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Diapositive 1

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the major Porins of Corynebacterium glutamicum. By. Parthasarathi Rath. Principal Investigator: ... Prof A. Milon, NMR Spectroscopy, IPBS/CNRS, Toulouse, France ... – PowerPoint PPT presentation

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Title: Diapositive 1


1
PhD project Solution state NMR structure
determination of PorA and PorH, the major Porins
of Corynebacterium glutamicum
By Parthasarathi Rath
  • Principal Investigator
  • Prof A. Milon, NMR Spectroscopy, IPBS/CNRS,
    Toulouse, France
  • In Collaboration With
  • Dr F. Bernhard, CBMR, Inst. Biophys. Chem.,
    Frankfurt, Germany
  • Dr M. Daffé, IPBS/CNRS, Toulouse, France

2
Objectives
  • Expression purification in Corynebacterium
    glutamicum
  • 2. Expression purification in cell free
    expression system
  • 3. Functional reconstitution in detergent
    micelles and in lipid bilayers
  • (biophysical and biochemical studies,
    oligomerisation states
  • and structure function relationship)
  • 4. 3D structure resolution of PorA and PorH by
    solution state NMR
  • 5. 3D structure in bilayers by solid state NMR

3
Introduction
  • Corynebacterium glutamicum
  • member of the mycolic-acid containing
    actinomycetes
  • aerobic and non-sporulating
  • genes are orthologous to number of human
    pathogens, such as
  • Corynebacterium diphtheriae, Mycobacterium
    tuberculosis and Mycobacterium leprae
  • (can be targeted as anti-tubercular agent)
  • industrial production of L-glutamate (
    appetite enhancer), L-lysine (animal food
    additive)
  • at the rate of about 1 Megaton/year
  • Challenges
  • Amino acid efflux properties ?
  • Understanding cell wall complexity ?

4
Cell Envelope of Gram-Negative, Gram-Positive and
Corynebacterineae
Porins
Lipoteichoic and Teichoic acids
Corynebacterineae
Gram-negative
Gram-positive
  • Mycolic acids
  • long chain a-alkyl, ß-hydroxyl fatty acids
  • play a crucial role in determining the
    fluidity
  • and permeability of the cell wall
  • Porins
  • major channel-forming proteins
  • ion-selective passage of small hydrophillic
  • molecules (substrates / products /
    antibiotics)
  • important for aminoacid excretion ??

5
Type of Porins
  • PorA
  • 45aa (5KDa) long polypeptide
  • cation-selective channel G 5,5nS in 1M KCl
  • major hydrophilic pathway, transport of
    antibiotics (Amp, Kan, Stp )
  • no N-terminal extension (Post-translationally
    modified ??)
  • (Reference J. Bacteriology, 2003,185,
    p.4779-4786)
  • 2) PorH
  • 57aa long polypeptide (12KDa dimer)
  • cation-selective channel G 2,5nS in 1M KCl
  • co-transcribed with PorA
  • no N-terminal extension (the export pathway ??)
  • (Reference BBA, 2005, 1715, p. 25-36)

Only PorB structure is known PDB no 2VQG
  • 3) PorB and PorC
  • Anion-selective channels with N-terminal
    extension
  • (Reference Mol. Microbiol. 2003, 50, p.
    1295-1308)

6
First objective Expression and Purification of
PorA and PorH(Cloning and Sequencing)
Vector constructions
pK18 E.coli based plasmid pBL1 C.glutamicum
plasmid
  • pXMJ19
  • pTAC (promotor)
  • laq Iq
  • CmR (resistance to chloramphenicol)
  • MCS (multiple cloning site)

PorA N-His
n-MASRGSHHHHHHHHIEGRENVYEFLGNLDVLSGSGLIGYVFDFLGASS
KWAGAVADLIGLLG -c
PorH C-His n-DLSLLKETLGNYETFGGNIGTALQSIPTLLDSILNFF
DNFGDLADTTGENLDNFSSIEGRASRGSHHHHHHHH -c
IEGR Factor Xa cleavage site
Expression
PorA / PorH Toxic for E. coli C.
glutamicum - PorA/-PorH
  • Homologous Expression
  • Post-translational modification (if any)

7
Extraction and Purification
TritonX-100
CHCl3 CH3OH
Yield/L culture 12mg PorA 4mg PorH
Yield/ L culture 11.2mg PorA
7.6mg PorH
8
Cell Free SynthesisDr. Frank Bernhard. CBMR,
Frankfurt
  • Low expression level in E. coli
  • Toxic effects
  • Inefficient transport

Expression PorA / PorH Toxic for E. coli
Reference Proteomics 2008, 8, 3933-3946
9
Prospectives
  • Express, Label (13C / 15N) in Minimal Medium for
    NMR
  • To characterize the purified protein in MALDI-TOF
  • in-vitro synthesis of pET28a-PorA / -PorH
    constructs

10
Thanks
  • Prof. Alain Milon, IPBS/CNRS, Toulouse
  • (NMR and protein - membrane interactions)
  • Prof J. Czaplicki
  • Dr P. Demange
  • Dr V. Gervais
  • Dr I. Muller
  • Dr V. Reat
  • Dr O. Saurel
  • P. Ramos

Future Collaborator Dr F.
Bernhard, CBMR, Frankfurt
  • Dr M. Daffé, IPBS/CNRS, Toulouse
  • (Mycobacterial envelopes structure,
    biosynthesis and functions)
  • Dr M. Tropis
  • Emilie Huc

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