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卡介苗负载阳离子纳米颗粒对膀胱肿瘤诱导大鼠模型膀胱内免疫治疗的抗肿瘤疗效

Antitumor Efficacy of Bacillus Calmette-Guerin Loaded Cationic Nanoparticles for Intravesical Immunotherapy of Bladder Tumor Induced Rat Model.

作者信息

Erdoğar Nazli, Iskit Alper B, Eroğlu Hakan, Sargon Mustafa F, Mungan N Aydin, Bilensoy Erem

出版信息

J Nanosci Nanotechnol. 2015 Dec;15(12):10156-64. doi: 10.1166/jnn.2015.11690.

Abstract

For bladder cancer, intravesical chemo/immunotherapy is widely used as adjuvant therapy after surgical transurethral resection. Bacillus Calmette-Guerin (BCG) is a live attenuated Mycobacterium of the same family as tuberculosis, that is capable of inducing a local inflammatory response upon instillation into the bladder. Intravesical therapy with BCG has proved to be more effective in the prophylaxis and treatment of superficial bladder tumors than most chemotherapeutic agents used for the same indication. However, compared to intravesical chemotherapy, BCG immunotherapy provokes more pronounced local and systemic reactions. In addition to the commonly induced granulomatous inflammatory changes in the bladder, which produce irritative symptoms, this therapy may cause systemic side effects varying from mild malaise and fever to, in rare instances, life-threatening or fatal sepsis. Nanoparticles with positive surface charge and mucoadhesive properties were developed to overcome these side effects. Hence, the aim of this study was to optimize and evaluate cationic chitosan (CS) nanoparticles encapsulating BCG in terms of antitumor efficacy after intravesical administration in bladder tumor, induced in rat model. It was found that nanoparticle formulations of 269-375 nm in size can be produced with 42% encapsulation efficiency. The zeta potential was positive and was suitable for intravesical administration. Antitumor efficacy was determined over the parameters of histopathological evaluation, survival rate and mean bladder weight in comparison to treatment with commercial BCG solution. Concerning survival rates, BCG-loaded chitosan nanoparticles resulted in significantly longer survival than BCG commercial product (up to 86 days of survival with no systemic side effects). When compared to healthy bladder weight averages, all groups (especially BCG commercial solution) showed higher bladder weights confirming tumor formation. Histopathological findings confirmed antitumor activity in all treatment groups and optimum findings were observed in groups treated with CS nanoparticles encapsulating BCG. At the same time, significant nanoparticle accumulation in bladder tissues was observed especially for BCG-loaded CS group. In this study, it was clearly observed that cationic CS nanoparticles provide a significantly improved perspective in intravesical immunotherapy of bladder tumors.

摘要

对于膀胱癌,膀胱内化学/免疫疗法广泛用作经尿道手术切除后的辅助治疗。卡介苗(BCG)是一种与结核同属的减毒活分枝杆菌,将其注入膀胱后能够引发局部炎症反应。事实证明,与用于相同适应症的大多数化疗药物相比,膀胱内注射卡介苗治疗浅表性膀胱肿瘤在预防和治疗方面更为有效。然而,与膀胱内化疗相比,卡介苗免疫疗法会引发更明显的局部和全身反应。除了通常在膀胱中诱发的肉芽肿性炎症变化(会产生刺激症状)外,这种疗法还可能导致全身副作用,从轻微不适和发热到罕见的危及生命或致命的败血症。开发具有正表面电荷和粘膜粘附特性的纳米颗粒以克服这些副作用。因此,本研究的目的是在大鼠模型诱导的膀胱肿瘤中,对膀胱内给药后包裹卡介苗的阳离子壳聚糖(CS)纳米颗粒的抗肿瘤疗效进行优化和评估。结果发现,可以制备尺寸为269-375nm、包封率为42%的纳米颗粒制剂。zeta电位为正,适合膀胱内给药。与使用商用卡介苗溶液治疗相比,通过组织病理学评估、存活率和平均膀胱重量等参数确定抗肿瘤疗效。关于存活率,负载卡介苗的壳聚糖纳米颗粒导致的存活时间明显长于商用卡介苗产品(存活时间长达86天,且无全身副作用)。与健康膀胱平均重量相比,所有组(尤其是商用卡介苗溶液组)的膀胱重量均较高,证实有肿瘤形成。组织病理学结果证实了所有治疗组的抗肿瘤活性,在用包裹卡介苗的壳聚糖纳米颗粒治疗的组中观察到最佳结果。同时,观察到纳米颗粒在膀胱组织中大量积聚,尤其是负载卡介苗的壳聚糖组。在本研究中,清楚地观察到阳离子壳聚糖纳米颗粒在膀胱肿瘤的膀胱内免疫治疗中提供了显著改善的前景。

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