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‘Good Cholesterol’ Structure Identified
Reported March 15, 2011
(Ivanhoe Newswire) –University of Cincinnati
researchers have determined the structure of human HDL cholesterol and
believe the finding could help explain how it protects against
cardiovascular disease, including heart attack and stroke.
HDL (high-density lipoproteins) also known as "good cholesterol," are
packets of protein and fat that deliver fat to specific locations within the
body. There is an increasing effort to create drugs that help to raise
levels of HDL working in conjunction with existing drugs that lower "bad
cholesterol," or low-density lipoproteins (LDL).
Studies of synthetically derived HDL have shown that an abundant protein in
HDL, apolipoprotein A-I, plays a key role in HDL's cardioprotective
anti-inflammatory and anti-oxidative properties.
"Unfortunately, we've known very little about the molecular details that
explain HDL's protective effects," W. Sean Davidson, PhD, professor in UC's
pathology and laboratory medicine department, and lead author of ths study
was quoted as saying.
"A major reason for this is an almost complete lack of understanding of
HDL's structure and how it interacts with other important plasma factors."
Rong Huang, PhD, a post-doctoral fellow in Davidson's laboratory, has
isolated human HDL and analyzed its 3-D structure as it circulates in human
plasma.
"Previous studies have only focused on synthetic HDL made in the test tube,"
Davidson said. "By isolating human HDL, we were able to focus on the broad
range of HDL particles actually circulating in humans."
Researchers found that proteins of HDL form a cage-like structure that
encapsulates its fatty cargo. They determined that most of the HDL particles
circulating in human plasma are similar in structure; however, they found
evidence that the particles have a twisting or shock absorber-like motion
that allows them to adapt to changes in particle fat content.
By determining the structure of HDL, Davidson and his team were able to
conclude that the majority of physiological interactions occurring with HDL—including
its twisting movements—occur at the particle surface, which is dominated by
the cardioprotective protein apolipoprotein A-I.
This monopolization of the particle surface suggests that other proteins
have very little room to bind to HDL and probably have to interact with the
protein itself, which could explain how apolipoprotein A-I plays such a
dominant role in HDL function and its protective effects.
"This work presents the first detailed models of human plasma HDL and has
important implications for understanding key interactions in plasma that
modulate its protective functions in the context of cardiovascular disease,"
Davidson said.
SOURCE: Nature Structural & Molecular Biology, published online March 13,
2011
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