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TRANSLATION- in Prokaryotes
SONIA JOHN
I M.Sc. Zoology
Mar Ivanios College
INTRODUCTION
• A well-conserved process among prokaryotes and eukaryotes.
• Protein synthesis is the final stage of gene expression .
• The genetic message transcribed to mRNA is translated into
protein by a complex cellular machinery. Additional
processing and assembly often required to modify the
proteins.
• Occurs in 3 stages:
initiation, elongation & termination
TOOLS OF TRANSLATION
• Mainly :Ribosomes, tRNA
• mRNA, Initiation factors, elongation factors,
termination factors, amino acids etc
RIBOSOME
• Protein synthesising factories of the cell.
• 70S & 80S
• Structure: A site, P site & E site. And also an mRNA binding
site. The mRNA-binding site binds a sequence near the 5
prime end of the mRNA, placing the mRNA in the proper
position for the translation of its first codon .
The binding sites are all located at or near the interface
between the large and small subunits
.
Transfer-RNA
• tRNA molecules contain
1) three major loops, a 3 prime terminal sequence of CCA
(where the appropriate amino acid can be attached by an ester
bond). etc
• Clover Leaf Model
PROCESS OF TRANSLATION
• A.A is activated by Rn with RNA(ATP) to form activated A.A.
• The activated A.A joined to the 3 prime terminus of tRNA to
form amino acyl tRNA (catalyzed by aminoacyltRNA
synthetase)
• Messenger RNA brings polypeptide-coding information to the
ribosome.
INITIATION
• In prokaryotes, 70S ribosome.
• Initiation starts with interaction of 30S subunit
with an mRNA mol & 3 IFs
• In prokaryotes, protein synthesis initiated with a modified
methionine residue i.e.. N-formylmethionine-tRNA
• Chain initiation begins with the formation of 2 complexes:
• 1.IF-2 & N-formylmet.TRNA
• mRNA,30s subunit,IF-3
• Prokaryotic mRNAs contains a consensus seq -ShineDalgarno
Sequence.
• Shine- dalgarno seq is complementary to a seq of nucleotides
at 3prime end of ribosomal rna of the 30 S subunit.
• Interaction b/w these complementary seq enhances the
attachment of the 30 S subunit to the AUG initiator codon.
• Both the complexes combine with each other with IF-1 and 1
mol of GTP
• 50 S subunit gets added to the complex structure. IF-3 is
released. The addition of50S subunit utilizes GTP which in
turn triggers the release of IF-1 and IF-2
• Addition of 50S to the complex,positions N-formyl met tRNA
in the P site directly with the anticodon of the tRNA aligned
with AUG codon of mRNA
• With the AUG initiatior codon positioned in the P site, 2d
codon in the mRNA positions in such a way that it
corresponds to the incoming aminoacyl-tRNA in the A -site
CHAIN ELONGATION
• Elongation begins with the binding of the second aminoacyl
tRNA at the ribosomal aminoacyl (A) site.
• The tRNA is escorted to the A site by the elongation factor EF-
Tu, which also carries bound GTPs. As the tRNA binds, the
GTPs are hydrolyzed and EF-Tu is released.
• A peptide bond formed b/w the N-f-met-Trna at the P site&
2nd amino acyl tRNA at the A site; catalyzed by the peptidyl
transferase .
•
• Transfer of N-f-met. to aminoacyl-tRNA at A site forming a
peptidyl tRNA at that position and leaving an uncharged
tRNA at the P site
• Peptidyl trna translocated to the P site & uncharged Trna is
translocated to E domain.
• A site unoccupied ; new aminoacyl-TRNA bind to A site
&process continues
CHAIN TERMINATION
• When a stop codon (UAG, UAA, or UGA) arrives at the A site, it is
recognized and bound by a protein release factor. (RFs).2 classes of
RFs: ClassI & Class II. In E.coli 2 Class I RFs are seen- RF-1 ,RF-2
• RFs bind to the termination codon at A site & stimulate hydrolysis
of bond b/w tRNA&polypeptide chain at P site , resulting in release
of complete polypeptide from ribosome.
• Termination is completed by release of mRNA mol from ribosome &
dissociation of ribosomes into its subunits
CONCLUSION
• Genetic information carried in the Mrna seq is translated into
the seq of amino acids in the polypeptide gene products by
intricate macromolecular structures called ribosomes.
• Translation process is very complex, requiring the
participation of many diff RNA and protein molecules
• Transfer RNA molecules serve as adaptors, mediating the
interaction b/w amino acids & codons in mRNA
• Process of translation involves- Initiation , Elongation &
Termination
REFERENCES
• Gerald Karp(2005).Cell and Molecular
Biology.John Wiley and Son.Inc.USA
• Snustad D.P & Simmons,M.J (2002).Principles
of Genetics.John Wiley and Sons.Inc.New York
• http://en.wikipedia.org/Translation
Translation in Prokaryotes

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Translation in Prokaryotes

  • 1. TRANSLATION- in Prokaryotes SONIA JOHN I M.Sc. Zoology Mar Ivanios College
  • 2. INTRODUCTION • A well-conserved process among prokaryotes and eukaryotes. • Protein synthesis is the final stage of gene expression . • The genetic message transcribed to mRNA is translated into protein by a complex cellular machinery. Additional processing and assembly often required to modify the proteins. • Occurs in 3 stages: initiation, elongation & termination
  • 3.
  • 4. TOOLS OF TRANSLATION • Mainly :Ribosomes, tRNA • mRNA, Initiation factors, elongation factors, termination factors, amino acids etc
  • 5. RIBOSOME • Protein synthesising factories of the cell. • 70S & 80S • Structure: A site, P site & E site. And also an mRNA binding site. The mRNA-binding site binds a sequence near the 5 prime end of the mRNA, placing the mRNA in the proper position for the translation of its first codon . The binding sites are all located at or near the interface between the large and small subunits .
  • 6.
  • 7. Transfer-RNA • tRNA molecules contain 1) three major loops, a 3 prime terminal sequence of CCA (where the appropriate amino acid can be attached by an ester bond). etc • Clover Leaf Model
  • 8.
  • 9. PROCESS OF TRANSLATION • A.A is activated by Rn with RNA(ATP) to form activated A.A. • The activated A.A joined to the 3 prime terminus of tRNA to form amino acyl tRNA (catalyzed by aminoacyltRNA synthetase) • Messenger RNA brings polypeptide-coding information to the ribosome.
  • 10. INITIATION • In prokaryotes, 70S ribosome. • Initiation starts with interaction of 30S subunit with an mRNA mol & 3 IFs
  • 11. • In prokaryotes, protein synthesis initiated with a modified methionine residue i.e.. N-formylmethionine-tRNA • Chain initiation begins with the formation of 2 complexes: • 1.IF-2 & N-formylmet.TRNA • mRNA,30s subunit,IF-3 • Prokaryotic mRNAs contains a consensus seq -ShineDalgarno Sequence.
  • 12. • Shine- dalgarno seq is complementary to a seq of nucleotides at 3prime end of ribosomal rna of the 30 S subunit. • Interaction b/w these complementary seq enhances the attachment of the 30 S subunit to the AUG initiator codon.
  • 13. • Both the complexes combine with each other with IF-1 and 1 mol of GTP • 50 S subunit gets added to the complex structure. IF-3 is released. The addition of50S subunit utilizes GTP which in turn triggers the release of IF-1 and IF-2
  • 14. • Addition of 50S to the complex,positions N-formyl met tRNA in the P site directly with the anticodon of the tRNA aligned with AUG codon of mRNA • With the AUG initiatior codon positioned in the P site, 2d codon in the mRNA positions in such a way that it corresponds to the incoming aminoacyl-tRNA in the A -site
  • 15.
  • 16. CHAIN ELONGATION • Elongation begins with the binding of the second aminoacyl tRNA at the ribosomal aminoacyl (A) site. • The tRNA is escorted to the A site by the elongation factor EF- Tu, which also carries bound GTPs. As the tRNA binds, the GTPs are hydrolyzed and EF-Tu is released. • A peptide bond formed b/w the N-f-met-Trna at the P site& 2nd amino acyl tRNA at the A site; catalyzed by the peptidyl transferase . •
  • 17. • Transfer of N-f-met. to aminoacyl-tRNA at A site forming a peptidyl tRNA at that position and leaving an uncharged tRNA at the P site • Peptidyl trna translocated to the P site & uncharged Trna is translocated to E domain. • A site unoccupied ; new aminoacyl-TRNA bind to A site &process continues
  • 18.
  • 19. CHAIN TERMINATION • When a stop codon (UAG, UAA, or UGA) arrives at the A site, it is recognized and bound by a protein release factor. (RFs).2 classes of RFs: ClassI & Class II. In E.coli 2 Class I RFs are seen- RF-1 ,RF-2 • RFs bind to the termination codon at A site & stimulate hydrolysis of bond b/w tRNA&polypeptide chain at P site , resulting in release of complete polypeptide from ribosome. • Termination is completed by release of mRNA mol from ribosome & dissociation of ribosomes into its subunits
  • 20.
  • 21. CONCLUSION • Genetic information carried in the Mrna seq is translated into the seq of amino acids in the polypeptide gene products by intricate macromolecular structures called ribosomes. • Translation process is very complex, requiring the participation of many diff RNA and protein molecules • Transfer RNA molecules serve as adaptors, mediating the interaction b/w amino acids & codons in mRNA • Process of translation involves- Initiation , Elongation & Termination
  • 22. REFERENCES • Gerald Karp(2005).Cell and Molecular Biology.John Wiley and Son.Inc.USA • Snustad D.P & Simmons,M.J (2002).Principles of Genetics.John Wiley and Sons.Inc.New York • http://en.wikipedia.org/Translation