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=== PsaA protein ===
=== PsaA protein ===
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Zinc in excess has significant toxicity to bacteria because it is an important innate defense mechanism. There are many Zinc molecules in the human body. Manganese is important for the virulence, growth and proliferation of ''Streptococcus pneumoniae''. Zinc could compete for Manganese binding. However Manganese has more affinity for PsaA than Zinc but Zinc is not transported by the ABC-transporter. Zinc competition reduces intracellular Manganese resulting in up-regulation of PsaBCA expression. <ref>PMID:22072971</ref>
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Zinc in excess has a significant toxicity to bacteria because it is an important innate defense mechanism. There are many Zinc molecules in the human body. Manganese is important for the virulence, growth and proliferation of ''Streptococcus pneumoniae''. Zinc could compete for Manganese binding. However Manganese has more affinity for PsaA than Zinc but Zinc is not transported by the ABC-transporter. Zinc competition reduces intracellular Manganese resulting in up-regulation of PsaBCA expression. <ref>PMID:22072971</ref>
[[Image:PsaA dans ABC transporteur.jpg |500px| Structure of ABC-transporter <ref>http://www.latrobe.edu.au/biochemistry-and-genetics/research/maher/psabca-manganese-uptake-by-streptococcus-pneumoniae</ref>]]
[[Image:PsaA dans ABC transporteur.jpg |500px| Structure of ABC-transporter <ref>http://www.latrobe.edu.au/biochemistry-and-genetics/research/maher/psabca-manganese-uptake-by-streptococcus-pneumoniae</ref>]]

Revision as of 17:55, 27 January 2017

User: Julie Langlois/PsaA


NCBI Accession: P42363.1

Uniprot Accesion: POA4G2

PDB ID: 3ZK7

3D structure of PsaA in the metal-free, open state

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