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负载伊立替康和5-氟尿嘧啶的高负载核壳纳米载体用于结直肠癌的联合化疗

High-Load Core@Shell Nanocarriers with Irinotecan and 5-Fluorouracil for Combination Chemotherapy in Colorectal Cancer.

作者信息

Notter Silke, Choezom Dolma, Griebel Titus, Ramos-Gomes Fernanda, Möbius Wiebke, De Oliveira Tiago, Conradi Lena-Christin, Alves Frauke, Feldmann Claus

机构信息

Institute of Inorganic Chemistry Karlsruhe Institute of Technology (KIT) Engesserstraße 15 76131 Karlsruhe Germany.

Clinic for Haematology and Medical Oncology University Medical Center Goettingen (UMG) Robert Koch Straße 40 37075 Goettingen Germany.

出版信息

Small Sci. 2024 Aug 19;4(11):2400196. doi: 10.1002/smsc.202400196. eCollection 2024 Nov.

Abstract

Colorectal cancer (CRC) is the third most common cancer type and second leading cause of cancer-related deaths worldwide, requiring novel drug-delivery concepts. ITC@ZrO(TocP)/ZrO(FdUMP) core@shell nanocarriers (designated ITC-FdUMP-NC) with the clinically relevant chemotherapeutics irinotecan (ITC) and fluoro-2'-deoxyuridine-5'-phosphate (FdUMP) (active derivative of 5'-fluorouracil/5-FU) are a new type of nanocarrier with high drug payload (22 wt% of lipophilic ITC: particle core; 10 wt% of hydrophilic FdUMP: particle shell). The nanocarriers are tested in different CRC cell lines, a normal cell line, and rectal cancer patient-derived organoids (PDOs). Fluorescence-labeled nanocarriers show efficient uptake by all CRC cells and allow to distinctly track the intracellular trafficking toward endolysosomal compartments. Although free chemotherapeutic drugs exhibit a greater potency in 2D cell cultures, ITC-FdUMP-NC demonstrate equivalent cytotoxic efficacies as the freely dissolved drugs in the more complex 3D rectal cancer PDOs. The sustained drug-release profile of the nanocarriers contrasts favorably with conventional free drugs, potentially enhancing the therapeutic outcome in vivo. With a chemotherapeutic cocktail comparable to the clinically applied FOLFIRI (ITC + 5-FU), the ITC-FdUMP-NC represent a novel type of nanocarrier with high anti-tumor effect and high drug payload, offering a promising strategy to circumvent chemoresistance and to improve therapy efficacy in vivo with less side effects.

摘要

结直肠癌(CRC)是全球第三大常见癌症类型,也是癌症相关死亡的第二大主要原因,因此需要新的药物递送理念。含有临床相关化疗药物伊立替康(ITC)和氟代2'-脱氧尿苷-5'-磷酸(FdUMP,5'-氟尿嘧啶/5-FU的活性衍生物)的ITC@ZrO(TocP)/ZrO(FdUMP)核壳纳米载体(命名为ITC-FdUMP-NC)是一种新型纳米载体,具有高药物负载量(亲脂性ITC占22 wt%:颗粒核心;亲水性FdUMP占10 wt%:颗粒外壳)。这些纳米载体在不同的结直肠癌细胞系、一种正常细胞系以及直肠癌患者来源的类器官(PDO)中进行了测试。荧光标记的纳米载体显示出能被所有结直肠癌细胞有效摄取,并能清晰地追踪其向溶酶体区室的细胞内运输。尽管游离化疗药物在二维细胞培养中表现出更强的效力,但在更复杂的三维直肠癌PDO中,ITC-FdUMP-NC显示出与游离溶解药物相当的细胞毒性效力。纳米载体持续的药物释放曲线与传统游离药物相比具有优势,可能会提高体内治疗效果。ITC-FdUMP-NC含有与临床应用的FOLFIRI(ITC + 5-FU)相当的化疗药物组合,代表了一种新型的具有高抗肿瘤效果和高药物负载量的纳米载体,为规避化疗耐药性以及在体内以较少副作用提高治疗效果提供了一种有前景的策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f69f/11935085/0ff40a6a3e66/SMSC-4-2400196-g001.jpg

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