Spatial analysis of nanoparticle distribution in human breast xenografts reveals nanoparticles targeted to cancer cells localized with tumor-associated stromal cells.

Q1 Pharmacology, Toxicology and Pharmaceutics

Nanotheranostics Pub Date : 2023-01-01 DOI:10.7150/ntno.84255

Sean Healy, Elizabeth T Henderson, Suqi Ke, Jacqueline Kelly, Brian W Simons, Chen Hu, Robert Ivkov, Preethi Korangath

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引用次数: 2

Abstract

The biological influence of physicochemical parameters of "targeted" nanoparticles on their delivery to cancer tumors remains poorly understood. A comparative analysis of nanoparticle distributions in tumors following systemic delivery across several models can provide valuable insights. Methods: Bionized nanoferrite nanoparticles (iron oxide core coated with starch), either conjugated with a targeted anti-HER2 antibody (BH), or unconjugated (BP), were intravenously injected into athymic nude or NOD-scid gamma (NSG) female mice bearing one of five human breast cancer tumor xenografts growing in a mammary fat pad. Tumors were harvested 24 hours after nanoparticle injection, fixed, mounted, and stained. We performed detailed histopathology analysis by comparing spatial distributions of nanoparticles (Prussian blue) with various stromal cells (CD31, SMA, F4/80, CD11c, etc.) and the target antigen-expressing (HER2) tumor cells. Results: Only BH nanoparticles were retained in tumors and generally concentrated in the tumor periphery, with nanoparticle content diminishing towards the tumor interior. Nanoparticle distribution correlated strongly with specific stromal cells within each tumor type, which varied among tumor types and between mouse strains. Weak or no correlation between nanoparticle distribution and HER2 positive cells, or CD31 cells was observed. Conclusion: Antibody-labeled nanoparticles were retained across all tumors, irrespective of presence of the "target" antigen. Though presence of antibody on nanoparticles correlated with retention, non-cancerous host stromal cells were responsible for their retention in the tumor microenvironment. This study highlights gaps in our understanding of the complex biological interplay between disease and host immune biology, and the need to account for the influence of underlying aberrant tumor biology as factors determining nanoparticle fate in vivo.

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对人类乳腺异种移植物中纳米颗粒分布的空间分析揭示了纳米颗粒靶向肿瘤相关基质细胞定位的癌细胞。

“靶向”纳米颗粒的物理化学参数对其递送到癌症肿瘤的生物学影响仍然知之甚少。通过几种模型对肿瘤系统给药后的纳米颗粒分布进行比较分析可以提供有价值的见解。方法:将结合靶向抗her2抗体(BH)或未结合靶向抗her2抗体(BP)的生物化纳米铁氧体纳米颗粒(淀粉包裹的氧化铁核)静脉注射到胸腺裸或NOD-scid γ (NSG)雌性小鼠体内，这些小鼠携带生长在乳腺脂肪层中的五种人类乳腺癌肿瘤异种移植物之一。注射纳米颗粒24小时后收获肿瘤，固定、载具和染色。我们通过比较纳米粒子(普鲁士蓝)与各种基质细胞(CD31、SMA、F4/80、CD11c等)和靶抗原表达(HER2)肿瘤细胞的空间分布，进行了详细的组织病理学分析。结果:只有BH纳米颗粒在肿瘤中保留，并且通常集中在肿瘤周围，纳米颗粒含量向肿瘤内部逐渐减少。纳米颗粒分布与不同肿瘤类型和不同小鼠品系的特异性基质细胞密切相关。纳米颗粒分布与HER2阳性细胞或CD31细胞之间的相关性较弱或无相关性。结论:无论“靶”抗原是否存在，抗体标记的纳米颗粒都能在所有肿瘤中保留。虽然纳米颗粒上抗体的存在与滞留相关，但非癌性宿主基质细胞负责其在肿瘤微环境中的滞留。这项研究强调了我们对疾病和宿主免疫生物学之间复杂的生物学相互作用的理解上的差距，以及需要考虑潜在的异常肿瘤生物学作为决定体内纳米颗粒命运的因素的影响。

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