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人工肝又近了一步 [复制链接]

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发表于 2013-6-7 17:17 |只看该作者 |倒序浏览 |打印
Artificial Livers A Step Closer


Article Date: 04 Jun 2013 - 1:00 PDT


Prometheus, the mythological figure who stole fire from the gods, was punished for this theft by being bound to a rock. Each day, an eagle swept down and fed on his liver, which then grew back to be eaten again the next day.

Modern scientists know there is a grain of truth to the tale, says MIT engineer Sangeeta Bhatia: The liver can indeed regenerate itself if part of it is removed. However, researchers trying to exploit that ability in hopes of producing artificial liver tissue for transplantation have repeatedly been stymied: Mature liver cells, known as hepatocytes, quickly lose their normal function when removed from the body.

"It's a paradox because we know liver cells are capable of growing, but somehow we can't get them to grow" outside the body, says Bhatia, the John and Dorothy Wilson Professor of Health Sciences and Technology and Electrical Engineering and Computer Science at MIT, a senior associate member of the Broad Institute and a member of MIT's Koch Institute for Integrative Cancer Research and Institute for Medical Engineering and Science.

Now, Bhatia and colleagues have taken a step toward that goal. In a paper appearing in the June 2 issue of Nature Chemical Biology, they have identified a dozen chemical compounds that can help liver cells not only maintain their normal function while grown in a lab dish, but also multiply to produce new tissue.

Cells grown this way could help researchers develop engineered tissue to treat many of the 500 million people suffering from chronic liver diseases such as hepatitis C, according to the researchers.

Lead author of the paper is Jing (Meghan) Shan, a graduate student in the Harvard-MIT Division of Health Sciences and Technology. Members of Bhatia's lab collaborated with researchers from the Broad Institute, Harvard Medical School and the University of Wisconsin.

Large-scale screen

Bhatia has previously developed a way to temporarily maintain normal liver-cell function after those cells are removed from the body, by precisely intermingling them with mouse fibroblast cells. For this study, funded by the National Institutes of Health and Howard Hughes Medical Institute, the research team adapted the system so that the liver cells could grow, in layers with the fibroblast cells, in small depressions in a lab dish. This allowed the researchers to perform large-scale, rapid studies of how 12,500 different chemicals affect liver-cell growth and function.

The liver has about 500 functions, divided into four general categories: drug detoxification, energy metabolism, protein synthesis and bile production. David Thomas, an associate researcher working with Todd Golub at the Broad Institute, measured expression levels of 83 liver enzymes representing some of the most finicky functions to maintain.

After screening thousands of liver cells from eight different tissue donors, the researchers identified 12 compounds that helped the cells maintain those functions, promoted liver cell division, or both.

Two of those compounds seemed to work especially well in cells from younger donors, so the researchers - including Robert Schwartz, an IMES postdoc, and Stephen Duncan, a professor of human and molecular genetics at the University of Wisconsin - also tested them in liver cells generated from induced pluripotent stem cells (iPSCs). Scientists have tried to create hepatocytes from iPSCs before, but such cells don't usually reach a fully mature state. However, when treated with those two compounds, the cells matured more completely.

Bhatia and her team wonder whether these compounds might launch a universal maturation program that could influence other types of cells as well. Other researchers are now testing them in a variety of cell types generated from iPSCs.

In future studies, the MIT team plans to embed the treated liver cells on polymer tissue scaffolds and implant them in mice, to test whether they could be used as replacement liver tissues. They are also pursuing the possibility of developing the compounds as drugs to help regenerate patients' own liver tissues, working with Trista North and Wolfram Goessling of Harvard Medical School.

Making connections

Bhatia and colleagues have also recently made progress toward solving another challenge of engineering liver tissue, which is getting the recipient's body to grow blood vessels to supply the new tissue with oxygen and nutrients. In a paper published in the Proceedings of the National Academy of Sciences in April, Bhatia and Christopher Chen, a professor at the University of Pennsylvania, showed that if preformed cords of endothelial cells are embedded into the tissue, they will rapidly grow into arrays of blood vessels after the tissue is implanted.

To achieve this, Kelly Stevens in the Bhatia lab worked with Peter Zandstra at the University of Toronto to design a new system that allows them to create 3-D engineered tissue and precisely control the placement of different cell types within the tissue. This approach, described recently in the journal Nature Communications, allows the engineered tissue to function better with the host tissue.

"Together, these papers offer a path forward to solve two of the longstanding challenges in liver tissue engineering - growing a large supply of liver cells outside the body and getting the tissues to graft to the transplant recipient," Bhatia says.

http://www.medicalnewstoday.com/releases/261356.php

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发表于 2013-6-7 17:18 |只看该作者
文章日期:2013年6月4日 -  1:00 PDT


谁偷火从神的神话人物,普罗米修斯,这个盗窃被处罚,被绑定到一块岩石。每一天,老鹰横扫下来,喂养他的肝脏,然后长大回来第二天再次被吃掉。

现代科学家知道的故事是有一定道理的,麻省理工学院的工程师Sangeeta巴蒂亚说:肝脏确实可以再生,如果它的一部分被删除。然而,研究人员试图利用这种能力,希望生产用于移植的人造肝脏组织曾多次受到阻碍:成熟的肝细胞,称为肝细胞,迅速从体内取出时失去其正常功能。

“这是一个悖论,因为我们知道肝细胞能够生长,但不知何故,我们不能让他们成长”以外的身体,巴蒂亚说,约翰和多萝西·威尔逊教授健康科学与技术,电气工程与计算机科学麻省理工学院Broad研究所和麻省理工学院的科赫综合癌症研究所和医学工程与科学研究所研究所成员的高级公会会员。

现在,巴蒂亚和他的同事们已经朝着这个目标迈出了一步。在一份文件中出现在6月2日发行的“自然化学生物学,他们已经确定了十几个化学化合物,可以帮助肝细胞不仅能维持其正常功能,而在实验室的培养皿中生长,但也繁殖产生新的组织。

这种方式可以帮助研究人员开发设计,组织500万人患有慢性肝脏疾病,如丙型肝炎治疗许多细胞生长,根据研究人员。

铅的论文的作者是静(梅根)山,哈佛 - 麻省理工学院卫生科学与技术部的研究生。巴蒂亚的实验室成员与Broad研究所,哈佛医学院和美国威斯康星大学的研究人员合作。

大型屏幕

巴蒂亚先前已开发了一种方法,通过精确地交织与小鼠成纤维细胞后,这些细胞从人体取出的暂时维持正常的肝细胞功能。在这项研究中,由美国国立卫生和霍华德休斯医学研究所资助,研究小组调整系统,使肝细胞生长层的成纤维细胞,在实验室的培养皿中的小洼地。这使研究人员能够进行大规模,快速的12500种不同的化学物质如何影响肝细胞的生长和功能的研究。

肝脏有大约500个功能分为四大类:清热解毒药,能量代谢,蛋白质合成和胆汁分泌。大卫·托马斯,副研究员与托德戈卢布工作在Broad研究院,代表的一些最挑剔的功能保持的83例肝酶的表达水平。

从8个不同的组织捐献者中筛选成千上万的肝细胞后,研究人员确定了12个化合物,帮助细胞维持这些功能,促进肝细胞的分裂,或两者兼而有之。

这些化合物似乎工作,特别是在年轻的捐助者,因此研究人员 - 包括罗伯特·施瓦茨,IMES博士后,美国威斯康星大学的人类遗传学和分子遗传学教授斯蒂芬·邓肯,细胞 - 他们还测试了在肝细胞产生的诱导性多能干细胞(iPS细胞)。科学家们试图建立肝从iPS细胞前,但这些细胞通常不会达到完全成熟的状态。然而,当用这两种化合物时,细胞完全成熟。

巴蒂亚和她的团队不知道这些化合物是否可能推出一个普遍的成熟程序,可能影响,以及其他类型的细胞。其他研究人员正在测试他们在不同类型的细胞产生的iPS细胞。

在今后的研究中,MIT的研究小组计划,嵌入聚合物组织支架和处理的肝细胞植入小鼠,测试它们是否可以作为替代肝脏组织。他们也追求药物到帮助重生患者的自己的肝脏组织开发的化合物的可能性与哈佛医学院北伶和Wolfram Goessling的工作。

连接

巴蒂亚和他的同事最近也取得了进展,对解决工程肝组织,这是越来越收件人的身体成长提供新的组织与氧气和营养物质的血管另一个挑战。在诉讼中的国家科学院发表的一篇论文,在4月,巴蒂亚在美国宾夕法尼亚大学教授,克里斯托弗·陈,显示,预制线嵌入到组织的内皮细胞,他们会迅速成长为阵列植入后的组织中的血管。

为了实现这一目标,凯利·史蒂文斯曾在多伦多大学的彼得Zandstra巴蒂亚实验室设计一个新的系统,使他们能够创建3-D的组织工程和精确控制放置不同类型的细胞组织内。这种做法,最近在Nature杂志上的通信,允许组织工程与宿主组织更好地发挥作用。

“总之,这些文件提供了一条前进的道路,以解决两个在肝组织工程的长期挑战 - 肝细胞生长大量供应外体组织移植到移植,”巴蒂亚说。

http://www.medicalnewstoday.com/releases/261356.ph​​p
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发表于 2013-6-9 23:42 |只看该作者
这些个基础研究还早呢,不如踏踏实实的吃合理,休息合理,多锻炼身体,现在人工肝都是在骗人的,尤其是国内,一次一万多块钱,赚死人钱。
qq:霸气一三私企二五

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发表于 2013-6-12 16:02 |只看该作者
感谢分享
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