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可成像荧光转移导致在与人源原发性胰腺癌标本原位植入的转基因 GFP 小鼠中。

Imageable fluorescent metastasis resulting in transgenic GFP mice orthotopically implanted with human-patient primary pancreatic cancer specimens.

机构信息

Anti Cancer, Inc., San Diego, CA 92111, USA.

出版信息

Anticancer Res. 2012 Apr;32(4):1175-80.

Abstract

Tumors from pancreatic cancer patients were established in NOD/SCID mice immediately after surgery and subsequently passaged orthotopically in transgenic nude mice ubiquitously expressing green fluorescent protein (GFP). The primary patient tumors acquired GFP-expressing stroma. Subsequent liver metastases, and disseminated peritoneal metastases maintained the stroma from the primary tumor, and possibly recruited additional GFP-expressing stroma, resulting in their very bright fluorescence. The GFP-expressing stroma included cancer-associated fibroblasts and tumor-associated macrophages in both the primary and metastatic tumors. This imageable model of metastasis from a patient-tumor is an important advance over patient "tumorgraft" models currently in use, which are implanted subcutaneously, do not metastasize and are not imageable. The new imageable model of patient pancreatic cancer metastasis provides unique opportunities to identify current and novel antimetastatic therapeutics for individual patients.

摘要

从胰腺癌患者手术后立即建立的 NOD/SCID 小鼠肿瘤,并随后在普遍表达绿色荧光蛋白 (GFP) 的转基因裸鼠中经直肠移植。原发患者肿瘤获得 GFP 表达的基质。随后的肝转移和播散性腹膜转移保留了原发肿瘤的基质,并可能招募了额外的 GFP 表达的基质,导致其非常明亮的荧光。GFP 表达的基质包括原发和转移肿瘤中的癌相关成纤维细胞和肿瘤相关巨噬细胞。与目前正在使用的患者“肿瘤移植物”模型相比,这种来自患者肿瘤的可成像转移模型是一个重要的进展,因为后者是皮下植入的,不会转移且不可成像。这种新的可成像患者胰腺癌转移模型为确定针对个体患者的当前和新型抗转移治疗提供了独特的机会。

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