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逐层组装的白细胞介素-12纳米颗粒在卵巢肿瘤中引发安全有效的反应。

Layer-by-layer interleukin-12 nanoparticles drive a safe and effective response in ovarian tumors.

作者信息

Barberio Antonio E, Smith Sean G, Pires Ivan S, Iyer Sonia, Reinhardt Ferenc, Melo Mariane B, Suh Heikyung, Weinberg Robert A, Irvine Darrell J, Hammond Paula T

机构信息

Department of Chemical Engineering Massachusetts Institute of Technology Cambridge Massachusetts USA.

Koch Institute for Integrative Cancer Research Massachusetts Institute of Technology Cambridge Massachusetts USA.

出版信息

Bioeng Transl Med. 2022 Dec 1;8(2):e10453. doi: 10.1002/btm2.10453. eCollection 2023 Mar.

Abstract

Ovarian cancer is especially deadly, challenging to treat, and has proven refractory to known immunotherapies. Cytokine therapy is an attractive strategy to drive a proinflammatory immune response in immunologically cold tumors such as many high grade ovarian cancers; however, this strategy has been limited in the past due to severe toxicity. We previously demonstrated the use of a layer-by-layer (LbL) nanoparticle (NP) delivery vehicle in subcutaneous flank tumors to reduce the toxicity of interleukin-12 (IL-12) therapy upon intratumoral injection. However, ovarian cancer cannot be treated by local injection as it presents as dispersed metastases. Herein, we demonstrate the use of systemically delivered LbL NPs using a cancer cell membrane-binding outer layer to effectively target and engage the adaptive immune system as a treatment in multiple orthotopic ovarian tumor models, including immunologically cold tumors. IL-12 therapy from systemically delivered LbL NPs shows reduced severe toxicity and maintained anti-tumor efficacy compared to carrier-free IL-12 or layer-free liposomal NPs leading to a 30% complete survival rate.

摘要

卵巢癌极具致命性,治疗颇具挑战性,且已证明对已知的免疫疗法具有抗性。细胞因子疗法是一种在免疫原性冷肿瘤(如许多高级别卵巢癌)中驱动促炎免疫反应的有吸引力的策略;然而,由于严重的毒性,该策略在过去受到了限制。我们之前证明了在皮下侧腹肿瘤中使用逐层(LbL)纳米颗粒(NP)递送载体来降低肿瘤内注射白细胞介素-12(IL-12)疗法的毒性。然而,卵巢癌无法通过局部注射进行治疗,因为它表现为分散的转移灶。在此,我们展示了使用具有癌细胞膜结合外层的全身递送LbL NPs,以有效靶向并激活适应性免疫系统,作为多种原位卵巢肿瘤模型(包括免疫原性冷肿瘤)的一种治疗方法。与无载体IL-12或无层脂质体NP相比,全身递送LbL NPs的IL-12疗法显示出较低的严重毒性并保持了抗肿瘤疗效,导致30%的完全生存率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a8cf/10013828/d39813240743/BTM2-8-e10453-g001.jpg

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