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MEDIA CONTACT: Elizabeth Crown at (312) 503-8928 or e-mail
at e-crown@northwestern.edu
June 3, 2002
Fighting Disease on the Cellular Level
“All disease results from
failed mechanisms within cells. Analyzing the workings
of healthy cells will lead to development of targeted
therapies, improved methods for facilitating wound healing,
development of artificial tissues and a better understanding
of the potential uses of human stem cells.” —
Robert D. Goldman, chairman |
Contrary to those static diagrams of a cell you may remember
from high school biology, a eukaryotic cell (cell with a nucleus)
is actually a dynamic and intricately ordered living creature,
complete with its own set of tiny "organs" and empowered
by thousands of chemical mechanisms that enable the cell to
digest, reproduce, move and communicate with other cells.
The remarkably complex anatomy of all eukaryotic cells and
many of their basic molecular mechanisms are strikingly uniform
in the 60 trillion cells comprising the human body. Cell biologists
relate these features to cellular functions by determining
the molecular mechanisms responsible for fundamental processes
ranging from cell division and protein transport to signal
transduction and the migratory behavior of cells underlying
tissue formation during embryonic development and wound healing.
It follows that an understanding of normal cells paves the
way for a greater comprehension of a variety of human diseases,
says Robert D. Goldman, Stephen Walter Ranson Professor and
chair of cell and molecular biology at The Feinberg School
of Medicine.
"All disease results from failed mechanisms within
cells. Analyzing the workings of healthy cells will lead to
development of targeted therapies, improved methods for facilitating
wound healing, development of artificial tissues and a better
understanding of the potential uses of human stem cells,"
he said.
LEFT TO RIGHT: Robert Goldman,
Gary Borisy, James Bartles, Edwin Taylor and Rex Chisolm.
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Goldman is a highly regarded authority on the structure and
function of the cytoskeleton. His other passion in science
lies in the area of the public’s understanding of science
and technology. With Boyce Rensberger, award-winning former
science editor of the Washington Post, he directs the Science
Writers Fellowship Program at the Marine Biological Laboratory
in Woods Hole, Mass., which offers journalists the opportunity
to gain hands-on experience with the laboratory techniques
used by biomedical researchers.
In his 20 years as chair, Goldman has overseen the development
of a department that now ranks in the top 10 of its peer departments
in 126 U.S. medical schools (American Association of Medical
Colleges data). This year, CMB faculty were awarded approximately
$10 million in grant funding from the National Science Foundation
and the National Institutes of Health, including several MERIT
awards and Program Project Grants (PPGs).
LEFT TO RIGHT: Alzheimer's researchers
Robert Berry, Adrianna Ferreira, Robert Vassar and Skip
Binder. Binder and NUIN researcher Ferreira recently collaborated
on an important study on Alzheimer's-associated neurodegeneration.
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The department is home to a number of scientists whose body
of research has been honored both nationally and internationally.
Laszlo Lorand and Edwin Taylor are members of the National
Academy of Sciences and the American Academy of Arts and Sciences.
Lorand, who joined Northwest-ern in 1955, is one of the
world’s leading experts on blood clotting mechanisms.
Taylor, widely acknowledged as one of the "fathers of
cytoskeletal research," received the E. B. Wilson Medal,
the highest honor awarded by the American Society for Cell
Biology. He also is a member of the Royal Society of London.
Three researchers, including Goldman, currently have prestigious
MERIT (Method to Extend Research in Time) awards from the
NIH for outstanding records of scientific achievements. The
other recipients are Lester I. (Skip) Binder and Linda Van
Eldik for their work on Alzheimer’s disease. Previous
MERIT award recipients in the department include Lorand, Arthur
Veis and Gary Borisy, Leslie B. Arey Professor of Cell, Molecular
and Anatomical Sciences. Borisy is currently the president
of the American Society for Cell Biology.
LEFT TO RIGHT: Sui Huang, Stephen
Adam and Carolyn Jahn are members of the group that studies
molecular mechanisms and the nucleus. |
Department researchers employ a broad range of technological
methods, including biochemical, biophysical and immunological
approaches, as well as digital and confocal microscopy, video-enhanced
light microscopy and molecular biological and genetic manipulation
of function at both the cellular and organismal level.
For this article, the work of these investigators is described
by areas of research: cytoskeleton; cell surface/extracellular
matrix; molecular mechanisms and the nucleus; and the cellular
basis of disease, emphasizing Alzheimer’s disease. (The
department also includes a group of physical anthropologists
who were featured in an earlier OBSERVER article.)
The cytoskeletal group studies one or more of the three
major "scaffolding" components of mammalian cells,
including actin, microtubules and intermediate filaments.
The pioneering research of Gunther Albrecht-Buehler, Robert
Laughlin Rea Professor of Cell and Molecular Biology, attempts
to integrate all of the cells’ cytoskeletal and molecular
activities that are responsible for regulating cellular behavior
patterns. His work on the role of the centrosome, a structure
located near the nucleus and the microtubule organizing center
of the cell, suggests that the centrosome is the "brain,"
or unifying system, that controls cell motility.
The Borisy lab is internationally recognized for groundbreaking
studies of the function and organization of microtubules,
filamentous structures that course through the cell and act
as "tracks" on which protein complexes called "molecular
motors" use energy to move other "molecular cargo"
from one part of the cell to another. Borisy’s group
also studies the organization and dynamics of actin which,
in addition to a multitude of its other duties, is essential
to processes involved in cell migration and, hence, embryonic
development.
CLOCKWISE FROM BOTTOM RIGHT:
Lazslo Lorand, Arthur Veis, Jonathan Jones, Sharon Stack
and James Kramer, whose research interests center on the
cell surface/extracellular matrix. |
James Bartles investigates the role of espin, a cytoskeletal
protein he discovered, which is present throughout the nervous
system and is a key structural component of the stereocilia
of hair cells, the apparatus in the inner ear that detects
sound and motion and helps control balance in the body. His
research showed that a defect in the espin gene causes abnormal
behavior in mice (the animals appear to dance) and also renders
them deaf. For this work, Bartles recently received a five-year
grant from the National Institute on Deafness and Other Communication
Disorders of the NIH.
Rex Chisholm, who also is the director of the Center for
Genetic Medicine, studies the myosins, a class of molecular
motors that interact with actin to power cell motility and
facilitate a wide range of processes ranging from intracellular
transport to cardiac and skeletal muscle contraction. Myosin
motors have been linked to numerous human diseases, including
hypertrophic cardiomyopathy, the leading cause of sudden death
in otherwise healthy adults. Because of this research, the
Chisholm lab has become a training ground for fellows in cardiovascular
surgery.
Yoshio Fukui’s studies, which employ high-resolution
light microscopic methods including digital fluorescence microscopy,
emphasize the remarkably dynamic activities of the various
cytoskeletal systems and their related proteins in living
cells.
Although it had been commonly believed that the intermediate
filament (IF) system serves literally only a supportive role
in terms of maintaining the structure of the cell, Goldman’s
research over the past 15 years has indicated otherwise.
The Goldman lab has shown that the IF system forms a continuous
dynamic network linking the nuclear and cell surfaces that
performs important functions ranging from maintaining cell
shape to regulating nuclear structures involved in regulating
gene expression and DNA replication. Abnormally functioning
IF have been linked to ALS, Parkinson’s disease and muscular
dystrophy.
The cell surface/extracellular matrix group consists of
Lorand; Veis; Mary Hunzicker-Dunn; Jonathan Jones; Sharon
Stack; and James M. Kramer.
Veis is another of the department’s celebrated researchers.
He studies the regulation of growth and remodeling processes
in the collagen fibril matrix, bone and dentin. Remarkably,
several of Veis’s NIH grants have been funded for over
40 years.
Hunzincker-Dunn studies the cell surface-mediated signaling
pathways by which reproductive hormones induce differentiation
of ovarian cells. She also leads an intercampus PPG that focuses
on the signaling pathways and actions of follicle-stimulating
hormone. Her collaborators in this venture are Weinberg researchers
Jon Levine, Fred Turek and Kelly Mayo; and Larry Jameson,
M.D., Irving S. Cutter Professor and chair of medicine.
The Jones lab concentrates on interactions between epithelial
cells and the extracellular matrix. They have conducted studies
on cell junctions called hemidesmosomes, which Jones believes
act as "signal transducers" between the connective
tissue and epithelial cell layers, thereby influencing epithelial
gene expression. His lab group also studies surface factors
that promote endothelial cells to form new blood vessels,
and he directs a PPG that is studying cell alterations in
oral cancer. The PPG co-investigators are Goldman, Stack and
Kathleen Green, Joseph L. Mayberry Professor of Pathology.
Stack’s research focuses on the molecular mechanisms
producing oral cancer and the regulatory mechanisms involved
in the development of ovarian cancer. In particular, she investigates
the mechanisms controlling the transition of normal cells
to malignant cells capable of migrating from their normal
locations to form tumors in other tissues.
Kramer studies the functions of collagen, one of the major
components of the extracellular matrix. He heads up a team
of researchers known affectionately as the "worm group"
because they study the nematode Caenorhabditis elegans. The
simplicity of this worm’s systems makes it a powerful
model for molecular genetic studies of extracellular matrix
functions. Kramer has shown that mutations in the genes that
code for collagen in C. elegans basement membranes cause embryonic
death and are similar to those in humans with Alport’s
syndrome.
The group focusing on molecular mechanisms and the nucleus
includes Stephen Adam, Sui Huang, Carolyn L. Jahn and Richard
C. Scarpulla.
Adam studies the regulation of the transport of molecules
in and out of the nucleus. He developed a biochemical assay
for quantifying the movement of materials into the nucleus,
now used in laboratories all over the world. His most recent
studies involve a genetic approach to understanding the function
and regulation of nuclear transport proteins known as the
importins. These proteins play a critical role in signal transduction
and the transport of gene regulators or transcription factors
into the nucleus.
Huang is investigating the nuclear mechanisms underlying
the processing of RNA, particularly the perinucleolar compartment
— a unique nuclear structure she discovered — which
is present primarily in cancer cells. She and her lab group,
in collaboration with researchers at The Robert H. Lurie Cancer
Comprehensive Cancer Center of Northwestern University, have
been studying the prevalence of this structure in breast cancer
to determine whether the presence of this nuclear structure
can be used as a diagnostic indicator of malignancy.
Jahn uses several types of ciliated protozoa to study the
mechanisms responsible for gene rearrangements, a phenomenon
found to be associated with a number of human diseases, including
birth defects and cancer. Recently she has also been collaborating
with Doug Engel on the Evanston campus in genetic studies
of blood cell development in the mouse.
Scarpulla’s studies center on the molecular interactions
and physiological functions of proteins involved in the nuclear
control of mitochondrial biogenesis. His research is widely
recognized as prerequisite to understanding numerous human
disorders ranging from cardiomyopathies to neuromuscular diseases
that are linked to mutations in mitochondrial genes.
In the group working on Alzheimer’s disease, Binder
studies the neurofibrillary tangles recognized to be a hallmark
of Alzheimer’s disease. Binder was the first to discover
that the tangle is made of the microtubule-associated protein,
tau. Working closely with Binder is Robert Berry, who carries
out biochemical studies of the self-assembly properties of
tau protein in a variety of neurodegenerative diseases including
Pick’s disease. In a related area, Yuri Geinisman, M.D.,
studies the neurobiological basis of learning and memory in
aging brains.
Van Eldik is widely recognized for research on molecular
mechanisms and modulation of glial cell activation during
the development of Alzheimer’s disease. Her lab also
studies the function of the brain nerve cell protein S100,
specifically, experiments to determine whether S100 can act
as a biomarker of Alzheimer’s disease and other disorders.
In addition, Van Eldik plays a major role in the Drug Discovery
Program and heads an NIH postdoctoral training grant in this
area.
The newest member of this group is Robert Vassar who studies
the role of beta-amyloid, another important marker of Alzheimer’s
disease. He studies an enzyme, BACE1, known to be involved
in amyloid production. Vassar also developed the BACE1 knockout
mouse required for studying the biological functions of this
enzyme. BACE1 has become a prime drug target for the treatment
of Alzheimer’s disease.
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