.1 μM, Cabozantinib at 5-10 μM significantly inhibits the MPNST cell growth. [2]

体内研究:Cabozantinib treatment at 30 mg/kg in RIP-Tag2 mice with spontaneous pancreatic islet tumors disrupts 83% of the tumor vasculature, reduces pericytes and empty basement membrane sleeves, causes widespread intratumoral hypoxia and extensive tumor cell apoptosis, and slows regrowth of the tumor vasculature after drug withdrawal, more significantly compared with XL999 that blocks VEGFR but not c-Met, leading to only 43% reduction in vascularity, suggesting that concurrent inhibition of VEGFR and other functionally relevant receptor tyrosine kinases (RTK) amplifies angiogenesis inhibition. Cabozantinib also decreases invasiveness of primary tumors and reduces metastasis. [1] Cabozantinib at 30 mg/kg/day significantly abrogates human MPNST xenografts growth and metastasis in SCID mice. [2] Administration of Cabozantinib induces dose-dependent inhibition of tumor growth in breast, lung, and glioma tumor models, in association with decreased tumor and endothelial cell proliferation as well as increased apoptosis. A single oral dose of Cabozantinib is sufficient to induce sustained tumor growth inhibition in MDA-MB-231 tumor-bearing mice and C6 tumor-bearing rats at 100 mg/kg and 10 mg/kg, respectively. [3]

特征: