Discovery Of Cell's 'Quality Control' Mechanism May Lead To New Treatments For Cystic Fibrosis, Other Inherited Diseases

Main Category: Cystic Fibrosis
Also Included In: Genetics;  Biology / Biochemistry
Article Date: 30 Jul 2008 - 4:00 PDT

email icon email to a friend   printer icon printer friendly   write icon opinions  

Current Article Ratings:

Patient / Public:not yet rated

Healthcare Prof:not yet rated


Researchers in Japan and Canada have discovered a key component of the quality control mechanism that operates inside human cells - sometimes too well. The breakthrough has significant implications for the development of new treatments for cystic fibrosis (CF) and some other hereditary diseases, the researchers say. Their results were published July 25 in the journal Science.

Dr. Kazahiro Nagata and colleagues at Kyoto University and the Japan Science Technology Agency, and Dr. David Thomas and Dr. Gregor Jansen at McGill University in Montreal, have discovered the important role played by an enzyme called ERdj5 inside the cell's endoplasmic reticulum (ER). The ER acts as a sort of packaging plant that folds and prepares proteins for distribution inside or outside the cell. But when proteins are misfolded in the ER, they must be destroyed in a degradation process - and that is where ERdj5 comes into play.

"ERdj5 is like a quality control inspector," explained Dr. Thomas, McGill's Chair of Biochemistry and Canada Research Chair in Molecular Genetics. "If you ever owned an AMC Pacer and you now drive a BMW, you know the difference quality control can make. That's what ERdj5 does, it recognizes when a protein has 'manufacturing defects' and degrades it before it can be distributed."

The ERdj5 enzyme is the first protein found to be capable of breaking the disulfide bonds that hold the misfolded proteins together in the ER. Once those bonds are broken, the researchers say ERdj5 also helps other enzymes and molecules break down the misfolded proteins completely so that the constituent amino acids can be recycled for further protein synthesis.

"Unfortunately, the mechanism sometimes works a little too well," Dr. Thomas said. "It insists on BMW quality when a Honda would do. For example, some people carry a mutated version of the protein CFTR. The mutated protein is damaged but would still work fine if it were distributed, but in some individuals, the quality control mechanism insists on degrading it. It's the degradation of the protein, not the mutation itself, which causes cystic fibrosis. We're hoping this discovery will open up new avenues of research into treatments for CF."

###

This release is available in French.

With contributions courtesy of Science Magazine.

Source: Mark Shainblum
McGill University

Article adapted by Medical News Today from original press release.
Visit our cystic fibrosis section for the latest news on this subject.
There are no references listed for this article.
Please use one of the following formats to cite this article in your essay, paper or report:

MLA
Mark Shainblum. "Discovery Of Cell's 'Quality Control' Mechanism May Lead To New Treatments For Cystic Fibrosis, Other Inherited Diseases." Medical News Today. MediLexicon, Intl., 30 Jul. 2008. Web.
14 Feb. 2012. <http://www.medicalnewstoday.com/releases/116623.php>
APA
Mark Shainblum. (2008, July 30). "Discovery Of Cell's 'Quality Control' Mechanism May Lead To New Treatments For Cystic Fibrosis, Other Inherited Diseases." Medical News Today. Retrieved from
http://www.medicalnewstoday.com/releases/116623.php.

Please note: If no author information is provided, the source is cited instead.


Cystic Fibrosis

Most Popular Articles



Follow Our Cystic Fibrosis News On Twitter

Follow Us On Twitter
Get the latest news for this category delivered straight to your Twitter account. Simply visit our Cystic Fibrosis Twitter account and select the 'follow' option.



View list of all 'What Is...' articles »