In vivo and in vitro inhibition of pancreatic cancer growth by targeted alpha therapy using 213Bi-CHX.A'-C595.

Qu CF; Songl YJ; Rizvi SM; Li Y; Smith R; Perkins AC; Morgenstern A; Brechbiel M; Allen BJ

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In vivo and in vitro inhibition of pancreatic cancer growth by targeted alpha therapy using 213Bi-CHX.A'-C595.

机译：通过使用213Bi-CHX.A” -C595的靶向α疗法在体内和体外抑制胰腺癌的生长。

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PURPOSE: The aim of this study was to investigate the effect of targeted alpha therapy for the control of in vitro pancreatic cancer cell clusters and micrometastatic cancer lesions in vivo. METHODS: The expression of tumor-associated antigen MUC-1 on three pancreatic cancer cell clusters and animal xenografts was detected by indirect immmunostaining. Monoclonal antibodies C595 (test) and A2 (non-specific control) were labeled with 213Bi using the chelator CHX.A" to form the alpha-immunoconjugate (AIC). Cell clusters were incubated with AIC and examined at 48 h. Apoptosis was documented using the TUNEL assay. In vivo, an antiproliferative effect for tumors was tested at two days post-subcutaneous cell inoculation. Mice were injected with different concentrations of AIC by regional or systemic administration. Changes in tumor progression were assessed by tumor size. RESULTS: MUC-1 is strongly expressed on CFPAC-1, PANC-1 and moderate expression was found CAPAN-1 cell clusters and tumor xenografts. The AICs can target and kill cancer cell clusters (100 mm) in vitro. Some 73-81 % of cells were TUNEL positive cells in the clusters after incubation with AIC. At two days post- cell inoculation in mice, a single local injection of 74 and 148 MBq/kg of AIC causes complete inhibition of tumor growth. Systemic injections of 111, 222 and 333 MBq/kg of AIC cause significant tumor growth delay after 16 weeks, compared with the nonspecific control providing 333 MBq/kg after 16 weeks. CONCLUSIONS: CFPAC-1, PANC-1 and CAPAN-1 pancreatic cancer cell clusters and pancreatic tumor xenografts show high expression of the MUC-1 target antigen. 213Bi-C595 can specifically target and regress pancreatic cancer cell clusters in vitro, and delay and inhibit tumor growth in vivo. 213Bi-C595 may be a useful agent for the treatment of micrometastatic pancreatic cancer with overexpression of MUC 1 antigen in post-surgical patients with minimal residual disease.

机译：目的：本研究的目的是研究靶向α疗法在体内控制体外胰腺癌细胞团和微转移癌病变的效果。方法：通过间接免疫染色检测三种胰腺癌细胞簇和动物异种移植物中肿瘤相关抗原MUC-1的表达。使用螯合剂CHX.A“用213Bi标记单克隆抗体C595（测试）和A2（非特异性对照）以形成α-免疫偶联物（AIC）。将细胞簇与AIC一起孵育并在48 h进行检查。使用TUNEL法在体内，在皮下接种细胞后两天测试了对肿瘤的抗增殖作用，通过局部或全身给药向小鼠注射了不同浓度的AIC，通过肿瘤大小评估了肿瘤进展的变化。 MUC-1在CFPAC-1，PANC-1上强烈表达，并在CAPAN-1细胞簇和肿瘤异种移植物中适度表达，AIC可以靶向并杀死100 mm的癌细胞簇，约占73-81％ AIC孵育后，细胞为TUNEL阳性细胞簇，在小鼠细胞接种后两天，一次局部注射74和148 MBq / kg AIC会完全抑制肿瘤生长，全身注射111、222和3.33亿与16周后提供333 MBq / kg的非特异性对照相比，AIC的Bq / kg AIC导致显着的肿瘤生长延迟。结论：CFPAC-1，PANC-1和CAPAN-1胰腺癌细胞簇和胰腺肿瘤异种移植物显示MUC-1靶抗原的高表达。 213Bi-C595可以在体外特异性靶向和消退胰腺癌细胞团，并在体内延迟和抑制肿瘤生长。 213Bi-C595可能是治疗微转移性胰腺癌且MUC 1抗原过表达的有效药物，可用于术后残留疾病极少的患者。

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《Cancer biology & therapy》 |2005年第8期|共6页
作者
Qu CF; Songl YJ; Rizvi SM; Li Y; Smith R; Perkins AC; Morgenstern A; Brechbiel M; Allen BJ;
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正文语种 eng
中图分类肿瘤学;
关键词
Antibodies; Monoclonal; Isothiocyanates; Pancreatic Neoplasms; Pentetic Acid; 抗体; 单克隆; 异硫氰酸盐类; 胰腺肿瘤; 三胺五乙酸; 放射免疫疗法;

机译：Antibodies;Monoclonal;Isothiocyanates;Pancreatic Neoplasms;Pentetic Acid;抗体;单克隆;异硫氰酸盐类;胰腺肿瘤;三胺五乙酸;放射免疫疗法;

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1. In vivo and in vitro inhibition of pancreatic cancer growth by targeted alpha therapy using 213Bi-CHX.A"-C595. [J] . Qu CF, Songl YJ, Rizvi SM, Cancer biology & therapy . 2005,第8期

机译：通过使用213Bi-CHX.A” -C595的靶向α疗法在体内和体外抑制胰腺癌的生长。
2. Inhibition of growth of experimental human and hamster pancreatic cancers in vivo by a targeted cytotoxic bombesin analog. [J] . Szepeshazi K, Schally AV, Nagy A, Pancreas . 2005,第3期

机译：靶向的细胞毒性蛙毒素类似物抑制体内实验性人和仓鼠胰腺癌的生长。
3. Targeting the yin and the yang: Combined inhibition of the tyrosine kinase c-Src and the tyrosine phosphatase SHP-2 disrupts pancreatic cancer signaling and biology in vitro and tumor formation in vivo [J] . GomesE.G., ConnellyS.F., SummyJ.M. Pancreas . 2013,第5期

机译：靶向阴和阳：酪氨酸激酶c-Src和酪氨酸磷酸酶SHP-2的联合抑制在体外破坏胰腺癌的信号传导和生物学，并在体内形成肿瘤
4. Small Molecule ONC201/TIC10 Targets Chemotherapy-Resistant Colorectal Cancer Stem Cells In Vitro and In Vivo [C] . Varun Vijay Prabhu, Joshua E. Allen, David T. Dicker, Molecular Medicine TRI-CON. . 2014

机译：小分子ONC201 / TIC10在体外和体内靶向化疗抗性结肠直肠癌干细胞
5. Inhibition of Ape1's DNA repair activity as a target in cancer: Identification of novel small molecules that have translational potential for molecularly targeted cancer therapy [D] . Bapat, Aditi Ajit 2009

机译：抑制Ape1的DNA修复活性作为癌症靶标：鉴定具有翻译潜力的新型小分子，可用于分子靶向癌症治疗
6. MEK Inhibition Targets Cancer Stem Cells and Impedes Migration of Pancreatic Cancer Cells In Vitro and In Vivo [O] . Karolin Walter, Kanishka Tiwary, Marija Trajkovic-Arsic, 2019

机译：MEK抑制靶向癌症干细胞并阻止胰腺癌细胞的体外和体内迁移。
7. In vivo and in vitro inhibition of pancreatic cancer growth by targeted alpha therapy using 213Bi-CHX.A”-C595 [O] . Chang F. Qu, Yan J. Song, Syed M.A. Rizvi, 2005

机译：在体内和体外抑制胰腺癌的靶向α-疗法使用213bi-chx.a“-c595

In vivo and in vitro inhibition of pancreatic cancer growth by targeted alpha therapy using 213Bi-CHX.A'-C595.

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