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简化的体内镶嵌分析平台,用于研究心脏发育过程中的细胞成熟。

Simplified platform for mosaic in vivo analysis of cellular maturation in the developing heart.

机构信息

Department of Cell Biology and Physiology, University of North Carolina at Chapel Hill, Chapel Hill, USA.

McAllister Heart Institute, University of North Carolina at Chapel Hill, Chapel Hill, USA.

出版信息

Sci Rep. 2019 Jul 24;9(1):10716. doi: 10.1038/s41598-019-47009-7.

Abstract

Cardiac cells develop within an elaborate electro-mechanical syncytium that continuously generates and reacts to biophysical force. The complexity of the cellular interactions, hemodynamic stresses, and electrical circuitry within the forming heart present significant challenges for mechanistic research into the cellular dynamics of cardiomyocyte maturation. Simply stated, it is prohibitively difficult to replicate the native electro-mechanical cardiac microenvironment in tissue culture systems favorable to high-resolution cellular/subcellular analysis, and current transgenic models of higher vertebrate heart development are limited in their ability to manipulate and assay the behavior of individual cells. As such, cardiac research currently lacks a simple experimental platform for real-time evaluation of cellular function under conditions that replicate native development. Here we report the design and validation of a rapid, low-cost system for stable in vivo somatic transgenesis that allows for individual cells to be genetically manipulated, tracked, and examined at subcellular resolution within the forming four-chambered heart. This experimental platform has several advantages over current technologies, chief among these being that mosaic cellular perturbations can be conducted without globally altering cardiac function. Consequently, direct analysis of cellular behavior can be interrogated in the absence of the organ level adaptions that often confound data interpretation in germline transgenic model organisms.

摘要

心脏细胞在一个精细的电-机械合胞体中发育,该合胞体不断产生并对生物物理力做出反应。正在形成的心脏中的细胞相互作用、血液动力学压力和电路的复杂性,对心肌细胞成熟的细胞动力学的机械研究提出了重大挑战。简单地说,在有利于高分辨率细胞/亚细胞分析的组织培养系统中复制天然的电-机械心脏微环境是非常困难的,并且高等脊椎动物心脏发育的现有转基因模型在操纵和检测单个细胞的行为方面能力有限。因此,心脏研究目前缺乏一个简单的实验平台,无法在复制天然发育的条件下实时评估细胞功能。在这里,我们报告了一种快速、低成本的体内稳定体转基因系统的设计和验证,该系统允许在正在形成的四腔心脏内以亚细胞分辨率对单个细胞进行遗传操作、跟踪和检查。与现有技术相比,该实验平台具有几个优势,其中最重要的是可以进行镶嵌细胞扰动,而不会全局改变心脏功能。因此,可以在没有经常使生殖系转基因模型生物中的数据解释复杂化的器官水平适应的情况下直接分析细胞行为。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b9bc/6656758/5307a7199e4a/41598_2019_47009_Fig1_HTML.jpg

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