What is Developmental
Biology?
Most broadly put, developmental biologists seek to understand the emergence
of all the complexity of a human, an insect or a flower from a single
fertilized ovum.
The Emergence of Form From Uniformity.
One of the most fundamental questions of developmental biology is how
initially symmetric or unformed structures give rise to highly complex
three-dimensional functional organs and tissues. An obvious example is
the formation of an embyro from an egg, but other examples include the
way that a bacteria selects the site for the formation of a flagellum,
or a yeast cell its bud site, or a field of epithelial cells the site
for the formation of hair cells. Understanding the ways that this fundamental
biologic problem is solved by Nature is the topic of projects in the
laboratories of Lucy Shapiro, Anne Villeneuve, Matt Scott, Dale Kaiser,
Harley McAdams, Stuart Kim, James Nelson and Jeff Axelrod.
Self renewal: stem cells and cloning.
The origins, functions and uses of stem cells are developmental issues
that have recently become the center of media attention. These cells
have the remarkable property of continually renewing themselves while
giving rise to different cell types that can give rise to the cells necessary
to make an organ, such as the immune system or the brain. Perhaps, most
astounding is the recent discovery that the egg cytoplasm has the ability
to reset the nucleus of many cell types to a ground state. From this
ground state, perhaps defined by genomic chromatin structure the nucleus
can serve as a stem cell to all the cells of an entire organism and produce
a genetically identical or “cloned” individual. More specialized
stem cells are well defined for the hematologic system and methods of
purification of these stem cells, developed at Stanford in the Weissman
laboratory, have become the basis of treatment of treatment of leukemia.
Stems cells for neurons are being defined and may be useful for treating
the many degenerative neurologic diseases. Studies in this area have
excited the imagination of the general public, politicians and religious
leaders. Work in this area is being conducted in the laboratories of
Margaret T. Fuller, Irving Weissman, James A. Spudich, Lucy Shapiro,
Anne Villeneuve, and several others on the campus including Helen Blau
and Paul Khavari.
Communication between cells and within cells: pattern formation.
Although the form of a human, insect or dog is clearly preprogrammed
in DNA, development requires extensive communication between cells. Thus
much of the work of developmental biology is directed at understanding
these pathways of communication and how they lead to the eventual organization
of cells within a tissue or an organism. For example, Roel Nusses laboratory
has found that a group of extracellular proteins known as the wnts play
extensive roles organizing cells in the brain, the immune system, as
well as many other tissues. Work in Matt Scott’s lab has shown
that another family of secreted proteins, Hedghog, interacts with Patched
receptors to regulate the associations and formation of essential regions
of the brain and spinal cord. These same signaling mechanisms play important
roles in causing cancer.
Will Talbot, Matthew Scott, Roel Nusse, Irving Weissman, William Talbot,
and Stuart K. Kim.
Development of Cell Types and Organ Systems
The origins of individual organ systems from stem cells involves general
rules, which are being dissected in fruit flies and worms. These general
rules form the conceptual framework for the understanding of the origin
of the many thousands of cell types that make up the mammalian body.
The ligands receptors, signaling pathways and the way that they are coordinated
to form an organism are being studied in many laboratories at Stanford.
Matt Scott’s, Roel Nusse’s and Gerald Crabtree’s laboratory
have defined fundamental signaling pathways essential for the formation
of many cell types and organ systems. Seung Kim’s laboratory is
studying the development of the pancrease and David Kingsley’s
laboratory the skeletonal system. Work in Irv Weissman’s laboratory
is directed at understanding the formation of the hematopoetic system
and the immune system while Tom Quertermous’s laboratory is studying
the development of the heart, Paul Khavari’s lab the development
of the skin and Mark Krasnow the development of the lungs and respiratory
systems.
Seung K. Kim, David Kingsley, Gerald Crabtree, Irv Weissman, , Matt Scott,
Roel Nusse, Marc Tessier Lavigne, Paul Khavari, Thomas Quertermous, Mark
Krasnow and. (Insert the Thinker by Rodin).
Development of the nervous system.
Understanding the immense complexity of the nervous system presents
some of the most challenging problems in developmental biology. However
over
the past 5 or 10 years, studies in many laboratories have shown that
many of the molecules and mechanisms used in other systems are also
used in the formation of the nervous system. For example, Wnt signaling
and
Hedgehog signaling are used in the early formative events of the nervous
system and signaling by Ca2+, calcineurin and NFAT is used to convey
responses to axonal guidance molecules as developing nerves make connections
with their targets. The formation of the nervous system is being studied
in many laboratories at Stanford including those of Roel Nusse, Matt
Scott, Ben Barres, Gerald Crabtree, Sue McConnell, Richard Tsien, Bill
Mobely, Sue Mc Connell, and Linquin Luo.
A growth cone, shown above guides the developing nerve cells
and leads to the generation of over a 1000 trillion connections in
the mammalian
nervous system.
Plant Development
The development of plants results in some of the most beautiful objects
on earth. Recently powerful genetic models have been developed for
understanding the formation of flowers, the proliferation of food crops
and basic mechanisms of cell biology in plants. Plant development is
being studied in the laboratories of Virgina Wolbert, Ron Davis, and
Sharon Long in the Stanford Biology Department and the Carnegie Institute
at Stanford.
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The Evolution
of Form and the Mechanisms
of Speciation
Work in the laboratory of David Kingsley, Matt Scott, and Roel Nusse are addressing
the age old question of how species originate and how the form of an organism
evolves in response to its environment. With the realization that our genome
is far more plastic than we had suspected, such studies are critical to understanding
the long term outlook of our species
In David Kingsley’s laboratory they have focused on the three-spine speckleback
to understand how organisms have adapted to rapid environmental changes and
produced new species. This small fish lives in isolated ponds and lakes and
has shown the emergence of new species since the end of the Ice Age. Their
work involves analysis of genetic changes in populations of fish that happen
to live in beautiful places. You can see David and his lab members collecting
fish
Aging and Senescence
Senescence appears to be a normal part of development, preprogramed by our
genetic makeup. Here studies are directed at understanding why different
organisms have different life spans and what are the genes that give
rise to these differences? How do these genes define the onset of age related
diseases like alzheimers and others and what is the basis of genetic
human
diseases such as Progeria. Studies in yeast, flys and worms have provided
fundamental insights into these processes. Stuart K. Kim is investigating
the mechanism of aging using worms as a model.
A 99 year old man goes into a doctor’s office and complains of pain in
his knee. After examining the man the doctor reminds the man that his knee
is, after all 99 years old. The mans says, “well my other knee is 99
years old and it doesn’t hurt”.
Development and Disease
Virtually every disease can be viewed as a failure of development.
For example, even diseases that occur late in life, such as heart
disease, arthritis or
epilepsy often have their origins in embryonic defects such as the patterning
of heart valves, joint formation or the migration of neurons. Treading this
borderland of embryology and pathology is actually a fundamental method of
learning the rules of development as the following examples illustrate. A
student in David Kingley’s laboratory recently discovered the ank gene, which
when inactivated produces arthritis. Such a discovery is informative both for
understanding and treating human disease as well as for the information that
it gives regarding the formation of joints. The most common cancer in humans
is a skin tumor known as basal cell carcinoma, which was shown in Matt Scott’s
laboratory to be caused by mutations in the Patched gene that plays important
roles in early development. In dissecting the intracellular signaling pathways
necessary for lymphocyte development the Crabtree lab discovered the mechanism
of action of the immunosuppressant, cyclosporin A. This same signaling pathway
has turned out to be essential for development of the heart, vascular, nervous
and skeletonal systems as well as the recombinational immune system.
Developmental Biology and Medicine
Clearly the closest medical disciplines to developmental biology are
Pediatrics and Obstetrics, but the interface between medicine and developmental
biology
extends through all medicine and surgery. For example, Roel Nusse discovered
the murine wnt genes, not as a developmental regulator, but as gene mutated
in certain types of cancer. Other associations with disease and treatment
emerge from unexpected directions. For example, a gene first cloned
in the Crabtree
laboratory as a protease inhibitor, and later developed by Eli Lilly, is
now the mainstay of treatment of a severe form of infection know as
sepsis. Studies
in the Weissman laboratory have lead to the purification of hematopoietic
stem cells needed for treatment of leukemia, cancer and organ transplantation.
Similar
approaches to purification of neural stem cells are paving the way for the
development of new methods of treatment of degenerative diseases of the nervous
system.
Gene Therapy
Many childhood and genetic diseases can only be treated by introducing the
defective gene. To do this is a complicated endeavor that has caught the imagination
of the general public. Mark A. Kay and Paul Khavari are developing and using
new methods to introduce genes into mice and humans with the goal of correcting
genetic diseases. Gerald Crabtree’s lab has developed a method of controlling
the activity of virtually any protein using small membrane permeable synthetic
ligands that can be given orally. This methods has been used to regulate the
production and local release of molecules such as growth hormone, insulin,
Vegf and others that are therapeutically useful.
Development of new techniques for biologic studies.
Information science is playing an ever more critical role in understanding
development. An aspect of these studies that is assuming increasing importance
in the future is the prediction of the outcome of modifications in developmental
pathways. Eventually work in this area is likely to lead to the development
of predictive criteria for the genetic disease as well as the results of
therapeutic efforts. Work in the laboratories of Harley McAdam and Lucy Shapiro
are directed at developing methods and approaches to predict the actions
of genetic circuits and how they respond to manipulation. Their work relies
on classic models in phage and bacterical genetics that serve as general
and widely applicable tests of the characteristics of biologic circuits. One
of these circuits defined by Harley McAdams and Lucy Shiparo is shown on
the right of the navigation bar above.
New computer methods of evaluating transcript expression and biologic control
mechanisms are also being developed in the labs of Pat Brown, Stuart Kim and
several other groups at Stanford.
Understanding certain questions in development will require entirely new approaches.
For example, how do certain behaviorial patterns develop, such as nurturing
of offspring? One can remove the function of a gene, but how can the effect
of the mutation be shown to lead directly to a failure of nurturing? Understanding
these more difficult problems of development will require approaches were the
function of a single gene can be rapidly and reversibly removed, allowing one
to define the immediate biochemical consequences of inactivating or activating
a gene. Such approaches will allow primary effects to be distinquished from
secondary effects and causation to be distinguished from coincidence. A fusion
of chemistry and biology is essential to bring about these goals and is being
developed in the labs of Gerald Crabtree and Tom Wandless. These methods use
small molecules control proximity of proteins as shown in the figure below
 .
New methods in manipulating signal molecules, such as myosin are being
development in the labs of Jim spudich. These methods allow the understanding
of mechanisms
of molecular moters. The flourscence activated cell sorter (FACS), which
revolutionized developmental studies, was invented at Stanford by
Len Hertzenberg and set
the model for many productive interactions between physics and biology. New
technique development is being conducted in the labs of Jim Spudich, Harley
McAdams, Lucy Shipiro, Stuart Kim, Gerald Crabtree, Pat Brown.
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