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Scientists Cite Fastest Case of Human Evolution

Tuesday, July 6th, 2010

human evolution 300x193 Scientists Cite Fastest Case of Human EvolutionTibetans live at altitudes of 13,000 feet, breathing air that has 40 percent less oxygen than is available at sea level, yet suffer very little mountain sickness.

The reason, according to a team of biologists in China, is human evolution, in what may be the most recent and fastest instance detected so far. Comparing the genomes of Tibetans and Han Chinese, the majority ethnic group in China, the biologists found that at least 30 genes had undergone evolutionary change in the Tibetans as they adapted to life on the high plateau. Tibetans and Han Chinese split apart as recently as 3,000 years ago, say the biologists, a group at the Beijing Genomics Institute led by Xin Yi and Jian Wang. The report appears in Friday’s issue of Science.

If confirmed, this would be the most recent known example of human evolutionary change. Until now, the most recent such change was the spread of lactose tolerance — the ability to digest milk in adulthood — among northern Europeans about 7,500 years ago. But archaeologists say that the Tibetan plateau was inhabited much earlier than 3,000 years ago and that the geneticists’ date is incorrect.

When lowlanders try to live at high altitudes, their blood thickens as the body tries to counteract the low oxygen levels by churning out more red blood cells. This overproduction of red blood cells leads to chronic mountain sickness and to lesser fertility — Han Chinese living in Tibet have three times the infant mortality of Tibetans.

The Beijing team analyzed the 3 percent of the human genome in which known genes lie in 50 Tibetans from two villages at an altitude of 14,000 feet and in 40 Han Chinese from Beijing, which is 160 feet above sea level. Many genes exist in a population in alternative versions. The biologists found about 30 genes in which a version rare among the Han had become common among the Tibetans. The most striking instance was a version of a gene possessed by 9 percent of Han but 87 percent of Tibetans.

[NYTimes]

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More Evidence of Intelligent Design Shot Down by Science

Thursday, December 10th, 2009

Intricate cellular components are often cited as evidence of intelligent design. They couldn’t have evolved, I.D. proponents say, because they can’t be broken down into smaller, simpler functional parts. They are irreducibly complex, so they must have been intentionally designed, as is, by an intelligent entity.

But new research comparing mitochondria, which provide energy to animal cells, with their bacterial relatives, shows that the necessary pieces for one particular cellular machine — exactly the sort of structure that’s supposed to prove intelligent design — were lying around long ago. It was simply a matter of time before they came together into a more complex entity.

tim23 500x283 More Evidence of Intelligent Design Shot Down by Science

The pieces “were involved in some other, different function. They were recruited and acquired a new function,” said Sebastian Poggio, a postdoctoral cell biologist at Yale University and co-author of the study published Monday in the Proceedings of the National Academy of Sciences.

Mitochondria are descended from free-living bacteria, which several billion years ago were swallowed by complex cells. The mitochondria soon became central to the cells’ function.

Mitochondria couldn’t have lasted in their new home without the help of a protein machine called TIM23, which delivers other proteins harvested from the cell’s body. Bacteria don’t possess TIM23, suggesting that it evolved in mitochondria. This seems to pose a cellular chicken-and-egg question: How could protein transport evolve when it was necessary to survive in the first place?

The essential paradox applies to other protein-transporting cell systems, providing disbelievers of evolution with a key part of their critique. As articulated by intelligent design proponent Michael Behe, “This constant, regulated traffic flow in the cell comprises another remarkably complex, irreducible system. All parts must function or the system breaks down.”

According to evolutionary theory, however, cellular complexity is reducible. It requires only that existing components be repurposed, with inevitable mutations providing extra ingredients as needed. Flagella, the hairlike propellers used by bacteria to move, are one example of this. Their component parts are found throughout cells, performing other tasks.

Intelligent design mavens once cited flagella as evidence of their theory. Scientific fact dispelled that illusion. The mitochondria study does the same for protein transport.

“This analysis of protein transport provides a blueprint for the evolution of cellular machinery in general,” write the researchers, led by molecular biologist Trevor Lithgow at Australia’s Monash University. “The complexity of these machines is not irreducible.”

When they analyzed the genomes of proteobacteria, the family that spawned the ancestors of mitochondria, Lithgow’s team found two of the protein parts used in mitochondria to make TIM23.

The parts are located on bacterial cell membranes, making them ideally positioned for TIM23’s eventual protein-delivering role. Only one other part, a molecule called LivH, would make a rudimentary protein-transporting machine — and LivH is commonly found in proteobacteria.

The process by which parts accumulate until they’re ready to snap together is called preadaptation. It’s a form of “neutral evolution,” in which the buildup of the parts provides no immediate advantage or disadvantage. Neutral evolution falls outside the descriptions of Charles Darwin. But once the pieces gather, mutation and natural selection can take care of the rest, ultimately resulting in the now-complex form of TIM23.

“It hasn’t been possible up until this point to trace any of those proteins back to a bacterial ancestor,” said Dalhousie University cell biologist Michael Gray, one of the researchers who originally described the origins of mitochondria, but was not involved in the new study. “These three proteins don’t perform precisely the same function in proteobacteria, but with a simple mutation could be transformed into a simple protein transport machine that could start the whole thing off.”

“You look at cellular machines and say, why on earth would biology do anything like this? It’s too bizarre,” he said. “But when you think about it in a neutral evolutionary fashion, in which these machineries emerge before there’s a need for them, then it makes sense.”

Citation: “The reducible complexity of a mitochondrial molecular machine.” By Abigail Clements,1, Dejan Bursac, Xenia Gatsos, Andrew J. Perry, Srgjan Civciristova, Nermin Celik, Vladimir A. Likic, Sebastian Poggio, Christine Jacobs-Wagner, Richard A. Strugnell, and Trevor Lithgow. Proceedings of the National Academy of Sciences, Vol. 106 No. 33, August 25, 2009.

Image: Journal of Cell Science
Source: Brandon Keim

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Intelligent Design’s 8 Biggest Fails

Friday, December 4th, 2009

intelligent design poster Intelligent Designs 8 Biggest Fails
Over at Discover, they have a photo gallery of 8 ways Intelligent Design fails.

Among my favorites are:

  • How mitochondria evolved from a free-living bacteria into the power generator for human cells
  • Admission by an ID proponent that blood clotting is not “irreducibly complex”. (Irreducible complexity is one of ID’s key arguments, that because some things are so complex they required an intelligent designer to create).
  • Bacteria which have recently evolved (without intervention from man) to eat nylon
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How Christians and Atheists See the Other

Thursday, November 5th, 2009

Christians vs Atheists How Christians and Atheists See the Other

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