PDB Newsletter
Number 19 -- Fall 2003

Published quarterly by the Protein Data Bank

Weekly PDB news is available online at
www.rcsb.org/pdb/latest_news.html.

Links to PDB newsletters are available at
www.rcsb.org/pdb/newsletter.html.

-----------------------------------------
SNAPSHOT -- October 1, 2003

22,700 released atomic coordinate entries

Molecule Type
      20,501 proteins, peptides, and viruses
       1,233 nucleic acids
         948 protein/nucleic acid complexes
          18 carbohydrates

Experimental Technique
      19,285 diffraction and other
      10,652 structure factor files
       3,415 NMR
       1,697 NMR restraint files

TABLE OF CONTENTS

Message from the PDB

Data Deposition and Processing
	PDB Deposition Statistics
	New Summary Report Available from TargetDB
	
Data Query, Reporting, and Access
	New Features on the PDB Web Site and FTP Archives
	New Version of OpenMMS Toolkit Released
	PDB Focus: Using rsync to Mirror the PDB FTP Site
	PDB Web Site Statistics

PDB Outreach
	PDB at the ISMB, ACA, and Protein Society Meetings	
	PDB Poster Prize -- 2003 Winners Announced
	PDB Art Part of Molecular Gallery Show at Cal State Fullerton
	Illustrations of "Macrophage and Bacterium" by
		Goodsell Win Award in NSF/Science Visualization Contest
	PDB Education Listserv 
	PDB Molecules of the Quarter:
	    Src Tyrosine Kinase, Calmodulin, and Estrogen Receptor

PDB Community Focus: Brian W. Matthews

PDB Education Corner

PDB Job Listings

Statement of Support
PDB Members

--------------------------------------------
MESSAGE FROM THE PDB

This past summer, the PDB attended several meetings and discussed with
users several of the new features available.  One of these
developments is the release of of files and images of the
biologically active units for all structures in the archive.  Another
is the release of standalone software for the preparation, validation,
and deposition of macromolecular data.

* The PDB has provided separate coordinate and image files containing
the biological molecule. These can be accessed from the Structure
Explorer "View Structure" and "Download/Display File" pages.

* Software is available for download and installation on your desktop
from deposit.pdb.org/software.  Software binaries are provided as
compressed files; README files are included with installation
instructions.  Some of the programs available include: PDB_EXTRACT,
which extracts mmCIF data from structure determination applications;
ADIT, which prepares files that can be emailed to the PDB for
deposition; and the PDB Validation Suite, which processes and checks
structure data.

We welcome your comments and questions about these features at
info@rcsb.org.

The PDB


DATA DEPOSITION AND PROCESSING

     PDB DEPOSITION STATISTICS

Since the beginning of the year, approximately 3,500 structures have
been deposited to the PDB. Eighty percent are deposited with a "hold until
publication status", 12% are deposited with a "release immediately"
status, and 8% are held until a specified date.

Eighty-three percent are from X-ray crystallographic studies and 12% are from NMR
studies. 

Fifty-five percent of these depositions release the sequence in advance of the
structure's release. Seventy-one percent of these depositions were deposited with
experimental data.  

     NEW SUMMARY REPORT AVAILABLE FROM TargetDB

TargetDB (targetdb.pdb.org) is a database of registration and tracking
information for structural genomics centers worldwide. TargetDB provides
timely status and tracking information on the progress of the production
and solution of structures.

The target database can be searched by sequence using FASTA
(W.R. Pearson and D.J. Lipman (1988): Improved tools for biological
sequence comparison. PNAS 85, pp. 2444-2448). Sequence searches may
include the target sequences, PDB sequences, or both. Target sequences
may also be searched by contributing site, protein name, project tracking
identifier, date of last modification, and the current status of the target
(e.g. cloned, expressed, crystallized, ...). Search results may be viewed
as HTML reports, FASTA data files, or in XML.

A new feature at the TargetDB site is a search form that can provide
summary tracking of target status. This form is now available from
TargetDB's main page. Users can search by Target ID, date, or site(s).
The summary report includes the number of targets at any given stage
in the pipeline. With this new option it is possible to track the progress
of a target or of an entire center over a user defined time interval.
For instance, reports can be created for each NIH center describing the
number of targets in each status category by project year.

Further information about TargetDB and links to structural genomics
resources are available at www.rcsb.org/pdb/strucgen.html.


DATA QUERY, REPORTING, AND ACCESS

     NEW FEATURES ON THE PDB WEB SITE AND FTP ARCHIVES

During this past quarter, several new developments that were previously
in beta test have been incorporated into the primary PDB web site, its
mirrors, and on the PDB FTP site:

 * Remediated mmCIF Files

The primary PDB Web site and its mirrors now offer the remediated mmCIF
files, previously referred to as the "beta" mmCIF files. These files have
replaced the set of automatically translated mmCIF files that were created
with pdb2cif.pl. The remediated files can be accessed from the 
Download/Display File section of the Structure Explorer page for any
entry, or for a set of query results.

The remediated mmCIF files are also available from the PDB FTP site at
ftp://ftp.rcsb.org/pub/pdb/data/structures/all/mmCIF/. The translated
files have been removed from the FTP site, and will be made available
upon individual request.

For every experimentally-solved structure, both current and obsolete,
there is now a remediated mmCIF file in the corresponding directory of
the FTP archive in Unix compressed (.Z) format. mmCIF files are not
provided for theoretical models. However, the translation software
(pdb2cif.pl) is provided at www.bernstein-plus-sons.com/software/pdb2cif
for users who wish to generate the translated mmCIF files.

 * Biological Unit Images and Coordinate Files

The View Structure section of the Structure Explorer now offers still
ribbon images of the assumed biological unit(s) for structures, where
relevant, in addition to static images of the asymmetric unit. Links
to the coordinate files that are used to generate the biological unit
images are also accessible here, as well as from the Download/Display
File section of the Structure Explorer.

Biological unit coordinate files are also available from the FTP archive
at ftp://ftp.rcsb.org/pub/pdb/data/biounit. These files are accessible
in gzipped (.gz) format. Links to a variety of free uncompression tools
can be found at www.rcsb.org/pdb/help-general.html#format_structure_compressed. 

 * Enzyme Names and EC Number Query

The Summary Information section of the Structure Explorer page for enzymes
in the PDB now displays the enzyme name for entries with complete EC numbers.
This section also supports queries for all other PDB entries with the same EC
number by clicking on the number shown for that entry.

Questions about these new features may be sent to info@rcsb.org.

     NEW VERSION OF OpenMMS TOOLKIT RELEASED

Version 1.5.1 of the OpenMMS software toolkit is now available on the OpenMMS
Web site at openmms.sdsc.edu. In addition to the fast database loader, this
version contains all of the pdbx fields from the PDB Exchange Dictionary
(deposit.pdb.org/mmcif). This includes attributes such as the model number
in the atom_site record which is needed for NMR structures. Also available
in this release is the "xconv" program which converts mmCIF files to XML
files with the standard XML/PDB format.
 
     PDB FOCUS: USING rsync TO MIRROR THE PDB FTP SITE

One freely available method for establishing and maintaining a local copy
of the PDB FTP Site is rsync. The RCSB-created script, rsyncPDB.sh, is a
template for using rsync to mirror the FTP archive from an anonymous rsync
server. This script can be found at ftp://ftp.rcsb.org/pub/pdb/software/,
and the comments in the script explain its usage. Prior to running it,
users will need to set three variables in rsyncPDB.sh to suit their local
setup. This script is used by the PDB to maintain its FTP mirrors. 

General rsync documentation can be found at www.samba.org/rsync. An
overview of PDB FTP mirroring procedures is offered at
www.rcsb.org/pdb/ftpproc.final.html, and the layout of the PDB FTP
archive is accessible at www.rcsb.org/pdb/ftp_plan.html.

For more information about rsync or mirroring the PDB FTP Site, please
send e-mail to info@rcsb.org.

     PDB WEB SITE STATISTICS

The PDB is available from several Web and FTP sites located around
the world.  Users are also invited to preview new features at the
PDB beta test site, accessible at beta.rcsb.org/pdb.

The access statistics are given below for the main PDB Web site
at www.pdb.org.

                  Access Statistics for www.pdb.org
..........Daily Average................Monthly Totals................
Month.....Hits......Files....Sites.....KBytes......Files......Hits...
Sep 03...202285....153680....96603....198614136....4456720....5866265 
Aug 03...131014....100838....65563....132975741....3025151....3930448 
Jul 03...146399....111723....75051....131039156....3351718....4391985 


PDB OUTREACH

     PDB AT THE ISMB, ACA, AND PROTEIN SOCIETY MEETINGS 

PDB staff members participated in several meetings this summer.  We
received excellent feedback from those in attendance at these events,
which will help to guide PDB's future developments:

11th International Conference on Intelligent Systems for Molecular
Biology (ISMB; June 29-July 3, Brisbane, Queensland, Australia) - New
query and reporting features of the re-engineered PDB site were
demonstrated at PDB's exhibit and as part of a presentation on
"The Re-engineered PDB" at this conference.

American Crystallographic Association's Annual Meeting
(ACA; July 26-31, Northern Kentucky Convention Center) - Desktop versions
of various software programs were demonstrated the PDB exhibit, and a
standalone version of ADIT software was distributed at this meeting.
Posters were presented on "TargetDB: A Target Registration Database for
Structural Genomics" and on the Ligand Depot. A presentation on "PDB Data
Assembly and Validation Tools" was part of the Computational Methods
session.  The PDB Poster prize, which is described further in this
newsletter, made its debut at the ACA meeting.

17th Symposium of the Protein Society (July 27-29, Boston, MA) - A poster
on the "New Features of the Protein Data Bank" was presented at this symposium.
 
     PDB POSTER PRIZE -- 2003 WINNERS ANNOUNCED

The PDB Poster Prize was awarded to the best student poster presentation
at this year's meetings of the IUCr Regional Associates--the American
Crystallographic Association (ACA), the Asian Crystallographic Association
(AsCA), and the European Crystallographic Association (ECA/ECM).

The winners are:

 * ACA - The first-ever PDB Poster Prize was awarded to Ty Gould for the
poster "Quorum Sensing Signal Generation by the AHL Synthsase LasI in 
Pseudomonas aeruginosa Pathogenesis" (T.A. Gould 1, R.C. Murphy 1, 
H.P. Schweizer 2, M.E.A. Churchill 1; 1 Dept. of Pharmacology, 
Univ. of Colorado Health Sciences Center, Denver, CO; 
2 Dept. of Microbiology, Colorado State Univ., Fort Collins, CO).
A runner-up award was made to Paul Hubbard for the poster "Structure
and Catalytic Mechanism of Bacterial 2, 4 - Dienoyl CoA Reductase."
(Xiquan Liang 3, Horst Schulz 3, Jung-Ja Kim, Department of Biochemistry,
Medical College of Wisconsin; 3 Department of Chemistry, The City University
of New York). Special thanks to the ACA PDB Poster Prize Committee members --
Vivien Yee (Chair), Victor Young, Tom Koetzle, Sylvie Doublie, 
Marvin L. Hackert, -- and the committee's organizer, Jeanette Krause Bauer. 

 * AsCA - The prize was awarded to Janet Deane for the poster "Crystal
structure of a complex of FLINC4, an intramolecular LMO4:LDB1 complex"
(Janet E. Deane, Megan Maher, J. Mitchell Guss, and Jacqueline M. Matthews,
School of Molecular and Microbial Biosciences, University of Sydney).
Special thanks to the judges of all of the student posters at AsCA --
Ted Baker (Chair), Peter Colman, Janet Smith, Mark Spackman, Colin Raston,
and Yu Wang.

 * ECM - The prize was awarded to Carina Lobley for the poster "Structural
Studies of the Enzymes of Pantothenate Synthesis" (Carina M.C. Lobley 1,
Mairi L. Kilkenny 1, Florian Schmitzberger 1, Michael E. Webb 2, 
Chris Abell 2, Alison G. Smith 3,1, Tom L. Blundell 1; 1 Department of 
Biochemistry, Cambridge; 2 University Chemical Laboratory, Cambridge; 
3 Department of Plant Sciences, Cambridge). Special thanks to the judges
of all of the student posters at ECM -- G. Davies, C. Kenyon, E.F. Garman,
and A. Roodt.

     PDB ART PART OF MOLECULAR GALLERY SHOW AT CAL STATE FULLERTON

The PDB's traveling art exhibit is part of the "Art of Science" show at
California State University, Fullerton. Featured are images from the PDB
and 3-D models by David Goodsell and Arthur Olson (The Scripps Research
Institute). Also included are objects from the Cal State Fullerton Keck
Center for Molecular Structure, such as an older generation X-ray camera.
The "Art of Science" will run through December 19 at the Atrium Gallery
in the Paulina June & George Pollak Library.

The PDB's "Art of Science" exhibit includes large-scale depictions of
proteins and images and text from the "Molecule of the Month" series.
The PDB would like to see the "Art of Science" travel to other places.
If you would be interested in sponsoring this exhibit at your institution,
please let us know at info@rcsb.org. 

     ILLUSTRATIONS OF "MACROPHAGE AND BACTERIUM" BY
     GOODSELL WIN AWARD IN NSF/SCIENCE VISUALIZATION CONTEST

PDB contributor and author of the "Molecule of the Month" series, 
David S. Goodsell, has been awarded second prize in the 2003 Science
and Engineering Visualization Challenge for his illustration "Macrophage
and Bacterium 2,000,000X". The challenge is a joint project of the 
National Science Foundation and "Science" Magazine that encourages and
promotes the visual and conceptual beauty of science and engineering.

Dr. Goodsell is an Associate Professor of Molecular Biology at The
Scripps Research Institute in La Jolla, California. His research
involves computational chemistry and biomolecular computer graphics.
Goodsell's artistic talents are multi-faceted, and include many renderings
of molecules and cells that are drawn, painted, or generated with the aid
of graphics programs. Previously he was awarded the Association of Medical
Illustrators Literary Award, among other distinctions he has received. He
has contributed many wonderful installments for the PDB "Molecule of the
Month" feature and has authored the popular PDB "Molecular Machinery" poster
--a recent interview with Dr. Goodsell that further describes these efforts
can be found in the PDB Newsletter's Spring 2003 issue.

Dr. Goodsell's winning series of three paintings shows a macrophage
engulfing a bacterium, including all of the macromolecules in the two
cells and in the surrounding blood serum. Goodsell used hundreds of PDB
structures for the paintings to get the sizes and shapes of the molecules
right: "The "Molecular Machinery" poster is a good example of the type of
information that I start with when I approach a new painting--lots of
structures all drawn at a consistent size."

The full winning entry can be viewed at 
www.scripps.edu/pub/goodsell/gallery/macrophagebacterium.html.
The original paintings are currently on display in the Center for
Integrative Molecular Biosciences at The Scripps Research Institute
in La Jolla.

     PDB EDUCATION LISTSERV

A listserv for educators who use the PDB has been established by
Dr. Judith Voet, Professor of Biochemistry at Swarthmore College
and member of the PDB Advisory Committee. The purpose of this forum
is to provide the PDB with feedback on its present usability by 
students and educators, and ideas for future directions in support
of education. If you would like to participate in the discussion,
send an e-mail message to jvoet1@swarthmore.edu with the request
to subscribe.

     PDB MOLECULES OF THE QUARTER:
     Src TYROSINE KINASE, CALMODULIN, AND ESTROGEN RECEPTOR

The "Molecule of the Month" series, by David S. Goodsell, explores
the functions and significance of selected biological macromolecules
for a general audience. These installments are available at 
www.rcsb.org/pdb/molecules/molecule_list.html.A sample of the
molecules featured during this past quarter are included below:

 * Src Tyrosine Kinase: Signaling, Redundancy, and Cancer

July, 2003 -- Your body is a democratic nation of cells. Each cell
is an individual with its own needs, but all of your cells work 
together to keep you alive. As you might imagine, this requires an
incredible amount of cooperation. Cells are in constant communication
to inform their neighbors of their needs and future plans. They send
messages to each other, passing hormones and chemokines and other
molecular messages from cell to cell. These messages are received by
proteins in the cell membrane, which transmit the signal inside. There,
a bewilderingly complex collection of proteins relays the message to
all of the appropriate places inside the cell.

The Src protein, shown in PDB entry 2src, is a signaling protein
that specializes in messages that control the growth of cells. It
sits just inside the cell membrane, where it assists in the passing
of signals from various protein receptors to the proteins that turn
"on" the engines of protein synthesis and cellular growth. Src is a
tyrosine kinase, so it relays its messages by adding phosphate groups
to special tyrosine amino acids in protein chains. It adds phosphate
groups to a wide variety of proteins that control cellular structure,
cell communication, and cellular growth, turning them "on" and releasing
them to perform their individual tasks.

For more information about Src tyrosine kinase, see
www.rcsb.org/pdb/molecules/pdb43_2.html.

 * Calmodulin: Sensing Calcium

August, 2003 -- Calcium is the most plentiful mineral element found
in your body, with phosphorous coming in second. This probably doesn't
come as a surprise, since your bones are strengthened and supported by
about two kilograms of calcium and phosphorous. Your body also uses a
small amount of calcium, in the form of calcium ions, to perform more
active duties. Calcium ions play essential roles in cell signaling,
helping to control processes such as muscle contraction, nerve signaling,
fertilization and cell division. Through the action of calcium pumps and
several kinds of calcium binding proteins, cells keep their internal
calcium levels 1000-10,000 times lower than the calcium levels in the
blood. Thus when calcium is released into cells, it can interact with
calcium sensing proteins and trigger different biological effects,
causing a muscle to contract, releasing insulin from the pancreas,
or blocking the entry of additional sperm cells once an egg has been
fertilized. 

As its name suggests, calmodulin is a CALcium MODULated proteIN. It
is abundant in the cytoplasm of all higher cells and has been highly
conserved through evolution. Calmodulin acts as an intermediary protein
that senses calcium levels and relays signals to various calcium-
sensitive enzymes, ion channels and other proteins. Calmodulin is a
small dumbbell-shaped protein composed of two globular domains connected
together by a flexible linker. Each end binds to two calcium ions. PDB
entry 3cln has all four sites filled with calcium ions and the linker
has formed a long alpha helix separating the two calcium-binding domains.

For more information on calmodulin, see
www.rcsb.org/pdb/molecules/pdb44_2.html.

 * Estrogen Receptor: a Large Family

September, 2003 -- Estrogens are small, carbon-rich molecules built
from cholesterol. This is quite different than larger hormones, such
as insulin and growth hormone, which are sensed by receptors on the
cell surface. Estrogens pass directly into cells throughout the body,
so the cell can use receptors that are in the nucleus, right at the
site of action on the DNA. When estrogen enters the nucleus, it binds
to the estrogen receptor, causing it to pair up and form a dimer.
This dimer then binds to several dozen specific sites in the DNA,
strategically placed next to the genes that need to be activated.
Then, the DNA-bound receptor activates the DNA-reading machinery
and starts the production of messenger RNA.

When researchers looked into the human genome, they found over 150
proteins that are similar to the estrogen receptor. This is a large
family of nuclear receptors that sense the levels of small hormones
and other signaling molecules, such as steroid and thyroid hormones,
vitamin D, and retinoic acid. Like estrogen, these are all small
molecules that pass directly into cells and find their way to the
nucleus. These receptors each bind to a specific signaling molecule
and then activate or repress their own set of 50-100 genes. For more
information on nuclear receptors from a genomic perspective, take a
look at the "Protein of the Month" feature at the European
Bioinformatics Institute (www.ebi.ac.uk/interpro/potm/archive.html).

For more information about the estrogen receptor, see
www.rcsb.org/pdb/molecules/pdb45_2.html.


PDB COMMUNITY FOCUS: BRIAN W. MATTHEWS

Brian W. Matthews is a long-time PDB depositor.  From 1982 through
the present time, he has contributed approximately 500 sets of
coordinates to the archive -- more than any other single author.
A Professor of Physics and a member of the Institute of Molecular
Biology at the University of Oregon, Matthews' numerous distinctions
and achievements also include an appointment as a Howard Hughes Medical
Institute investigator and membership in the U.S. National Academy of
Sciences.  He is involved in studying some of the fundamental problems
in biology, and his X-ray studies have always played a critical role
in his research.

The PDB recently interviewed Prof. Matthews on his experiences
in this field:

PDB: Over the years you have been an integral part of the tremendous
technical revolution that has taken place in protein crystallography.
How long did it take you to solve your first structure and what methods
did you use?  How long would it take to do the same structure today 
and why?

Prof. Matthews: The first structure that I solved was of a "small molecule"
of 14 atoms including a sulfur that was used as a "heavy atom".  It took
me over a year in part because all of the calculations had to be done by
hand and also because the Patterson function gave misleading information
regarding the location of the sulfur.  Today such a structure would be
solved in hours if not minutes.

The first protein structure determination with which I was involved was
that of alpha-chymotrypsin.  David Blow had been working on the project
at the MRC Lab in Cambridge and he and Michael Rossmann had used the
structure as a test case during their early development of the molecular
replacement technique.  Their calculations suggested that the two molecules
in the asymmetric unit were probably related by a local two-fold axis.
Shortly after I arrived in Cambridge, Barbara Jeffries, a technician working
on the project, found that the inclusion of 2% dioxane in the crystallizing
medium eliminated persistent twinning.  This made it possible to grow large,
untwinned crystals and to make a serious attempt at high-resolution data
collection. Data collection was by precession photography.  A single data
set necessitated 20-30 film packs, took perhaps three months to collect and
a similar amount of time to process.  Paul Sigler joined the project about
six months after I had arrived and Richard Henderson joined the group later
as a starting graduate student.  From the time that I joined the project
until the structure was solved took over three years, but as I mentioned,
the project had already been underway for several years.  We used the method
of isomorphous replacement following the pattern set with myoglobin and
lysozyme.  In the case of alpha-chymotrypsin we could average the density for
the two molecules in the asymmetric unit and this substantially improved the
quality of the electron density map.  We also included information from
anomalous scattering measurements incorporating ideas that were being
developed around that time.  Given high quality crystals the structure
could probably be solved today within a month or so.  As I mentioned,
however, the initial crystals were subject to frequent twinning.  Without
the introduction of dioxane by our technician, Barbara Jeffries, the
structure might still remain unsolved even today.

PDB: How has your research program evolved over the years? What role
has crystallography played in that evolution?

Prof. Matthews: Because of my involvement with the alpha-chymotrypsin
project, I had an early interest in proteolytic enzymes.  Therefore
it was natural for me, when I started my own laboratory at the
University of Oregon, to work on the thermostable protease thermolysin.
Because it was a zinc peptidase we were curious as to whether the structure
might be related to that of carboxypeptidase which by then had been
determined by the Lipscomb group at Harvard.  Also I had begun to develop
an interest in protein stability and folding.
  
Crystallography has been central to all of the subsequent work that we
have done.  The structure of the Cro protein immediately suggested how
it might bind to DNA.  The introduction of site-directed mutagenesis,
coupled with crystallography, led to our exploitation of the T4 lysozyme
system as a way to try to understand the structural basis of protein
stability.  It also contributed to what has been described as our
"pollution" of the Protein Data Bank with structures of mutant lysozymes.

PDB: You deposited your first structure approximately 20 years ago -
what do you think crystallography will be like for someone depositing
their first structure 20 years from now?

Prof. Matthews: I was extremely excited when we were able to determine
our first structure in my own lab.  This was thanks to the outstanding
contributions of Peter Colman, my first postdoc, together with Hans
Jansonius who spent 1971 in Eugene as a sabbatical visitor.  I am
pleased to see that students and postdocs who determine their first
structure in my group still share that same excitement.  I certainly
hope that this will remain 20 years in the future.  At the time that
I started my career in structural biology it was sufficient to be just
a crystallographer.  Now knowledge of crystallography is just one tool
in the repertoire of skills that are necessary.  I like to think that
crystallography remains as the most powerful tool that we have and hope
that it will remain so in the future.

PDB: The PDB plans to be there and to be ready - do you have any advice
for us based on your experience?

Prof. Matthews: Based on my own experience I have nothing but good things
to say about the PDB.  On a technical level the PDB has adapted extremely
well to handle the ever-increasing number of depositions.  I have also
found the PDB willing to consider suggestions for improvement.  Also the
PDB has played an essential role in helping to ensure that key structural
information are preserved and made available in a timely fashion to the
community at large.  Keep up the good work!


PDB EDUCATION CORNER

PDB's Education Corner features a different teacher each quarter,
offering an account of how he or she uses the PDB to educate
students. This quarter's column is by Prof. Paul A. Craig, Associate Professor
of Chemistry at the Rochester Institute of Technology:

The Protein Data Bank plays a critical role in teaching, learning and
research in Biochemistry education at the Rochester Institute of
Technology (RIT), a career-oriented comprehensive university with about
17,000 students. In the College of Science, students majoring in Biology,
Chemistry, Biochemistry, Biotechnology and Clinical Chemistry all take
courses in Biochemistry.  The complete Biochemistry sequence consists
of three courses which last a full academic year under our quarter system.
The first course covers amino acids, proteins and membranes, the second
is metabolism and the third is about nucleic acids and molecular genetics.  

 * Teaching and Learning

We use "Biochemistry" by Berg, Tymoczko and Stryer (Berg JM, Tymoczko JL,
Stryer L, 5th edition, W.H. Freeman, New York, 2002) in our courses.
Tim Driscoll of molvisions (molvisions.com) has developed an excellent
set of “Living Figures” for the publisher which we use in lecture to
demonstrate the structural features of proteins and nucleic acids
throughout the course sequence.   We believe that the students learn
much more, however, when they work on developing their own structure
documentaries based on PDB files. To emphasize the importance of
understanding structure and function in these courses, these docu-
mentaries account for 20% of their course grades.  For these projects,
students are asked to select a particular type of protein (e.g., a
kinase or a protease) from the PDB which includes either an inhibitor
(for the first course in our sequence) or a complex with a nucleic acid
(for the third course, which focuses on molecular biology). They then
use the PDB Structure Explorer page to identify the primary reference
for the structure.  From this starting point, they go to PubMed 
(www.ncbi.nlm.nih.gov) to identify at least two additional referred
resources. From these sources the students prepare a structure annotation
that includes a brief introduction, a statement of the physiological role
of the structure, a detailed description of the structure of the protein
which includes general features (e.g., secondary structures) and specific
features of the active site and the interaction between the protein and 
inhibitor (or nucleic acid), and a summary of the family relationships
of the structure.

Students are also required to prepare a series of molecular visualizations
for the structure part of the documentary.  This requires that students
spend a few hours learning how to read PDB files and compare information
in their files with the related publications.  After earlier attempts with
Kinemage and Rasmol, we spent several years helping students prepare Chime
pages, with varying degrees of success.  For the last two years the students
have been preparing their structure documentaries using a program called
BioEditor (bioeditor.sdsc.edu) that was developed at the San Diego Super-
computer Center (more on that below).

A more detailed description of the project requirements can be found at
www.rit.edu/~pac8612/Biochemistry/502(702)/protein_vis.htm.   A number
of students have produced stellar documentaries using BioEditor and these
can be viewed on the BioEditor Web site at
bioeditor.sdsc.edu/documentaries.shtml.

 * Software Development

My professional interests are at the interface between computers and
biology.  This has included simulations of several protein separation
processes.  The most successful of these is an electrophoresis simulation
(www.rit.edu/~pac8612/electro/Electro_Sim.html).  In communicating with
the programmers, I have always found that PDB files are an effective
starting point to explain sequence and structure information.

I was fortunate to spend the 2001-2002 academic year on sabbatical at
the San Diego Supercomputer Center where I worked Peng Yang (a programmer),
David Goodsell (a molecular biologist and a wonderful artist – see the
PDB "Molecule of the Month" pages) and Phil Bourne on developing a
software tool called BioEditor (bioeditor.sdsc.edu), which is designed
to facilitate the annotation of macromolecular structure (Yang P,
Craig PA, Goodsell D, Bourne PE.  BioEditor – Simplifying Macromolecular
Structure Annotation,  Bioinformatics (2003) 19: 897-898).  This tool
enables users to assemble information and images they need to create
documentaries about a particular structure or family of structures.
It includes a number of powerful features that enable users to prepare
structure documentaries: a built-in browser based on Internet Explorer
which enables users to directly download and incorporate PDB structure
files, a molecular visualization interface based on the Chime plug-in,
a tool for cataloguing images that are created by the user or collected
from other sites, and the ability to assemble references based only on
their PubMed ID numbers (PMIDs).

Students in Computer Science and Bioinformatics at RIT continue to work
on improving the ease of use and power of BioEditor as part of their
undergraduate and M.S. degree programs.


PDB JOB LISTINGS

PDB career opportunities are posted at www.rcsb.org/pdb/jobs.html.
The current available openings are:

     BIOCHEMICAL INFORMATION SPECIALIST

The Protein Data Bank at Rutgers University has a position open for
a Biochemical Information Specialist to curate and standardize
macromolecular structures for the Protein Data Bank. A background in
biological chemistry, as well as some experience with UNIX-based
computer systems, is required. Experience in crystallography and/or
NMR spectroscopy is a strong advantage. The successful candidate
should be well-motivated, able to pay close attention to detail, and
meet deadlines. This position offers the opportunity to participate
in an exciting project with significant impact on the scientific
community.

Please send resume to Dr. Helen Berman at pdbjobs@rcsb.rutgers.edu.

-----------------------------------------
STATEMENT OF SUPPORT

The PDB is supported by funds from the National Science Foundation,
the Department of Energy, and the National Institutes of Health,
in addition to resources and staff made available by the host 
institutions.

-----------------------------------------
The PDB is managed by three partner sites of the Research
Collaboratory for Structural Bioinformatics:

RUTGERS
Rutgers, The State University of New Jersey
Department of Chemistry and Chemical Biology
610 Taylor Road
Piscataway, NJ 08854-8087

SDSC/UCSD
San Diego Supercomputer Center
University of California, San Diego
9500 Gilman Drive
La Jolla, CA 92093-0537

CARB/NIST
Center for Advanced Research in Biotechnology
National Institute of Standards and Technology
9600 Gudelsky Drive
Rockville, MD 20850


PDB PROJECT TEAM LEADERS

Dr. Helen M. Berman - Director
Rutgers University
berman@rcsb.rutgers.edu

Dr. Philip E. Bourne - Co-Director
SDSC/UCSD
bourne@sdsc.edu

Judith L. Flippen-Anderson - Production and Outreach Leader
Rutgers University
flippen@rcsb.rutgers.edu

Dr. Gary L. Gilliland - Co-Director
CARB/NIST
gary.gilliland@nist.gov

Dr. John Westbrook - Co-Director
Rutgers University
jwest@rcsb.rutgers.edu


PDB MEMBERS

RUTGERS

Prentice Bisbal
prentice@rcsb.rutgers.edu

Kyle Burkhardt
kburkhar@rcsb.rutgers.edu

Li Chen
lchen@rcsb.rutgers.edu

Sharon Cousin
sharon@rcsb.rutgers.edu

Dr. Shuchismita Dutta
sdutta@rcsb.rutgers.edu

Dr. Zukang Feng
zfeng@rcsb.rutgers.edu

Lew-Christiane Fernandez
fernandz@rcsb.rutgers.edu

Dr. Rachel Kramer Green
kramer@rcsb.rutgers.edu

Vladimir Guranovic
vladimir@rcsb.rutgers.edu

Dr. Shri Jain
sjain@rcsb.rutgers.edu

Dr. Rose Oughtred
rose@rcsb.rutgers.edu

Dr. Irina Persikova
irina@rcsb.rutgers.edu

Suzanne Richman
richman@rcsb.rutgers.edu

Melcoir Rosas
melcoir@rcsb.rutgers.edu

Dr. Bohdan Schneider
bohdan@rcsb.rutgers.edu

Dr. Huanwang Yang
hyang@rcsb.rutgers.edu

Dr. Jasmin Yang
jasmin@rcsb.rutgers.edu

Christine Zardecki
zardecki@rcsb.rutgers.edu


SDSC/UCSD

Dr. Ken Addess
addess@sdsc.edu

David Archbell
dave@sdsc.edu

Tammy Battistuz
tammyb@sdsc.edu

Dr. Wolfgang Bluhm
wbluhm@sdsc.edu

Dr. Nita Deshpande
nita@sdsc.edu

Jeff Ott
jott@sdsc.edu

Wayne Townsend-Merino
wayne@sdsc.edu


CARB/NIST

Al Carlson
carlson@umbi.umd.edu

Dr. Veerasamy Ravichandran
vravi@nist.gov

Padma Priya Paragi Vedanthi
padmap@nist.gov

Elizabeth Walker
walkere@umbi.umd.edu

-----------------------------------------
PDB Newsletter
Number 19 -- Fall 2003

Published quarterly by the Protein Data Bank

Weekly PDB news is available online at
www.rcsb.org/pdb/latest_news.html.

Links to PDB newsletters are available at
www.rcsb.org/pdb/newsletter.html.