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肝胆相照论坛 论坛 精华资料 存档 1 中国医药网 --美开发出杀死乙肝病毒的一种微型载体 ...
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中国医药网 --美开发出杀死乙肝病毒的一种微型载体 [复制链接]

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41
发表于 2005-4-27 23:01

按照美国人的规矩,从这个到临床试验至少5年,如果是上市,再加4-5年。

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42
发表于 2005-4-28 22:43

希望吧!

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发表于 2005-6-29 02:26

这个消息可信吗???

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发表于 2005-7-1 12:29

其实没有了歧视,我多等个几年也无妨,这才是关键。

——有感情没欲望就是朋友, 有感情有欲望就是情人—— QQ 419337610 [无锡]

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发表于 2005-7-18 10:32
建议应该成立注册性会员组织,建立基金会,专门来推动消灭乙肝的事业。

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荣誉之星 驴版 大财主勋章 郊游活动

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发表于 2005-7-20 05:06
  等得到那一天吗,真是急死人了,等 等  等到什么时候。
想找一个接近天堂与上帝的地方住下来

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发表于 2005-7-21 10:30
2004年的新闻啊!不知道现在进展如何?

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发表于 2005-7-23 02:49

什么时候用到临床上啊,小弟着急等着呢!顶!

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元帅勋章 功勋会员 小花 管理员或超版 荣誉之星 勤于助新 龙的传人 大财主勋章 白衣天使 旺旺勋章 心爱宝宝 携手同心 驴版 有声有色 东北版 美食大使 幸福四叶草 翡翠丝带 健康之翼 幸福风车 恭喜发财 人中之龙

49
发表于 2005-7-23 03:58

Tiny Ribozyme package could be future treatment of Hepatitis B virus

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Penn State College of Medicine researchers have developed a tiny package that searches for and destroys up to 80 percent of hepatitis B virus in the livers of mice.

"This marks one of the few successful in vivo, or in-animal, models of an effective therapy to reduce the production of hepatitis B virus," said Gary Clawson, M.D., Ph.D., professor of pathology, biochemistry and molecular biology, Penn State College of Medicine. "Although this work focused on hepatitis B virus, our method of targeting and packaging ribozymes should also be applicable to the development of therapies to fight other viruses."

The study was published March 5 in the online version of the journal, Molecular Therapy, the official journal of the American Society of Gene Therapy, and will appear in the journal's April print edition.

Hepatitis B virus (HBV) attacks the liver and can cause lifelong infection, liver cancer and, eventually, death. Although HBV is treated with drugs, it cannot be cured. The chronic disease affects about 1.25 million Americans, 20 percent to 30 percent of whom acquired the virus in childhood. HBV is transmitted via blood or sexual activity, but also may be transmitted from mother to child during childbirth. Once infected, the virus continues to reproduce in the liver.

Clawson, who is also director of the Jake Gittlen Cancer Research Center at Penn State Milton S. Hershey Medical Center, and his team developed the SNIPAA cassette, which contains a double-dose of a special type of ribozyme called a trans-acting hammerhead ribozyme. Ribozymes are ribonucleic acid (RNA) segments that, like enzymes, cause chemical changes or splitting in other RNA segments. RNA, which is critical to the replication of DNA - life's instruction book - also is critical to the replication of viruses. The SNIPAA cassette was packaged in liposomes, typical vehicles for delivering drugs in the body, and the liposomes in turn were modified with proteins so that they would seek out the liver cells where the HBVs replicate.

Once at the liver cell, the SNIPAA cassette package is released into the cell and finds its way to the cell nucleus, where the active ribozymes are produced. The ribozymes destroy the viral RNA's ability to produce proteins by cleaving, or cutting, the viral RNAs, rendering them useless. Proteins are critical to virus replication.

First, Clawson and co-workers used proprietary in vitro selection techniques to identify the best target sites in HBV RNA, and then used cells in culture to test the effectiveness of the cassette. In the cell cultures, he found that the SNIPAA cassette containing a double-dose of ribozymes eliminated more of the virus over a period of three to five days than did cassettes containing a single dose of the ribozymes.

Specialized transgenic mice, which contain the HBV in their DNA and which are chronic carriers of HBV, were treated with the tiny HBV-fighting packages. Clawson and co-workers chose the dosage and schedule of the drug delivery to the mice based on their cell culture work. Studies with the transgenic mice were performed with John Morrey, Ph.D., at Utah State, under the auspices of an NIH contract which supports testing of antiviral reagents.

"The treatment effects were quite dramatic," Clawson said. "We recorded a greater than 80 percent reduction in the HBV liver DNA, meaning far less virus was being produced, and staining for the virus using antibodies also showed a dramatic decrease in residual viral production. This is significant because there are so few examples of successful in vivo applications of ribozymes against bona fide naturally-occurring, disease-causing organisms."

Clawson believes this cassette is more effective than previous ones for a number of reasons. First, the best target sites were chosen using a "library selection" process. Second, the ribozyme cassette is engineered to cut itself into pieces, thereby freeing the HBV-targeted ribozymes from extraneous sequences that could interfere with their activity. In addition, Clawson's cassette included two distinct trans-acting ribozymes, whereas previous versions included only one. With two trans-acting hammerhead ribozymes in the SNIPAA cassette, twice the amount of "medicine" was present and was delivered over a longer period.

Co-authors on the study were: Wei-Hua Pan, Pin Xin, Departments of Pathology and Biochemistry and Molecular Biology, The Gittlen Cancer Research Institute, Penn State Milton S. Hershey Medical Center, and John D. Morrey, Institute for Antiviral Research, Utah State University.

This work was supported by a research and development contract with Biosan Laboratories/Hexal AG and by a contract from the National Institutes of Health.

God Made Everything That Has Life. Rest Everything Is Made In China

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发表于 2005-7-28 13:53

顶一下

与天斗其乐无穷; 与地斗其乐无穷; 与己斗其乐无穷; 与她斗其乐无穷; 与乙肝斗更是其乐无穷; 阿德福韦学术与治疗用药 专业论坛群号 :7118578
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