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首页> 外文期刊>癌と化学療法 >A study of the oncolytic effect of a newly designed CDDP system on an experimental animal model with carcinomatous ascites
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A study of the oncolytic effect of a newly designed CDDP system on an experimental animal model with carcinomatous ascites

机译:新设计的CDDP系统对癌性腹水实验动物模型的溶瘤作用研究

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We provided a novel cancer chemotherapeutic system for the treatment of locoregional cancer lesions, e.g. malignant peritonitis and pleuritis. The carriers were prepared with fibrin hydrogel clots (FCs) and hemostatic gelatin powder (Gp) using an original technique, after which cis-platinum (CDDP) was loaded into the carriers. In in vitro tests, the new carrier gradually degraded in 10-15 days in our fibrinolytic systems and the release of CDDP from the carrier continued for the same period. The CDDP delivered in the incubation medium was mainly the protein-bound type, and the released CDDP inhibited the proliferation of AH-130 ascitic hepatoma. To evaluate antineoplastic activities in vivo, we placed CDDP-loaded carriers into the abdominal cavities of AH-130 cancer-bearing rats. Seven of 8 cancer-bearing animals treated with our CDDP-systems survived for more than 5 weeks, and evidence of malignancy completely disappeared. These surviving rats were then challenged with AH-130 cells. Four of 5 repeatedly challenged rats survived for more than 7 months and revealed no evidence of recurrence of the cancer. All other rats died of cachexia with massive ascites and metastases within 2 weeks. Thus, our newly devised system exhibited a sustained release of CDDP with possible antineoplastic efficacy in an experimental animal model with carcinomatous ascites.
机译:我们提供了一种新型的癌症化学治疗系统,用于治疗局部癌灶,例如恶性腹膜炎和胸膜炎。使用原始技术,使用纤维蛋白水凝胶凝块(FCs)和止血明胶粉(Gp)制备载体,然后将顺铂(CDDP)加载到载体中。在体外测试中,新的载体在我们的纤溶系统中在10-15天内逐渐降解,并且CDDP从载体中的释放持续了同一时期。在培养液中传递的CDDP主要是蛋白结合型,释放的CDDP抑制了AH-130腹水型肝癌的增殖。为了评估体内抗肿瘤活性,我们将载有CDDP的载体置于AH-130荷癌大鼠的腹腔中。用我们的CDDP系统治疗的8只荷瘤动物中,有7只存活了超过5周,并且恶性肿瘤的证据完全消失了。然后用AH-130细胞攻击这些存活的大鼠。 5只反复受到挑战的大鼠中有4只存活超过7个月,并且没有发现癌症复发的证据。所有其他大鼠在2周内死于恶病质,并伴有大量腹水和转移。因此,我们新设计的系统在具有癌性腹水的实验动物模型中显示出CDDP的持续释放,并具有抗肿瘤作用。

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