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卵巢癌细胞芯片中的切变流与细胞外基质的平衡

The Balance Between Shear Flow and Extracellular Matrix in Ovarian Cancer-on-Chip.

机构信息

PASTEUR, Département de chimie, École normale supérieure, PSL University, Sorbonne Université, CNRS, Paris, 75005, France.

Equipe de Recherche sur les Relations Matrice Extracellulaire-Cellules, ERRMECe (EA1391), Groupe Matrice Extracellulaire et physiopathologie (MECuP), Institut des Matériaux, I-MAT (FD4122), CY Cergy Paris Université, Cergy, 95000, France.

出版信息

Adv Healthc Mater. 2024 Sep;13(23):e2400938. doi: 10.1002/adhm.202400938. Epub 2024 Jun 8.

Abstract

Ovarian cancer is the most lethal gynecologic cancer in developed countries. In the tumor microenvironment, the extracellular matrix (ECM) and flow shear stress are key players in directing ovarian cancer cells invasion. Artificial ECM models based only on ECM proteins are used to build an ovarian tumor-on-chip to decipher the crosstalk between ECM and shear stress on the migratory behavior and cellular heterogeneity of ovarian tumor cells. This work shows that in the shear stress regime of the peritoneal cavity, the ECM plays a major role in driving individual or collective ovarian tumor cells migration. In the presence of basement membrane proteins, migration is more collective than on type I collagen regardless of shear stress. With increasing shear stress, individual cell migration is enhanced; while, no significant impact on collective migration is measured. This highlights the central position that ECM and flow shear stress should hold in in vitro ovarian cancer models to deepen understanding of cellular responses and improve development of ovarian cancer therapeutic platforms. In this frame, adding flow provides significant improvement in biological relevance over the authors' previous work. Further steps for enhanced clinical relevance require not only multiple cell lines but also patient-derived cells and sera.

摘要

卵巢癌是发达国家最致命的妇科癌症。在肿瘤微环境中,细胞外基质(ECM)和流动切应力是指导卵巢癌细胞侵袭的关键因素。仅基于 ECM 蛋白的人工 ECM 模型被用于构建卵巢肿瘤芯片,以破译 ECM 和切应力对卵巢肿瘤细胞迁移的迁移行为和细胞异质性的串扰。这项工作表明,在腹腔的切应力范围内,ECM 在驱动单个或集体卵巢肿瘤细胞迁移中起主要作用。在存在基底膜蛋白的情况下,迁移比在 I 型胶原上更具集体性,而与切应力无关。随着切应力的增加,单个细胞的迁移得到增强;而对集体迁移没有明显的影响。这凸显了 ECM 和流动切应力在体外卵巢癌模型中应占据的核心地位,以加深对细胞反应的理解并改善卵巢癌治疗平台的开发。在这种情况下,与作者之前的工作相比,添加流动显著提高了生物学相关性。为了提高临床相关性,不仅需要多个细胞系,还需要患者来源的细胞和血清。

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