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开发极化适当的滋养层干细胞衍生类器官以模拟早期人类妊娠。

Development of properly-polarized trophoblast stem cell-derived organoids to model early human pregnancy.

作者信息

Zhou J, Sheridan M A, Tian Y, Dahlgren K J, Messler M, Peng T, Ezashi T, Schulz L C, Ulery B D, Roberts R M, Schust D J

出版信息

bioRxiv. 2023 Oct 2:2023.09.30.560327. doi: 10.1101/2023.09.30.560327.

Abstract

UNLABELLED

The development of human trophoblast stem cells (hTSC) and stem cell-derived trophoblast organoids has enabled investigation of placental physiology and disease and early maternal-fetal interactions during a stage of human pregnancy that previously had been severely restricted. A key shortcoming in existing trophoblast organoid methodologies is the non-physiologic position of the syncytiotrophoblast (STB) within the inner portion of the organoid, which neither recapitulates placental villous morphology nor allows for facile modeling of STB exposure to the endometrium or the contents of the intervillous space. Here we have successfully established properly-polarized human trophoblast stem cell (hTSC)-sourced organoids with STB forming on the surface of the organoid. These organoids can also be induced to give rise to the extravillous trophoblast (EVT) lineage with HLA-G migratory cells that invade into an extracellular matrix-based hydrogel. Compared to previous hTSC organoid methods, organoids created by this method more closely mimic the architecture of the developing human placenta and provide a novel platform to study normal and abnormal human placental development and to model exposures to pharmaceuticals, pathogens and environmental insults.

MOTIVATION

Human placental organoids have been generated to mimic physiological cell-cell interactions. However, those published models derived from human trophoblast stem cells (hTSCs) or placental villi display a non-physiologic "inside-out" morphology. , the placental villi have an outer layer of syncytialized cells that are in direct contact with maternal blood, acting as a conduit for gas and nutrient exchange, and an inner layer of progenitor, single cytotrophoblast cells that fuse to create the syncytiotrophoblast layer. Existing "inside-out" models put the cytotrophoblast cells in contact with culture media and substrate, making physiologic interactions between syncytiotrophoblast and other cells/tissues and normal and pathogenic exposures coming from maternal blood difficult to model. The goal of this study was to develop an hTSC-derived 3-D human trophoblast organoid model that positions the syncytiotrophoblast layer on the outside of the multicellular organoid.

摘要

未标注

人类滋养层干细胞(hTSC)和干细胞来源的滋养层类器官的发展,使得在人类怀孕的一个此前受到严格限制的阶段,能够对胎盘生理和疾病以及早期母胎相互作用进行研究。现有滋养层类器官方法的一个关键缺点是合体滋养层(STB)在类器官内部的非生理性位置,这既不能重现胎盘绒毛形态,也无法方便地模拟STB与子宫内膜或绒毛间隙内容物的接触。在此,我们成功建立了具有正确极性的、源自人类滋养层干细胞(hTSC)的类器官,其表面形成了STB。这些类器官还可被诱导产生绒毛外滋养层(EVT)谱系,带有侵入基于细胞外基质的水凝胶中的HLA - G迁移细胞。与先前的hTSC类器官方法相比,通过这种方法创建的类器官更紧密地模拟了发育中的人类胎盘结构,并为研究正常和异常的人类胎盘发育以及模拟药物、病原体和环境损伤的暴露提供了一个新平台。

动机

已生成人类胎盘类器官以模拟生理细胞间相互作用。然而,那些源自人类滋养层干细胞(hTSC)或胎盘绒毛的已发表模型呈现出非生理性的“由内向外”形态。胎盘绒毛有一层与母体血液直接接触的合体化细胞外层,作为气体和营养交换的通道,以及一层祖细胞、单个细胞滋养层细胞内层,这些细胞融合形成合体滋养层。现有的“由内向外”模型使细胞滋养层细胞与培养基和底物接触,使得合体滋养层与其他细胞/组织之间的生理相互作用以及来自母体血液的正常和致病性暴露难以模拟。本研究的目标是开发一种源自hTSC的三维人类滋养层类器官模型,将合体滋养层定位在多细胞类器官的外部。

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