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通过可生物降解的131I-降胆固醇植入物预防乳腺癌小鼠模型中的肿瘤复发和远处转移形成

Prevention of tumor recurrence and distant metastasis formation in a breast cancer mouse model by biodegradable implant of 131I-norcholesterol.

作者信息

Azab Abdel Kareem, Kleinstern Jackie, Doviner Victoria, Orkin Boris, Srebnik Morris, Nissan Aviram, Rubinstein Abraham

机构信息

Department of Pharmaceutics, The Hebrew University of Jerusalem, School of Pharmacy, Jerusalem, Israel.

出版信息

J Control Release. 2007 Nov 6;123(2):116-22. doi: 10.1016/j.jconrel.2007.07.014. Epub 2007 Aug 8.

Abstract

Brachytherapy has many potential roles in cancer therapy. However, major constraints are associated with placement and removal procedures of the brachytherapy machinery. An attractive approach would be the use of a biodegradable implant loaded with a radioisotope, thus enabling targeted radiotherapy, while reducing the need for surgical procedures for the removal of brachytherapy hardware. In this study, crosslinked chitosan (Ct) hydrogels were prepared and loaded with (131)I-norcholesterol ((131)I-NC). The radioactive hydrogels ((131)I-NC-Ct) were implanted adjacent to 4T1 cell-induced tumors in two different xenograft mice models either as primary therapy or surgical adjuvant therapy of breast cancer. Non-treated mice and mice implanted with naive (non-radioactive) hydrogels served as control groups. In the primary therapy model, the progression rate of the tumor was delayed by two weeks compared with the non-treated and the naive-implant control animals, resulting in a one-week extension in the survival of the treated animals. In the adjuvant therapy model, for the treatment of minimal residual disease, (131)I-NC-Ct implants were able to prevent 69% of tumor recurrence, and to prevent metastatic spread resulting in long-term survival, compared with 0% long-term survival of the non-treated and the naive control groups. Imaging of the hydrogel's in vivo elimination revealed a first order process with a half-life of 14 days. The degradation was caused by oxidation of the Ct as was assessed by in vitro H&E stain. Biodegradable radioactive implants are suggested as a novel platform for the delivery of brachytherapy. This radiotherapy regimen may prevent locoregional recurrence and metastatic spread after tumor resection.

摘要

近距离放射治疗在癌症治疗中具有许多潜在作用。然而,主要限制与近距离放射治疗设备的放置和移除程序相关。一种有吸引力的方法是使用负载放射性同位素的可生物降解植入物,从而实现靶向放射治疗,同时减少移除近距离放射治疗硬件所需的外科手术。在本研究中,制备了交联壳聚糖(Ct)水凝胶并负载了131I-降胆固醇(131I-NC)。将放射性水凝胶(131I-NC-Ct)作为乳腺癌的初始治疗或手术辅助治疗,植入两种不同异种移植小鼠模型中4T1细胞诱导的肿瘤附近。未治疗的小鼠和植入未处理(非放射性)水凝胶的小鼠作为对照组。在初始治疗模型中,与未治疗和植入未处理水凝胶的对照动物相比,肿瘤的进展速度延迟了两周,导致治疗动物的生存期延长了一周。在辅助治疗模型中,为了治疗微小残留病,与未治疗组和未处理对照组0%的长期生存率相比,131I-NC-Ct植入物能够预防69%的肿瘤复发,并防止转移扩散,从而实现长期生存。水凝胶体内消除的成像显示为一级过程,半衰期为14天。通过体外苏木精和伊红染色评估,降解是由Ct的氧化引起的。可生物降解的放射性植入物被认为是一种新型的近距离放射治疗递送平台。这种放射治疗方案可能预防肿瘤切除后的局部区域复发和转移扩散。

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