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NEWS
INDEX
Archives
2004
August
Molecular motor Myosin VI moves
'hand over hand,' researchers say
James
E. Kloeppel, Physical Sciences Editor
217-244-1073; kloeppel@uiuc.edu
8/30/04
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Click
photo to enlarge |
| Graphic
courtesy Paul Selvin |
| Myosin
VI (blue) is a molecular motor that walks "backwards"
on filaments of actin (red). By labeling a myosin VI on the
head (green), or on the neck (red), and localizing the dye
within a few nanometers, scientists determined that myosin
walks "hand-over-hand," while causing a part of
the protein to come undone. |
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CHAMPAIGN,
Ill. — In the human body, hundreds of different types of biomolecular
motors help carry out such essential tasks as muscle contraction, moving
chromosomes during cell division, and reloading nerve cells so they
can repeatedly fire.
How these little proteins perform their duties is becoming clearer to
scientists using an extremely sensitive measurement technique. Myosin
VI, they found, moves by the same “hand-over-hand” mechanism
as two other molecular motors, myosin V and kinesin.
“Now
that a third molecular motor has been found to move in the same hand-over-hand
fashion, the argument for a rival ‘inchworm’ motion is getting
pretty weak,” said Paul Selvin, a professor of physics
at the University of Illinois at Urbana-Champaign and a co-author of
a paper to appear in the Journal of Biological Chemistry.
 |
Click
photo to enlarge |
| Photo
by Kwame Ross |
| Physics
professor Paul Selvin has found another molecular motor that
uses the hand-over-hand model of movement. |
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Myosin
VI is a reverse-direction molecular motor that moves materials to various
locations within a living cell. Like the related protein myosin V, myosin
VI has two “arms” connected to a “body.” The
tiny molecule converts chemical energy into mechanical motion, and transports
its load by “stepping” along polarized filaments of actin
– but in the opposite direction from other myosin variants.
“Studies have suggested two main models for the stepping movement,”
Selvin said. “One is the hand-over-hand model in which the two
arms alternate in the lead. The other model is the inchworm model in
which one arm always leads.”
To examine the myosin VI stepping mechanism, the researchers applied
the same technique that was used to study both myosin V and kinesin.
Called FIONA – Fluorescence Imaging with One Nanometer Accuracy
– the measurement technique can track the position of a single
molecule to within 1.5 nanometers. (One nanometer is a billionth of
a meter, or about 10,000 times smaller than the width of a human hair).
 |
Click
photo to enlarge |
| Photo
by Kwame Ross |
| Selvin
excites molecules with a laser. |
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“First,
we attached a small fluorescent dye to one of the arms and took a picture
with a digital camera attached to a microscope to find exactly where
the dye was,” Selvin said. “Then we fed the myosin a little
food called adenosine triphosphate, and it took a step. We took another
picture, located the dye, and measured how far the dye moved.”
By examining the step size, the scientists could determine whether the
protein used a hand-over-hand mechanism or an inchworm mechanism for
movement. “The average step size for the myosin VI arm was approximately
60 nanometers, while the molecule’s center of mass moved only
half that distance,” Selvin said. “This clearly indicated
that a
hand-over-hand model was being employed.”
Surprisingly, myosin VI has a step size that is highly variable, but
on average is nearly as large as that of myosin V, which has a lever
arm that is three times longer.
“For myosin VI to reach the same distance, the molecule must somehow
come apart and then snap together again,” Selvin said. “To
understand how it accomplishes this feat will require further study.”
The co-authors of the paper are Selvin, Hyokeun Park and Ahmet Yildiz
at Illinois, and Li-Qiong Chen, Dan Safer, H. Lee Sweeney and Zhaohui
Yang at the University of Pennsylvania. The National Institutes of Health
funded the work.
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