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单克隆抗磷脂酰丝氨酸抗体与吉西他滨联合使用可强烈抑制小鼠原位胰腺肿瘤的生长和转移。

Combination of a monoclonal anti-phosphatidylserine antibody with gemcitabine strongly inhibits the growth and metastasis of orthotopic pancreatic tumors in mice.

作者信息

Beck Adam W, Luster Troy A, Miller Andrew F, Holloway Shane E, Conner Chris R, Barnett Carlton C, Thorpe Philip E, Fleming Jason B, Brekken Rolf A

机构信息

Simmons Comprehensive Cancer Center and Hamon Center for Therapeutic Oncology Research, University of Texas Southwestern Medical Center, Dallas, TX 75390-8593, USA.

出版信息

Int J Cancer. 2006 May 15;118(10):2639-43. doi: 10.1002/ijc.21684.

DOI:10.1002/ijc.21684
PMID:16353142
Abstract

Pancreatic cancer continues to have a dismal prognosis and novel therapy is needed. In this study, we evaluate a promising new target for therapy, phosphatidylserine (PS). PS is an anionic phospholipid located normally on the inner leaflet of the plasma membrane in mammalian cells. In the tumor microenvironment, PS becomes externalized on vascular endothelium. The monoclonal antibody 3G4 binds PS and promotes an inflammatory response against tumor blood vessels, resulting in reduction of tumor growth. Mice with orthotopic pancreatic tumors were treated with 3G4, gemcitabine or a combination of both drugs. Tumor burden including pancreas weight and metastatic lesions (liver, lymph node and peritoneal) were reduced 3- to 5-fold by the combination therapy as compared with 1.5- to 2-fold with 3G4 and gemcitabine alone, respectively. Treatment of tumor-bearing animals with the combination therapy increased macrophage infiltration into the tumor mass 10-fold and reduced microvessel density in the tumor by 2.5-fold compared with tumors from untreated animals. Gemcitabine alone and 3G4 alone were less effective than the combination of the 2 agents together. The additive therapeutic effect of both agents appears to be because chemotherapy increases PS exposure on tumor vascular endothelium and amplifies the target for attack by 3G4. In conclusion, 3G4 enhanced the anti-tumor and anti-metastatic activity of gemcitabine without contributing to toxicity.

摘要

胰腺癌的预后仍然很差,需要新的治疗方法。在本研究中,我们评估了一种有前景的新治疗靶点——磷脂酰丝氨酸(PS)。PS是一种阴离子磷脂,正常情况下位于哺乳动物细胞质膜的内小叶。在肿瘤微环境中,PS在血管内皮细胞上外化。单克隆抗体3G4与PS结合,促进针对肿瘤血管的炎症反应,从而导致肿瘤生长减缓。将原位胰腺肿瘤小鼠用3G4、吉西他滨或两种药物联合治疗。与单独使用3G4和吉西他滨分别使肿瘤负担(包括胰腺重量和转移病灶(肝脏、淋巴结和腹膜))降低1.5至2倍相比,联合治疗使其降低了3至5倍。与未治疗动物的肿瘤相比,联合治疗荷瘤动物可使巨噬细胞向肿瘤块内浸润增加10倍,并使肿瘤内微血管密度降低2.5倍。单独使用吉西他滨和单独使用3G4的效果均不如两种药物联合使用。两种药物的相加治疗效果似乎是因为化疗增加了肿瘤血管内皮细胞上PS的暴露,并扩大了3G4的攻击靶点。总之,3G4增强了吉西他滨的抗肿瘤和抗转移活性,且无毒性作用。

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