麻豆淫院

May 19, 2010

Biologists Unravel Mechanisms of How Immune Cells Move (w/ Video)

(麻豆淫院Org.com) -- Human white blood cells navigate to and destroy bacteria by following a chemical that bacteria secrete. But less well understood are the biochemical processes within these immune cells that allow them to speed their way to bacteria and the sites of wounds and infections, often causing inflammation.

Now a team of biologists from the University of California, San Diego, led by Richard Firtel, a professor of biology at UCSD, has uncovered a major piece of the puzzle. In the May 18 issue of the journal Developmental Cell, the UCSD scientists report that they discovered a previously unknown complex of proteins that guides amoebae and mammalian immune cells toward their prey.

The team鈥檚 discoveries were made in Dictyostelium, a simple social amoeba and model genetic system that exhibits many of the properties of human . This amoeba is controlled by the same navigation system as mammalian , but has a much simpler genetic system and can be grown more easily and rapidly in a laboratory than mammalian cells.

Video of moving cells.

Working in collaboration with UCSD biology professor Steven Briggs and Zhouxin Shen, a senior scientist in Briggs鈥 laboratory, Pascale Charest, a postdoctoral fellow in Firtel鈥檚 UCSD laboratory and the first author of the paper, discovered a large multi-protein complex, called the 鈥淪ca1 complex,鈥 and found that it controlled the action of another protein called 鈥淩as,鈥 known to be important in directing a cell鈥檚 movements.

Ras connects the cell鈥檚 direction-sensing compass to its molecular motors, which allows the cell to move toward its targeted prey by making actin in the parts of the cell closest to the food and then taking the actin away from the other ends of the cell. The Sca1 complex acts as a navigator, activating Ras only at the correct spot along the cell鈥檚 surface and thus defining the direction of cell movement.

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This constant extension and contraction of the cell鈥檚 contents, which occurs over a period of about two minutes, is controlled by Ras and the Sca1 complex, and by another complex of proteins called TORC2, for Target of Rapamycin Complex 2, which helps in the chemical navigation system of the amoeba.

The UCSD biologists found that TORC2 inhibits the actions of the Sca1 complex and Ras in a way that allows the cells to regulate their own molecular motors, damping down their activity like a thermostat that shuts off the furnace when the room temperature gets too high or letting the activity continue.

鈥淲e knew before that Ras and these other components were at the front of the cell, but we had no idea how they got there and how they were turned on,鈥 said Firtel.

鈥淲e now have a better understanding of how white blood cells find their way to an infection,鈥 he added. 鈥淎nd we now know that these cells move in a highly regulated way. The discovery that Pascale made is more than just another cog in the wheel of understanding how these cells move. She鈥檚 found a novel underlying mechanism.鈥

The new findings not only improve our understanding of how and amoebae move, they are likely to guide the development of new drugs that control inflammation and limit the spread of tumors within the body caused during metastasis, when cancer cells use the same internal compass to home in on blood vessels and spread.

鈥淜nowing all of the players and how everything works in cell movement, we can now offer drug companies more biochemical targets to reduce inflammation and metastasis,鈥 said Charest.

鈥淲ith these discoveries, we are now closer to understanding how white blood cells move to sites of infection,鈥 said Firtel. 鈥淎nd if we now understand the biochemical pathways at this level, we can intercede in a way that will allow us to control inflammation and the metastasis of cancer.鈥

The researchers added that how these protein complexes regulate one another to limit or enhance cell movements is critical in designing new drugs that can control , such as arthritis, or the metastasis of tumors.

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