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Title: MA /GENERAL_SPEC: ALPHABET ... 3D structure Contain the

1
An introduction to biological databases
2
Database or databank ?

At the beginning, subtle distinctions were done
between databases and databanks (in UK, but not
in the USA), such as
Database management programs for the gestion
of databanks
From now on, the term database (db) is
usually preferred

3
What is a database ?

A collection of...
structured
searchable (index) -gt table of contents
updated periodically (release) -gt new edition
cross-referenced (hyperlinks) -gt links with
other db
data
Includes also associated tools (software)
necessary for db access, db updating, db
information insertion, db information deletion.

4
Databases an simple example
Introduction To Database Teacher Database
(ITDTdb) (flat file, 3 entries)

Accession number 1
First Name Amos
Last Name Bairoch
Course DEAoct-nov-dec 2000
http//expasy4.expasy.ch/people/amos.html
//
Accession number 2
First Name Laurent
Last name Falquet
Course EMBnetsept 2000DEAoct-nov-dec 2000
//
Accession number 3
First Name Marie-Claude
Last name Blatter Garin
Course EMBnetsept 2000DEAoct-nov-dec 2000
http//expasy4.expasy.ch/people/Marie-Claude.Blatt
er-Garin.html
//
Easy to manage all the entries are visible at
the same time !

5
Databases an simple example (cont.)
Relational database ( table file )
Easier to manage choice of the output
6
Why biological databases ?

Explosive growth in biological data
Data (sequences, 3D structures, 2D gel analysis,
MS analysis.) are no longer published in a
conventional manner, but directly submitted to
databases
Essential tools for biological research, as
classical publications used to be !

7
Biological databases

Some databases in the field of molecular
biology
AATDB, AceDb, ACUTS, ADB, AFDB, AGIS, AMSdb,
ARR, AsDb, BBDB, BCGD, Beanref,
Biolmage,
BioMagResBank, BIOMDB, BLOCKS,
BovGBASE,
BOVMAP, BSORF, BTKbase, CANSITE, CarbBank,
CARBHYD, CATH, CAZY, CCDC, CD4OLbase, CGAP,
ChickGBASE, Colibri, COPE, CottonDB, CSNDB, CUTG,
CyanoBase, dbCFC, dbEST, dbSTS, DDBJ, DGP,
DictyDb,
Picty_cDB, DIP, DOGS, DOMO, DPD, DPlnteract,
ECDC,
ECGC, EC02DBASE, EcoCyc, EcoGene, EMBL, EMD db,
ENZYME, EPD, EpoDB, ESTHER, FlyBase, FlyView,
GCRDB, GDB, GENATLAS, Genbank, GeneCards,
Genline, GenLink, GENOTK, GenProtEC,
GIFTS,
GPCRDB, GRAP, GRBase, gRNAsdb, GRR, GSDB,
HAEMB, HAMSTERS, HEART-2DPAGE, HEXAdb, HGMD,
HIDB, HIDC, HlVdb, HotMolecBase, HOVERGEN, HPDB,
HSC-2DPAGE, ICN, ICTVDB, IL2RGbase, IMGT, Kabat,
KDNA, KEGG, Klotho, LGIC, MAD, MaizeDb, MDB,

8
Some statistics

More than 1000 different databases
Generally accessible through the web
(useful link www.expasy.ch/alinks.html)
Variable size lt100Kb to gt10Gb
DNA gt 10 Gb
Protein 1 Gb
3D structure 5 Gb
Other smaller
Update frequency daily to annually

9
Categories of databases for Life Sciences

Sequences (DNA, protein) -gt Primary db
Genomics
Protein domain/family -gt Secondary db
Mutation/polymorphism
Proteomics (2D gel, MS)
3D structure -gt Structure db
Metabolism
Bibliography
Others

10
Distribution of sequence databases

Books, articles 1968 -gt 1985
Computer tapes 1982 -gt1992
Floppy disks 1984 -gt 1990
CD-ROM 1989 -gt ?
FTP 1989 -gt ?
On-line services 1982 -gt 1994
WWW 1993 -gt ?
DVD 2001 -gt ?

11
Sequence Databases some technical definitions

Data storage management
flat file text file
relational (e.g., Oracle)
object oriented (rare in biological field)
Format (flat file)
fasta
GCG
NBRF/PIR
MSF.
standardized format ?
Federated databases different autonomous,
redundant, heterogeneous db linked together by
links/hyperlinks.

12
Ideal minimal content of a sequence db

Sequences !!
Accession number (AC)
References
Taxonomic data
ANNOTATION/CURATION
Keywords
Cross-references
Documentation

13
Sequence database example
SWISS-PROT Flat file
ID EPO_HUMAN STANDARD PRT 193
AA. AC P01588 DT 21-JUL-1986 (Rel. 01,
Created) DT 21-JUL-1986 (Rel. 01, Last sequence
update) DT 30-MAY-2000 (Rel. 39, Last
annotation update) DE Erythropoietin
precursor. GN EPO. OS Homo sapiens
(Human). OC Eukaryota Metazoa Chordata
Craniata Vertebrata Euteleostomi OC
Mammalia Eutheria Primates Catarrhini
Hominidae Homo. RN 1 RP SEQUENCE FROM
N.A. RX MEDLINE 85137899. RA Jacobs K.,
Shoemaker C., Rudersdorf R., Neill S.D., Kaufman
R.J., RA Mufson A., Seehra J., Jones S.S.,
Hewick R., Fritsch E.F., RA Kawakita M.,
Shimizu T., Miyake T. RT "Isolation and
characterization of genomic and cDNA clones of
human RT erythropoietin." RL Nature
313806-810(1985). ... CC -!- FUNCTION
ERYTHROPOIETIN IS THE PRINCIPAL HORMONE INVOLVED
IN THE CC REGULATION OF ERYTHROCYTE
DIFFERENTIATION AND THE MAINTENANCE OF A CC
PHYSIOLOGICAL LEVEL OF CIRCULATING ERYTHROCYTE
MASS. CC -!- SUBCELLULAR LOCATION SECRETED. CC
-!- TISSUE SPECIFICITY PRODUCED BY KIDNEY OR
LIVER OF ADULT MAMMALS CC AND BY LIVER OF
FETAL OR NEONATAL MAMMALS. CC -!-
PHARMACEUTICAL Available under the names Epogen
(Amgen) and CC Procrit (Ortho Biotech). CC
-!- DATABASE NAMERD Systems' cytokine source
book CC WWW"http//www.rndsystems.com/cyt_
cat/epo.html". DR EMBL X02158 CAA26095.1
-. DR EMBL X02157 CAA26094.1 -. DR EMBL
M11319 AAA52400.1 -. DR EMBL AF053356
AAC78791.1 -. DR EMBL AF202308 AAF23132.1
-. DR EMBL AF202306 AAF23132.1
JOINED. ... KW Erythrocyte maturation
Glycoprotein Hormone Signal Pharmaceutical. FT
SIGNAL 1 27 FT CHAIN 28
193 ERYTHROPOIETIN. FT PROPEP 190
193 MAY BE REMOVED IN PROCESSED PROTEIN. FT
DISULFID 34 188 ...
taxonomy
reference
annotations
Cross-references
Keywords
14
Sequence database example (cont.)
FT DISULFID 34 188 FT DISULFID 56
60 FT CARBOHYD 51 51 N-LINKED
(GLCNAC...). FT CARBOHYD 65 65
N-LINKED (GLCNAC...). FT CARBOHYD 110 110
N-LINKED (GLCNAC...). FT CARBOHYD 153
153 FT CONFLICT 40 40 E -gt Q
(IN CAA26095). FT CONFLICT 85 85
Q -gt QQ (IN REF. 5). FT CONFLICT 140 140
G -gt R (IN CAA26095). Chromosomal
location 7q22 SQ SEQUENCE 193 AA 21306 MW
C91F0E4C26A52033 CRC64 MGVHECPAWL
WLLLSLLSLP LGLPVLGAPP RLICDSRVLE RYLLEAKEAE
NITTGCAEHC SLNENITVPD TKVNFYAWKR MEVGQQAVEV
WQGLALLSEA VLRGQALLVN SSQPWEPLQL HVDKAVSGLR
SLTTLLRALG AQKEAISPPD AASAAPLRTI TADTFRKLFR
VYSNFLRGKL KLYTGEACRT GDR //
sequence
15
Sequence database example

a SWISS-PROT entry, in fasta format
gtspP01588EPO_HUMAN ERYTHROPOIETIN PRECURSOR -
Homo sapiens (Human).
MGVHECPAWLWLLLSLLSLPLGLPVLGAPPRLICDSRVLERYLLEAKEAE
NITTGCAEHCSLNENITVPDTKVNFYAWKRMEVGQQAVEVWQGLALLSEA
VLRGQALLVNSSQPWEPLQLHVDKAVSGLRSLTTLLRALGAQKEAISPPD
AASAAPLRTITADTFRKLFRVYSNFLRGKLKLYTGEACRTGDR

16
Databases 1 nucleotide sequence

The main DNA sequence db are
EMBL (Europe)/GenBank (USA) /DDBJ (Japan)
There are also specialized databases for the
different types of RNAs (i.e. tRNA, rRNA, tm RNA,
uRNA, etc)
3D structure (DNA and RNA)
Others Aberrant splicing db Eucaryotic promoter
db (EPD) RNA editing sites, Multimedia Telomere
Resource

17
EMBL/GenBank/DDJB

These 3 db contain mainly the same informations
within 2-3 days (few differences in the format
and syntax)
Serve as archives containing all sequences
(single genes, ESTs, complete genomes, etc.)
derived from
Genome projects and sequencing centers
Individual scientists
Patent offices (i.e. European Patent Office, EPO)
Non-confidential data are exchanged daily
Currently 8.3 x106 sequences, over 9.7 x109 bp
Sequences from gt 50000 different species

18
EMBL/GenBank/DDBJ

Heterogeneous sequence length genomes, variants,
fragments
Sequence sizes
max 300000 bp /entry (! genomic sequences,
overlapping)
min 10 bp /entry
Archive nothing goes out -gt highly redundant !
full of errors in sequences, in annotations, in
CDS attribution
no consistency of annotations most annotations
are done by the submitters heterogeneity of the
quality and the completion and updating of the
informations

19
EMBL/GenBank/DDJB

Unexpected informations you can find in these db
FT source 1..124
FT /db_xref"taxon4097"
FT /organelle"plastidchloropla
st"
FT /organism"Nicotiana
tabacum"
FT /isolate"Cuban cahibo
cigar, gift from President Fidel
FT Castro"
Or
FT source 1..17084
FT /chromosome"complete
mitochondrial genome"
FT /db_xref"taxon9267"
FT /organelle"mitochondrion"
FT /organism"Didelphis
virginiana"
FT /dev_stage"adult"
FT /isolate"fresh road killed
individual"
FT /tissue_type"liver"

20
EMBL entry example

ID HSERPG standard DNA HUM 3398 BP.
XX
AC X02158
XX
SV X02158.1
XX
DT 13-JUN-1985 (Rel. 06, Created)
DT 22-JUN-1993 (Rel. 36, Last updated, Version
2)
XX
DE Human gene for erythropoietin
XX
KW erythropoietin glycoprotein hormone
hormone signal peptide.
XX
OS Homo sapiens (human)
OC Eukaryota Metazoa Chordata Craniata
Vertebrata Euteleostomi Mammalia
OC Eutheria Primates Catarrhini Hominidae
Homo.
XX
RN 1
RP 1-3398

keyword
taxonomy
references
Cross-references
21
EMBL entry (cont.)

CC Data kindly reviewed (24-FEB-1986) by K.
Jacobs
FH Key Location/Qualifiers
FH
FT source 1..3398
FT /db_xreftaxon9606
FT /organismHomo sapiens
FT mRNA join(397..627,1194..1339,1596
..1682,2294..2473,2608..3327)
FT CDS join(615..627,1194..1339,1596
..1682,2294..2473,2608..2763)
FT /db_xrefSWISS-PROTP01588
FT /producterythropoietin
FT /protein_idCAA26095.1
FT /translationMGVHECPAWLWLLLSL
LSLPLGLPVLGAPPRLICDSRVLQRYLLE
FT AKEAENITTGCAEHCSLNENITVPDTKVN
FYAWKRMEVGQQAVEVWQGLALLSEAVLRG
FT QALLVNSSQPWEPLQLHVDKAVSGLRSLT
TLLRALGAQKEAISPPDAASAAPLRTITAD
FT TFRKLFRVYSNFLRGKLKLYTGEACRTGD
R
FT mat_peptide join(1262..1339,1596..1682,22
94..2473,2608..2763)
FT /producterythropoietin
FT sig_peptide join(615..627,1194..1261)
FT exon 397..627

annotation
sequence
22
GenBank entry example

LOCUS HSERPG 3398 bp DNA
PRI 22-JUN-1993
DEFINITION Human gene for
erythropoietin.
ACCESSION X02158
VERSION X02158.1
GI31224
KEYWORDS
erythropoietin glycoprotein hormone hormone
signal peptide.
SOURCE human.
ORGANISM Homo sapiens
Eukaryota
Metazoa Chordata Vertebrata Mammalia
Eutheria
Primates
Catarrhini Hominidae Homo.
REFERENCE 1 (bases 1 to
3398)
AUTHORS Jacobs,K.,
Shoemaker,C., Rudersdorf,R., Neill,S.D.,
Kaufman,R.J.,
Mufson,A.,
Seehra,J., Jones,S.S., Hewick,R., Fritsch,E.F.,
Kawakita,M.,
Shimizu,T. and Miyake,T.
TITLE Isolation and
characterization of genomic and cDNA clones of
human
erythropoietin
JOURNAL Nature 313
(6005), 806-810 (1985)
MEDLINE 85137899
COMMENT Data kindly
reviewed (24-FEB-1986) by K. Jacobs.
FEATURES
Location/Qualifiers

23
GenBank entry (cont.)

TADTFRKLFRVYSNFLRGKLKLYTGEACRTGDR"
intron
628..1193
/number1
exon
1194..1339
/number2
mat_peptide
join(1262..1339,1596..1682,2294..2473,2608..2760)
/product"erythropoietin"
intron
1340..1595
/number2
exon
1596..1682
/number3
intron
1683..2293
/number3
exon
2294..2473
/number4
intron
2474..2607
/number4
exon
2608..3327
/note"3' untranslated region"

24
DDJB entry example

LOCUS HSERPG 3398 bp DNA
HUM 22-JUN-1993
DEFINITION Human gene for erythropoietin.
ACCESSION X02158
VERSION X02158.1
KEYWORDS erythropoietin glycoprotein hormone
hormone signal peptide.
SOURCE human.
ORGANISM Homo sapiens
Eukaryota Metazoa Chordata
Craniata Vertebrata Mammalia
Eutheria Primates Catarrhini
Hominidae Homo.
REFERENCE 1 (bases 1 to 3398)
AUTHORS Jacobs,K., Shoemaker,C.,
Rudersdorf,R., Neill,S.D., Kaufman,R.J.,
Mufson,A., Seehra,J., Jones,S.S.,
Hewick,R., Fritsch,E.F.,
Kawakita,M., Shimizu,T. and Miyake,T.
TITLE Isolation and characterization of
genomic and cDNA clones of human
erythropoietin
JOURNAL Nature 313, 806-810(1985)
MEDLINE 85137899
COMMENT Data kindly reviewed (24-FEB-1986) by
K. Jacobs
FEATURES Location/Qualifiers

25
DDJB (cont.)

mat_peptide join(1262..1339,1596..1682,2294..2
473,2608..2763)
/product"erythropoietin"
sig_peptide join(615..627,1194..1261)
exon 397..627
/number1
intron 628..1193
/number1
exon 1194..1339
/number2
intron 1340..1595
/number2
exon 1596..1682
/number3
intron 1683..2293
/number3
exon 2294..2473
/number4
intron 2474..2607
/number4

26
The tremendous increase in nucleotide sequences

EMBL datafirst increase in data due to the PCR
development

1980 80 genes fully sequenced !
27
EMBL divisions

EMBL has been divided into subdatabases to allow
easier data management and searches
fun, hum, inv, mam, org, phg, pln, pro, rod, syn,
unc, vrl, vrt
est, gss, htg, sts, patent

28
RefSeq a SWISS-PROT clone?

The NCBI Reference Sequence project (RefSeq) will
provide reference sequence standards for the
naturally occurring molecules of the central
dogma, from chromosomes to mRNAs to proteins.
RefSeq standards provide a foundation for the
functional annotation of the human genome. They
provide a stable reference point for mutation
analysis, gene expression studies, and
polymorphism discovery.
Molecule Accession Format Genome
Complete Genome NC_ Archaea, Bacterial,
Organelle,Virus, Viroid
Complete Chrom. NC_ Eukaryote
Complete Sequence NC_ Plasmid
Genomic Contig NT_ Homo sapiens
mRNA NM_ Homo sapiens, Mus musculus,
Rattus norvegicus
Protein NP_ All of the above

29
RefSeq a SWISS-PROT clone?

RefSeq records are created via a process
consisting of
identifying sequences that represent distinct
genes
establishing the correct gene name-to-accession
number association
identifying the full extent of available sequence
data
creating a new RefSeq record with a status of
PREDICTED
PROVISIONAL
REVIEWED
Provisional RefSeq records are reviewed by a
biologist who confirms the initial
name-to-sequence association, adds information
including a summary of gene function, and, more
importantly, corrects, re-annotates, or extends
the sequence data using data available in other
GenBank records.

30
Databases 2 genomics

Contain information on genes, gene location
(mapping), gene nomenclature and links to
sequence databases
Exist for most organisms important for life
science research
Examples MIM, GDB (human), MGD (mouse), FlyBase
(Drosophila), SGD (yeast), MaizeDB (maize),
SubtiList (B.subtilis), etc.
Format generally relational (Oracle, SyBase or
AceDb).

31
MIM

OMIM Online Mendelian Inheritance in Man
a catalog of human genes and genetic disorders
contains a summary of literature, pictures, and
reference information. It also contains numerous
links to articles and sequence information.

32
MIM example

133170 ERYTHROPOIETIN EPO
Alternative titles symbols
EP
TABLE OF CONTENTS
TEXT
REFERENCES
SEE ALSO
CONTRIBUTORS
CREATION DATE
EDIT HISTORY
Database Links
Gene Map Locus 7q21

33
Ensembl

Contains all the human genome DNA sequences
currently available in the public domain.
Automated annotation by using different software
tools, features are identified in the DNA
sequences
Genes (known or predicted)
Single nucleotide polymorphisms (SNPs)
Repeats
Homologies
Created and maintained by the EBI and the Sanger
Center (UK)
www.ensembl.org

34
Database 3 protein sequence

SWISS-PROT created in 1986 (A.Bairoch)
TrEMBL created in 1996 complement to
SWISS-PROT derived from automated EMBL CDS
translations ( proteomic version of EMBL)
GenPept derived from automated GenBank CDS
translations and journal scans ( proteomic
version of GenBank)
PIR Protein Information Resources
MIPS Martinsried Institute for Protein Sequences
PIR PATCHX (supplement of unverified protein
sequences from external sources)

35
Database 3 protein sequence

NRL-3D produced by PIR from PDB (3D struture)
sequences
Many specialized protein databases for specific
families or groups of proteins.
Examples YPD (yeast proteins), AMSDb
(antibacterial peptides), GPCRDB (7 TM
receptors), IMGT (immune system) etc.

36
SWISS-PROT

Collaboration between the SIB (CH) and EMBL/EBI
(UK)
Annotated (manually), non-redundant,
cross-referenced, documented protein sequence
database.
88 000 sequences from more than 6800 different
species 70 000 references (publications)
550 000 cross-references (databases) 200 Mb of
annotations.
Weekly releases available from about 50 servers
across the world, the main source being ExPASy

37
SWISS-PROT example
Never changed
38
SWISS-PROT (cont.)
39
SWISS-PROT (cont.)
40
TrEMBL (Translation of EMBL)

Computer-annotated supplement to SWISS-PROT, as
it is impossible to cope with the flow of data
Well-structure SWISS-PROT-like resource
Derived from automated EMBL CDS translation
(maintained at the EBI (UK))
TrEMBL is automatically generated and annotated
using software tools (incompatible with the
SWISS-PROT in terms of quality)
TrEMBL contains all what is not yet in SWISS-PROT
Yerk!! But there is no choice and these software
tools are becoming quite good !

41
The simplified story of a Sprot entry
cDNAs, genomes, .

Automatic
Redundancy check (merge)
InterPro (family attribution)
Annotation

EMBLnew EMBL
CDS
TrEMBLnew TrEMBL

Manual
Redundancy (merge, conflicts)
Annotation
Sprot tools (macros)
Sprot documentation
Medline
Databases (MIM, MGD.)
Brain storming

SWISS-PROT
Once in Sprot, the entry is no more in TrEMBL,
but still in EMBL (archive)
42
SWISS-PROT introduces a new arithmetical concept !

How many sequences in SWISS-PROT TrEMBL ?
88000 300 000 about 240000
SWISS-PROT and TrEMBL (SPTR)
a minimal of redundancy

43
TrEMBL divisions

TrEMBL SPTrEMBL REMTrEMBL
SPTrEMBL TrEMBL entries that will eventually be
integrated into SWISS-PROT, but that have not yet
be manually annotated
REMTrEMBL sequences that are not destined to be
included in SWISS-PROT
Immunoglobulins and T-cell receptors
Synthetic sequences
Patented sequences
Small fragments (lt8 aa)
CDS not coding for real proteins
TrEMBL new updates to the latest release of
TREMBL

44
TrEMBL divisions

Subdivisions
Archae arc
Fungus fun
Human hum
Invertebrate inv
Mammals mam
Major Hist. Comp. mhc
Organelles org
Phage phg
Plant pln
Prokaryote pro
Rodent rod
Uncommented unc
Viral vrl
Vertebrate vrt

45
TrEMBL example
46
GenPept (translation of GenBank)

GenPept is a protein database translated from the
last release of GenBank ( journal scans)
The current release has 484496 entries
In contrast to TrEMBL, keeps all protein
sequences including small fragments (lt 8 aa),
immunoglobulins.
Redundancy 20 entries for human EPO

47
GenPept example

LOCUS L33410_1
HUMMLCMPL
DEFINITION Human c-mpl
ligand (ML) mRNA, complete cds
erythropoietin
homology domain bp 66..522.
DATE 07-JAN-1995
ACCESSION L33410
NID
ORGANISM Homo_SP_sapiens
Eukaryota
Metazoa Chordata Craniata Vertebrata
Euteleostomi
Mammalia
Eutheria Primates Catarrhini Hominidae Homo.
COMMENT CDS 216..1277
/gene"ML"
/product"c-mpl
ligand"
/protein_id"AAA59857.1"
/db_xref"GI506827"
WEIGHT 37823
LENGTH 353
ORIGIN
1 MELTELLLVV
MLLLTARLTL SSPAPPACDL RVLSKLLRDS HVLHSRLSQC
PEVHPLPTPV
61 LLPAVDFSLG
EWKTQMEETK AQDILGAVTL LLEGVMAARG QLGPTCLSSL
LGQLSGQVRL

48
PIR

Protein Information Resource, created in 1984
Successor of the National Biochemical Research
Foundation (NBRF) protein sequence database
developed in 1965 by M. O. Dayhoff Atlas of
Protein Sequence and Structure
Maintained by MIPS (Germany) and JIPID (Japan)
Provides some cross-referencing to
EMBL/GenBank/DDJB and PDB, GDB, FlyBase, OMIM,
SGD, and MGD
In august 2000 178050 entries.
Redundancy 3 entries for human EPO

49
PIR example

gtP1ZUHU
erythropoietin precursor - human
CSpecies Homo sapiens (man)
CDate 27-Nov-1985 sequence_revision
27-Nov-1985 text_change 22-Jun-1999
CAccession A01855 A24744 A25384 A22210
S56178
RJacobs, K. Shoemaker, C. Rudersdorf, R.
Neill, S.D. Kaufman, R.J. Mufson, A. Seehra,
J. Jones, S.S. Hewick, R. Fritsch, E.F.
Kawakita, M. Shimizu, T. Miyake, T.
Nature 313, 806-810, 1985
ATitle Isolation and characterization of
genomic and cDNA clones of human erythropoietin.
AReference number A01855 MUID85137899
AAccession A01855
AMolecule type mRNA DNA
AResidues 1-193
ACross-references GBX02157 GBX02158
RLin, F.K. Suggs, S. Lin, C.H. Browne, J.K.
Smalling, R. Egrie, J.C. Chen, K.K. Fox, G.M.
Martin, F. Stabinsky, Z. Badrawi, S.M. Lai,
P.H. Goldwasser, E.
Proc. Natl. Acad. Sci. U.S.A. 82, 7580-7584, 1985
ATitle Cloning and expression of the human
erythropoietin gene.
AReference number A24744 MUID86067948
AAccession A24744
AMolecule type DNA

50
PIR (cont.)

AAccession A22210
AMolecule type protein
AResidues 28-29,'X',31-33,'L',35-50,'X',52-53,'D
',55,'G',57
RMatsumoto, S. Ikura, K. Ueda, M. Sasaki, R.
Plant Mol. Biol. 27, 1163-1172, 1995
ATitle Characterization of a human glycoprotein
(erythropoietin) produced in cultured tobacco
cells.
AReference number S56178 MUID95284365
AAccession S56178
AMolecule type protein
AResidues 28-33,'X',35-37
CComment Erythropoietin is produced by kidney
or liver of adult mammals and by liver of fetal
or neonatal mammals.
CGenetics
AGene GDBEPO
ACross-references GDB119110 OMIM133170
AMap position 7q21.3-7q22.1
AIntrons 5/1 53/3 82/3 142/3
CFunction
ADescription the primary inducer of erythrocyte
formation
CSuperfamily erythropoietin
CKeywords erythropoiesis glycoprotein
hormone kidney liver

51
Composite protein sequence db
Different composite db use different primary
sources and different redundancy criteria in
their amalgamation procedures
Redundancy priority criteria
Also called SWall at EBI SWIR SPTrEMBL
Wormpep
52
Composite protein family

The proteins /genes are classified by
superfamily/family according to Blast/Fasta
(homology) results
General
ProtFam PIR
ProtoMap SWISS-PROT
SYSTERS SWISS-PROT and PIR (non redundant)
ProClass PIR and PROSITE
Species specific
HOVERGEN vertebrates
HOBACGEN bacteria
COG complete organism genome

53
ProtoMap example
54
ProtoMap (cont.)
55
Database 4 protein domain/family

Contains biologically significant pattern /
profiles/ HMM formulated in such a way that,
with appropriate computional tools, it can
rapidly and reliably determine to which known
family of proteins (if any) a new sequence
belongs to
-gt tools to identify what is the function of
uncharacterized proteins translated from genomic
or cDNA sequences ( functional diagnostic )

56
Protein domain/family

Most proteins have modular structure
Estimation 3 domains / protein
Domains (conserved sequences or structures) are
identified by multi sequence alignments
Domains can be defined by different methods
Pattern (regular expression) used for very
conserved domains
Profiles (weighted matrices) two-dimensional
tables of position specific match-, gap-, and
insertion-scores, derived from aligned sequence
families used for less conserved domains
Hidden Markov Model (HMM) probabilistic models
an other method to generate profiles.

57
Some statistics

15 most common protein domains for H. sapiens
(Incomplete)
Immunoglobulin and major histocompatibility
complex domain
Eukaryotic protein kinase
Zinc finger, C2H2 type
Rhodopsin-like GPCR superfamily
Src homology 3 (SH3) domain
RNA-binding region RNP-1 (RNA recognition motif)
Fibronectin type III domain
Pleckstrin homology (PH) domain
Homeobox domain
Major histocompatibility complex protein, Class
I
EF-hand family
EGF-like domain
RING finger
Cadherin domain
PDZ domain (also known as DHR or GLGF)
Serine proteases, trypsin family
http//www.ebi.ac.uk/proteome/HUMAN/interpro/top15
d.html

58
Protein domain/family db

Secondary databases are the fruit of analyses of
the sequences found in the primary db
Either manually curated (i.e. PROSITE, Pfam,
etc.) or automatically generated (i.e. ProDom,
DOMO)
Some depend on the method used to detect if a
protein belongs to a particular domain/family
(patterns, profiles, HMM)

59
Protein domain/family db
60
Prosite

Created in 1988 (SIB)
Contains functional domains fully annotated,
based on two methods patterns and profiles
Entries are deposited in PROSITE in two distinct
files
Pattern/profiles with the lists of all matches in
the parent version of SWISS-PROT
Documentation
Aug 2000 contains 1064 documentation entries
that
describe 1424 different patterns, rules and
profiles/matrices.

61
Prosite (pattern) example
ID EPO_TPO PATTERN. AC PS00817 DT
OCT-1993 (CREATED) NOV-1995 (DATA UPDATE)
JUL-1998 (INFO UPDATE). DE Erythropoietin /
thrombopoeitin signature. PA P-x(4)-C-D-x-R-LIV
M(2)-x-KR-x(14)-C. NR /RELEASE38,80000 NR
/TOTAL14(14) /POSITIVE14(14) /UNKNOWN0(0)
/FALSE_POS0(0) NR /FALSE_NEG0
/PARTIAL1 CC /TAXO-RANGE??E??
/MAX-REPEAT1 CC /SITE3,disulfide
/SITE11,disulfide DR P48617, EPO_BOVIN , T
P33707, EPO_CANFA , T P33708, EPO_FELCA , T DR
P01588, EPO_HUMAN , T P07865, EPO_MACFA , T
Q28513, EPO_MACMU , T DR P07321, EPO_MOUSE ,
T P49157, EPO_PIG , T P29676, EPO_RAT , T
DR P33709, EPO_SHEEP , T P42705, TPO_CANFA ,
T P40225, TPO_HUMAN , T DR P40226, TPO_MOUSE
, T P49745, TPO_RAT , T DR P42706, TPO_PIG
, P DO PDOC00644 //
Diagnostic performance
List of matches
62
Prosite (profile) example

PROSITE PS50097
ID BTB MATRIX.
AC PS50097
DT DEC-1999 (CREATED) DEC-1999 (DATA UPDATE)
DEC-1999 (INFO UPDATE).
DE BTB domain profile.
MA /GENERAL_SPEC ALPHABET'ABCDEFGHIKLMNPQRSTVW
YZ' LENGTH67
MA /DISJOINT DEFINITIONPROTECT N16 N262
MA /NORMALIZATION MODE1 FUNCTIONLINEAR
R1.9751 R2.02068202 TEXT'-LogE'
MA /CUT_OFF LEVEL0 SCORE363 N_SCORE8.5
MODE1 TEXT'!'
MA /CUT_OFF LEVEL-1 SCORE267 N_SCORE6.5
MODE1 TEXT'?'
MA /DEFAULT D-20 I-20 B1-50 E1-50
MI-105 MD-105 IM-105 DM-105 MM1 M0-2
MA /I B10 BI-105 BD-105
MA /M SY'C' M-6,-10,28,-14,-9,-15,-20,-14,-1
9,-15,-17,-14,-8,-19,-14,-15,0,0,-9,-32,-17,-12
MA /M SY'D' M-16,41,-28,53,15,-34,-11,-1,-33
,0,-27,-25,21,-11,0,-8,2,-6,-26,-38,-19,7
MA /M SY'V' M2,-23,-8,-28,-24,-1,-24,-25,16,
-20,7,6,-20,-25,-23,-20,-10,-4,24,-23,-9,-24
MA /M SY'T' M-2,-13,-18,-19,-13,-7,-24,-19,6
,-8,-2,1,-11,-17,-11,-10,-1,10,10,-24,-6,-13
MA /M SY'L' M-11,-30,-22,-33,-24,15,-32,-23,
25,-29,35,17,-26,-27,-23,-22,-24,-9,16,-17,3,-24
MA /M SY'V' M0,-11,-18,-13,-10,-12,-20,-13,1
,-6,-4,2,-10,-19,-6,-7,-4,-2,8,-25,-9,-9

63
Prosite (profile) example (cont.)

MA /M SY'T' M-3,3,-16,1,-3,-18,-12,-9,-20,-6
,-19,-15,2,-7,-6,-6,10,15,-13,-27,-12,-5
MA /M SY'G' M-1,1,-25,2,-9,-26,31,-12,-32,-1
0,-26,-18,4,-17,-12,-10,1,-12,-24,-25,-22,-11
MA /M SY'E' M-9,3,-24,4,13,-25,-16,-1,-24,13
,-21,-13,3,-9,6,13,-3,-6,-20,-27,-13,8
MA /M SY'I' M-6,-21,-18,-25,-21,-2,-29,-21,2
1,-21,14,10,-19,-24,-17,-19,-13,-3,19,-23,-3,-20
MA /M SY'E' M-4,3,-23,3,4,-18,-11,-7,-17,-1,
-18,-13,3,-9,-1,-5,1,-4,-14,-25,-11,1
MA /M SY'I' M-8,-25,-23,-27,-20,1,-30,-21,21
,-20,18,12,-22,-18,-18,-18,-18,-7,16,-21,-1,-20
MA /M SY'P' M-6,0,-24,2,1,-22,-13,-8,-21,-2,
-23,-15,1,14,-4,-7,3,2,-19,-31,-18,-3
MA /M SY'E' M-7,1,-27,4,11,-24,-15,-4,-19,2,
-18,-11,0,-1,6,-1,-2,-6,-19,-25,-14,7
MA /I E10 IE-105 DE-105
NR /RELEASE39,87397
NR /TOTAL46(44) /POSITIVE45(43)
/UNKNOWN1(1) /FALSE_POS0(0)
NR /FALSE_NEG0 /PARTIAL0
CC /TAXO-RANGE??E?V /MAX-REPEAT2
DR O14867, BAC1_HUMAN, T P97302, BAC1_MOUSE,
T P97303, BAC2_MOUSE, T
DR P41182, BCL6_HUMAN, T P41183, BCL6_MOUSE,
T Q01295, BRC1_DROME, T
DR Q01296, BRC2_DROME, T Q01293, BRC3_DROME,
T Q28068, CALI_BOVIN, T
DR Q13939, CALI_HUMAN, T Q08605, GAGA_DROME,
T Q01820, GCL1_DROME, T
DR P10074, HKR3_HUMAN, T Q04652, KELC_DROME,
T P42283, LOLL_DROME, T

64
PRINTS

Compendium of protein motif fingerprints
Most protein families are characterized by
several conserved motifs
Fingerprint set of motif(s) (simple or
composite, such as multidomains) signature of
family membership
True family members exhibit all elements of the
fingerprint, while subfamily members may possess
only a part

65
ProDom

consists of an automated compilation of
homologous domain alignment (procedure based on
PSI-BLAST searches)
Updating problem !
Last ProDom update February 7, 2000
built from SWISS-PROT 38 TREMBL TREMBL
updates - October 22, 1999

66
ProDom example
Your query
67
Protein domain/family Composite databases

Example InterPro
Unification of PROSITE, PRINTS, Pfam and ProDom
into an integrated resource of protein families,
domains and functional sites
Single set of documents linked to the various
methods
Will be used to improve the functional annotation
of SWISS-PROT (classification of unknown
protein)
This release contains 3052 entries, representing
574 domains, 2418 families, 46 repeats and 14
post-translational modification sites.

68
InterPro example

IPR001323
Name
Erythropoietin/thrombopoeitin
Type
Family
Abstract
Erythropoietin,
a plasma glycoprotein, is the primary
physiological mediator of erythropoiesis 1 . It
is involved in
the regulation
of the level of peripheral erythrocytes by
stimulating the differentiation of erythroid
progenitor cells,
found in the
spleen and bone marrow, into mature erythrocytes
2 . It is primarily produced in adult kidneys
and
foetal liver,
acting by attachment to specific binding sites on
erythroid progenitor cells, stimulating their
differentiation
3 . Severe kidney dysfunction causes reduction
in the plasma levels of erythropoietin, resulting
in
chronic anaemia
- injection of purified erythropoietin into the
blood stream can help to relieve this type of
anaemia.
Levels of
erythropoietin in plasma fluctuate with varying
oxygen tension of the blood, but androgens and
prostaglandins
also modulate the levels to some extent 3 .
Erythropoietin glycoprotein sequences are well
conserved, a
consequence of which is that the hormones are
cross-reactive among mammals, i.e. that from one
species, say
human, can stimulate erythropoiesis in other
species, say mouse or rat 4 .
Thrombopoeitin
(TPO), a glycoprotein, is the mammalian hormone
which functions as a megakaryocytic lineage
specific growth
and differentiation factor affecting the
proliferation and maturation from their committed
progenitor

69
InterPro example

...
Examplelist
P33708
P33709
P49745
view matches for
the examples
Publications
1. Shoemaker
C.B., Mitsock L.D. 849-858 (1986)
2. Takeuchi M.,
Takasaki S., Miyazaki H., Kato T., Hoshi S.,
Kochibe N., Kobata A. J. Biol. Chem. 263
3657-3663 (1988)
3. Lin F.K., Lin
C.H., Lai P.H., Browne J.K., Egrie J.C., Smalling
R., Fox G.M., Chen K.K., Castro M., Suggs
S. Gene 44
201-209 (1986)
4. Nagao M.,
Suga H., Okano M., Masuda S., Narita H., Ikura
K., Sasaki R.
Nucleotide
sequence of rat erythropoietin.
1171 99-102
(1992)
Children
IPR003013
Signatures
PROSITE PS00817
EPO_TPO

70
Databases 5 mutation/polymorphism

Contain informations on sequence variations that
are linked or not to genetic diseases
Mainly human but OMIA - Online Mendelian
Inheritance in Animals
General db
OMIM
HMGD - Human Gene Mutation db
SVD - Sequence variation db
HGBASE - Human Genic Bi-Allelic Sequences db
dbSNP - Human single nucleotide polymorphism
(SNP) db
Disease-specific db most of these databases are
either linked to a single gene or to a single
disease
p53 mutation db
ADB - Albinism db (Mutations in human genes
causing albinism)
Asthma and Allergy gene db
.

71
Mutation/polymorphisms definitions

SNPs single nucleotide polymorphisms
c-SNPs coding single nucleotide polymorphisms
(Single Nucleotide Polymorphisms within cDNA
sequences)
SAPs single amino-acid polymorphisms
Missense mutation -gt SAP
Nonsense mutation -gt STOP
Insertion/deletion of nucleotides -gt frameshift
! Numbering of the mutation depends on the db (aa
no 1 is not necessary the initiator Met !)

72
Mutation/polymorphisms

dbSNP consortium http//snp.cshl.org/
Bayer, Roche, IBM, Pfizer, Novartis, Motorola
Mission develop up to 300,000 SNPs distributed
evenly throughout the human genome and make the
informations related to these SNPs available to
the public without intellectual property
restrictions. The project started in April 1999
and is anticipated to continue until the end of
2001.
dbSNP at NCBI http//www.ncbi.nlm.nih.gov/SNP/
Collaboration between the National Human Genome
Research Institute and the National Center for
Biotechnology Information (NCBI)
Mission central repository for both single base
nucleotide subsitutions and short deletion and
insertion polymorphisms
Aug 24, 2000 , dbSNP has submissions for 803557
SNPs.
Chromosome 21 dbSNP http//csnp.isb-sib.ch/
A joint project between the Division of Medical
Genetics of the
University of Geneva Medical School and the SIB
Mission comprehensive cSNP (Single Nucleotide
Polymorphisms within cDNA sequences) database and
map of chromosome 21

73
Mutation/polymorphisms

Very heterogeneous format
Generally modest size
There are initiatives to standardize and to unify
these databases (SVD - Sequence Variation
Database project at EBI HMutDB)

74
Databases 6 proteomics

Contain informations obtained by 2D-PAGE master
images of the gels and description of identified
proteins
Examples SWISS-2DPAGE, ECO2DBASE, Maize-2DPAGE,
Sub2D, Cyano2DBase, etc.
Format composed of image and text files
Most 2D-PAGE databases are federated and
use SWISS-PROT as a master index
There is currently no protein Mass Spectrometry
(MS) database (not for long)

75
Databases 7 3D structure

Contain the spatial coordinates of macromolecules
whose 3D structure has been obtained by X-ray or
NMR studies
Proteins represent more than 90 of available
structures (others are DNA, RNA, sugars, virus,
complex protein/DNA)
PDB (Protein Data Bank), SCOP (structural
classification of proteins (according to the
secondary structures)), BMRB (BioMagResBank RMN
results)
Future Homology-derived 3D structure db.

76
PDB

Protein Data Bank, managed by RCSB
Currently there are 13000 structures for about
4000 different molecules, but far less protein
family !
There are also databases that contain data
derived from PDB. Examples HSSP
(homology-derived secondary structure of
proteins), SWISS-3DIMAGE (images)

Restriction enzyme
77
PDB example

HEADER LYASE(OXO-ACID)
01-OCT-91 12CA 12CA 2
COMPND CARBONIC ANHYDRASE /II (CARBONATE
DEHYDRATASE) (/HCA II) 12CA 3
COMPND 2 (E.C.4.2.1.1) MUTANT WITH VAL 121
REPLACED BY ALA (/V121A) 12CA 4
SOURCE HUMAN (HOMO SAPIENS) RECOMBINANT
PROTEIN 12CA 5
AUTHOR S.K.NAIR,D.W.CHRISTIANSON
12CA 6
REVDAT 1 15-OCT-92 12CA 0
12CA 7
JRNL AUTH S.K.NAIR,T.L.CALDERONE,D.W.CHRI
STIANSON,C.A.FIERKE 12CA 8
JRNL TITL ALTERING THE MOUTH OF A
HYDROPHOBIC POCKET. 12CA 9
JRNL TITL 2 STRUCTURE AND KINETICS OF
HUMAN CARBONIC ANHYDRASE 12CA 10
JRNL TITL 3 /II MUTANTS AT RESIDUE
VAL-121 12CA 11
JRNL REF J.BIOL.CHEM.
V. 266 17320 1991 12CA 12
JRNL REFN ASTM JBCHA3 US ISSN 0021-9258
071 12CA 13
REMARK 1
12CA 14
REMARK 2
12CA 15
REMARK 2 RESOLUTION. 2.4 ANGSTROMS.
12CA 16
REMARK 3
12CA 17
REMARK 3 REFINEMENT.
12CA 18
REMARK 3 PROGRAM PROLSQ
12CA 19

78
PDB (cont.)

SHEET 3 S10 PHE 66 PHE 70 -1 O ASN
67 N LEU 60 12CA 68
SHEET 4 S10 TYR 88 TRP 97 -1 O PHE
93 N VAL 68 12CA 69
SHEET 5 S10 ALA 116 ASN 124 -1 O HIS
119 N HIS 94 12CA 70
SHEET 6 S10 LEU 141 VAL 150 -1 O LEU
144 N LEU 120 12CA 71
SHEET 7 S10 VAL 207 LEU 212 1 O ILE
210 N GLY 145 12CA 72
SHEET 8 S10 TYR 191 GLY 196 -1 O TRP
192 N VAL 211 12CA 73
SHEET 9 S10 LYS 257 ALA 258 -1 O LYS
257 N THR 193 12CA 74
SHEET 10 S10 LYS 39 TYR 40 1 O LYS
39 N ALA 258 12CA 75
TURN 1 T1 GLN 28 VAL 31 TYPE VIB
(CIS-PRO 30) 12CA 76
TURN 2 T2 GLY 81 LEU 84 TYPE
II(PRIME) (GLY 82) 12CA 77
TURN 3 T3 ALA 134 GLN 137 TYPE I
(GLN 136) 12CA 78
TURN 4 T4 GLN 137 GLY 140 TYPE I
(ASP 139) 12CA 79
TURN 5 T5 THR 200 LEU 203 TYPE VIA
(CIS-PRO 202) 12CA 80
TURN 6 T6 GLY 233 GLU 236 TYPE II
(GLY 235) 12CA 81
CRYST1 42.700 41.700 73.000 90.00 104.60
90.00 P 21 2 12CA 82
ORIGX1 1.000000 0.000000 0.000000
0.00000 12CA 83
ORIGX2 0.000000 1.000000 0.000000
0.00000 12CA 84
ORIGX3 0.000000 0.000000 1.000000
0.00000 12CA 85
SCALE1 0.023419 0.000000 0.006100
0.00000 12CA 86

79
Databases 8 metabolic

Contain informations that describe enzymes,
biochemical reactions and metabolic pathways
ENZYME and BRENDA nomenclature databases that
store informations on enzyme names and reactions
Examples of metabolic databases EcoCyc
(specialized on Escherichia coli), KEGG, EMP/WIT
Usualy these databases are tightly coupled with
query software that allows the user to visualise
reaction schemes.

80
Databases 9 bibliographic

Bibliographic reference databases contain
citations and abstract informations of published
life science articles
Example Medline
Other more specialized databases also exist
(example Agricola).

81
Medline

MEDLINE covers the fields of medicine, nursing,
dentistry, veterinary medicine, the health care
system, and the preclinical sciences
more than 4,000 biomedical journals published in
the United States and 70 other countries
Contains over 10 million citations since 1966
until now
Contains links to biological db and to some
journals
New records are added to PreMEDLINE daily!
Many papers not dealing with human are not in
Medline !
Before 1970, keeps only the first 10 authors !
Not all journals have citations since 1966 !

82
Medline/Pubmed

PubMed is developed by the National Center for
Biotechnology Information (NCBI)
PubMed provides access to bibliographic
information such as MEDLINE, PreMEDLINE,
HealthSTAR, and to integrated molecular biology
databases (composite db)
PMID 10923642 (PubMed ID), UI 20378145 (Medline
ID)

83
Databases 10 others

There are many databases that cannot be
classified in the categories listed previously
Examples ReBase (restriction enzymes), TRANSFAC
(transcription factors), O-GLYCBASE (O-linked
sugars), Protein-protein interactions db (DIR),
biotechnology patents db, etc.
As well as many other resources concerning any
aspects of macromolecules and molecular biology.

84
Proliferation of databases

What is the best db for sequence analysis ?
Which does contain the highest quality data ?
Which is the more comprehensive ?
Which is the more up-to-date ?
Which is the less redundant ?
Which is the more indexed (allows complex
queries) ?
Which Web server does respond most quickly ?
.??????

85
Some important practical remarks

Databases many errors (automated annotation) !
Not all db are available on all servers
The update frequency is not the same for all
servers creation of db_new between releases
(exemple EMBLnew TrEMBLnew.)
Some servers add automatically useful
cross-references to an entry (implicit links) in
addition to already existing links (explicit
links)

86
Database retrieval tools

Sequence Retrieval System (SRS, Europe) allows
any flat-file db to be indexed to any other
allows to formulate queries across a wide range
of different db types via a single interface,
without any worry about data structure, query
languages
Entrez (USA) less flexible than SRS but exploits
the concept of neighbouring , which allows
related articles in different db to be linked
together, whether or not they are
cross-referenced directly
ATLAS specific for macromolecular sequences db
(i.e. NRL-3D)
.

87
More informations about SWISS-PROT
88
The golden goals of SWISS-PROT

Annotated / curated
Complete
Non-redundant
Highly cross-referenced
Available from a variety of servers and through
sequence analysis software tools
Associated with wide range of documentation
Review Protein sequence databases
R. Apweiler (2000), Adv. in protein chemistry,
54, 31-70

89
SWISS-PROT species

6840 different species
20 species represent about 45 of all sequences
in the database
5000 species are only represented by one to
three sequences. In most cases, these are
sequences which were obtained in the context of a
phylogenetic study

90
SWISS-PROT cross-references

SWISS-PROT was the first database with
cross-references.
Explicitly cross-referenced to 34 databases
Cross-ref to DNA (EMBL/GenBank/DDBJ),
3D-structure (PDB), literature (Medline), genomic
(MIM, MGD, FlyBase, SGD, SubtiList, etc.), 2D-gel
(SWISS-2DPAGE), specialized db (PROSITE,
TRANSFAC)
Implicitly cross-referenced to additional db on
the WWW (GeneCards, PRODOM, etc.)

91
Annotations

Function(s)
Post-translational modifications (PTM)
Domains
Quaternary structure
Similarities
Diseases, mutagenesis
Conflicts, variants
Cross-references

92
A Swiss-Prot entry
93
Sprot entry (cont.)
94
Sprot entry (cont.)
95
Sprot entry (cont.)
96
Sprot entry (cont.)
97
Future for human proteins

Original estimate from 70000 to 100000 genes
Incyte recently announced an estimation of
140000 genes
More recent estimations give about 30000 to
40000 genes
C. elegans and Drosophila have 15000 genes.
There was two sets of genome duplication in the
evolutionary history leading to vertebrates. Very
roughly it means that
Human genes60000 genes - losses new genes
But more than 1 million proteins !
(due to PTM, alternative products, variants)
http//www.ensembl.org/genesweep.html

98
Genesweep
http//www.ensembl.org/genesweep.html
99
What after genomes?

Proteome projects are an essential tool for the
understanding of real proteins
There will be a flood of characterization data
(MS, 2D) that will be the equivalent of ESTs at
the protein level
Protein databases are going to be more and more
important for new biological studies

100
(No Transcript)
101
Databases in GCG