^(99m)Tc-D_2C_5用于人肝细胞癌肿瘤受体显像研究

目的:探讨99mTc-D2C5用于人肝癌细胞系SMMC-7721裸鼠原位种植肝癌模型肿瘤受体成像的价值。方法:人肝细胞癌SMMC-7721采用隧道包埋法植入Balb/c nu/nu裸鼠肝左叶建立原位种植肿瘤模型。荷瘤裸鼠16只,随机分为2组,每组8只,分别经尾静脉注射99mTc-D2C5、99mTc-mIgG,放射剂量为14.8MBq。采用SPECT采集99mTc-D2C5和99mTc-mIgG注射后1h、3h显影图像。显像结束后处死动物,采用γ计数器检测体内放射性分布。结果:注射99mTc-D2C5后1 h时,裸鼠肝肿瘤部位显影,3h时肿瘤显影最清晰。注射99mTc-mIgG后,肿瘤部位未见明显放射性浓聚;3h时99mTc-D2C5裸鼠体内靶/非靶组织的比值中,肿瘤/血(T/B)为6.8,肿瘤/肝(T/L)为2.8,肿瘤/肌肉(T/M)为17.3。结论:研究表明99mTc-D2C5可与人肝癌细胞SMMC-7721高特异性和高亲和力的结合,在肝癌显像中应用前景十分乐观。

人肝细胞癌转铁蛋白受体显像及靶向治疗研究

目的探讨131I-D2C5用于肿瘤受体成像和放射免疫治疗的价值。方法人肝细胞癌SMMC-7721采用隧道包埋法植入Balb/c(-/-)裸鼠肝左叶,建立原位种植肿瘤模型。①12只荷瘤裸鼠随机分为两组,每组6只,分别经尾静脉注射131I-D2C51、31I-mIgG,放射剂量均为14.8MBq/只;SPECT采集131I-D2C5和131I-mIgG注射后6h、24h放射自显影图像;γ计数器检测体内放射性分布。②18只荷瘤裸鼠随机分为两组,每组9只,每周分别经腹腔注射131I-D2C51、31I-mIgG,连续6周;另外9只荷瘤裸鼠每周腹腔注射生理盐水200μl作为对照组。8周后比较各组肿瘤体积,计算其生长抑制率,评估肿瘤坏死程度。结果注射131I-D2C5后6h时,裸鼠肝肿瘤部位显影,24h时肿瘤显影最清晰。注射131I-mIgG后,肿瘤部位未见明显放射性浓聚。24h时131I-D2C5组裸鼠体内肿瘤/血为6.6,肿瘤/肝为2.2,肿瘤/肌肉为20.8。静脉注射131I-D2C5导向治疗较131I-mIgG更显著抑制人肝细胞癌裸鼠模型中肿瘤的生长,促进肿瘤坏死。结论131I-D2C5能与人肝细胞癌SMMC-7721高特异性、高亲和力地结合。在肝癌显像及生物靶向治疗中具有广泛的应用前景。

Modern treatment of gastric gastrointestinal stromal tumors

Gastrointestinal stromal tumors (GIST) are rare mesenchymal smooth muscle sarcomas that can arise anywhere within the gastrointestinal tract. Sporadic mutations within the tyrosine kinase receptors of the interstitial cells of Cajal have been identified as the key molecular step in GIST carcinogenesis. Although many patients are asymptomatic, the most common associated symptoms include: abdominal pain, dyspepsia, gastric outlet obstruction, and anorexia. Rarely, GIST can perforate causing life-threatening hemoperitoneum. Most are ultimately diagnosed on cross-sectional imaging studies (i.e., computed tomography and/or magnetic resonance imaging in combination with upper endoscopy. Endoscopic ultrasonographic localization of these tumors within the smooth muscle layer and acquisition of neoplastic spindle cells harboring mutations in the c-KIT gene is pathognomonic. Curative treatment requires a complete gross resection of the tumor. Both open and minimally invasive operations have been shown to reduce recurrence rates and improve long-term survival. While there is considerable debate over whether GIST can be benign neoplasms, we believe that all GIST have malignant potential, but vary in their propensity to recur after resection and metastasize to distant organ sites. Prognostic factors include location, size (i.e., > 5 cm), grade (> 5-10 mitoses per 50 high power fields and specific mutational events that are still being defined. Adjuvant therapy with tyrosine kinase inhibitors, such as imatinib mesylate, has been shown to reduce the risk of recurrence after one year of therapy. Treatment of locally-advanced or borderline resectable gastric GIST with neoadjuvant imatinib has been shown to induce regression in a minority of patients and stabilization in the majority of cases. This treatment strategy potentially reduces the need for more extensive surgical resections and increases the number of patients eligible for curative therapy. The modern surgical treatment of gastric GIST combines the novel use of targeted therapy and aggressive minimally invasive surgical procedures to provide effective treatment for this lethal, but rare gastrointestinal malignancy.