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From:http://scienceblogs.com/seed/2007/06/seven_new_wonders_1.php
Category: Announcement • ScienceBlogs • Things We Like
Posted on: June 23, 2007 9:43 AM, by Virginia Hughes
你能列举出古代的世界七大奇迹么?
我也做不到。不过为了加深你的印象,它们分别是(按照兴建时间顺序):
The Great Pyramids of Giza, 吉札金字塔
The Hanging Gardens of Babylon, 巴比伦空中花园
The Temple of Artemis at Ephesus, 阿提密斯神殿
The Statue of Zeus at Olympia, 宙斯神像
The Mausoleum of Maussollos at Halicarnassus, 毛索洛斯墓庙
The Colossus of Rhodes, and the Lighthouse of
上面这个著名的列表是由由拜占庭的菲伦于公元前200年所做,现在是不是到了一个可以更新的时候了?
New7Wonders 基金会是这么想的。2001年,加拿大籍瑞士人伯纳德.韦伯(Bernard Weber)创建了一个网站,访问者可以投票选举新七大奇迹,其中包括柬埔寨的吴哥窟(Angkor Wat in Cambodia)、埃菲尔铁塔(the Eiffel Tower in Paris)和悉尼歌剧院(the Sydney Opera House)。伯纳德.韦伯是电影制片人、博物馆馆长、飞行家和探险家。
尽快投下你的一票---在线投票、电话投票和短信投票将于格林尼治时间7月6日午夜中止。
相关资料: Britannica Blog
From:http://eternalremont.blogspot.com/
The current administration in Poland has given an opportunity for the biting humor of the communist era to return. Here is an email forward concerning the infamous teletubby scandal.
Subtext: This is the only way any sort of controversial programming can make it on TV.

Daniel Goldstein (Credit: Hebrew University photo by Sasson Tiram)
Science Daily — A novel method of drug delivery to inhibit the growth of prostate cancer cells has been developed by a doctoral candidate in pharmacy at the Hebrew University of Jerusalem.
These findings were published in the June 8 issue of Molecular Cell by Dr. Hao Wu, a professor in the Department of Biochemistry of Weill Cornell, and her team.
Experts know that cancers spread in two separate ways — by the uncontrolled proliferation of cells, and by their refusal to undergo normal, healthy, programmed cell death, or "apoptosis."
In many cancers, dysfunction in a biochemical cascade called the NF-kappa B pathway causes tumor cells to sidestep apoptosis and become dangerously immortal.
"So, drug development aimed at short-circuiting NF-kappa B has become very hot in the past few years," Dr. Wu says.
Her team focused on a particular protein involved in the NF-kappa B pathway called the "X-linked inhibitor of apoptosis" (XIAP). Scientists had already discovered that XIAP thwarts the apoptotic impulse by putting the brakes on key enzymes called caspases. XIAP is also known to be highly active in cancer cells, but it is found in relatively low levels in healthy cells. How XIAP inhibits caspases is known, but how XIAP induces NF-kappa B activation is entirely unclear.
"We wondered if we could find out how XIAP induces the NF-kappa B pathway," explains lead researcher Dr. Miao Lu, a postdoctoral fellow of biochemistry at Weill Cornell.
In their experiments, the researchers used a variety of cutting-edge techniques, including X-ray crystallography, to track changes in the structure and activity of XIAP and the molecules it interacts with in cells.
"We discovered that XIAP interacts with the NF-kappa B cycle in two distinct ways," Dr. Wu says.
"It interacts with another key protein, called TAB1, and it also interacts on a structural level with itself — a process called dimerization," the researcher explains.
Since both of these two activities might be vulnerable to some kind of pharmaceutical interference or interruption, they present promising new targets for the development of anti-cancer drugs.
"This is really exciting," says Dr. Wu, "because it provides two new points of attack against cancer in a pathway that pharmacological researchers are already very familiar with. It's exactly this type of basic science discoveries that we hope — one day — will help lead to a cure."
This work was funded by the U.S. National Institutes of Health.
Co-researchers include Dr. Yu-Chih Lo, Su-Chan Lin and Yihua Huang — all of Weill Cornell Medical College; Dr. Young Jun Kang and Dr. Jiahuai Han, of The Scripps Research Institute, La Jolla, Calif; and Dr. David Myszka and Rebecca Rich of the University of Utah, Salt Lake City.
Note: This story has been adapted from a news release issued by Weill Cornell Medical College.


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