Researchers find how newborn neurons replace dying cells

US scientists discovered in a new study how new neurons born from endogenous neural stem cells are sent to regions of the brain where they can replace old and dying cells.
This finding, suggesting how stem cell therapies can be specifically targeted to brain regions affected by neurodegenerative diseases like Alzheimer’s and Parkinson’s, or by stroke, is published in the June 24 issue of the journal Science.

Qun-Yong Zhou, an associate professor at University of California, Irvine, and his graduate student Kwan L. Ng identified a protein that guides these new neurons to a particular brain region.

The protein, a small peptide called prokineticin 2 (PK2), was found to play a key regulatory role for the proper functional integration of these new neurons in the brain. A few years ago, PK2 was shown by the same research group to be an important regulator of circadian rhythms.

“One of the keys to developing promising new therapies for debilitating neurodegenerative diseases lies in our understanding of how new neurons are created and integrated into mature brain tissue,” Zhou said.

“In this process, it’s very crucial how the newborn neurons are guided to move toward their right sites. And that’s what our study has shown,” he said. The PK2 protein is an attractive drug target for either boosting neuron-forming processes or stem cell- based therapies.

While all neurons are originally born and differentiated from their stem cell progenitors during development, the adult brain maintains at least some regions where neural stem cells create new neurons to replace old and dying ones. One area is the subventricular zone of the lateral ventricles, which are fluid- filled cavities in both brain hemispheres connected the central canal of the spinal cord.

Zhou and his colleagues discovered how PK2 guides the migration of neurons born from neural stem cells from the subventricular zone in the brain’s core through mature tissue to reach the olfactory bulb, the part of the brain responsible for smell located above the sinus cavity. PK2 allows these new neurons to settle into the proper areas of the olfactory bulb, thus permitting these neurons to function normally.

“Our findings identify one of the first endogenous guidance molecules for migrating neurons in the adult brain,” Zhou said.

PK2 accomplishes this task by working with its corresponding cell receptors, which are part of the G protein-coupled receptor ( GPCR) family. GPCRs are proteins found in a cell’s membrane and play a critical role in transferring signals from outside of a cell to the molecular machinery within the cell. GPCRs are the largest family of proteins that serve as drug targets. It has been estimated that at least 40 percent of all medicines on the market act on this family of receptors.

http://www.biotechonline.net/?p=27



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