Sandbox Reserved 1070

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===Potential for Binding Amino Acids===
===Potential for Binding Amino Acids===
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The exploration of this role for MgtC was first considered because of the ACT domain-like structure of the C-terminal domain. ACT domains commonly bind small amino acids within the cell as a form of regulation.  Yang et al. showed that the structure of the C-terminal domain overlaps significantly with the structure of SerA, a known amino acid-binding ACT domain from ''E. coli''. However, the glycine that is critical for the binding of amino acids in these ACT domains has been substituted in MgtC with a tyrosine, likely abolishing any potential amino acid binding activity
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[[Image:1aligned.png |200 px|right]]
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The exploration of this role for MgtC was first considered because of the ACT domain-like structure of the C-terminal domain.
 +
ACT domains commonly bind small amino acids within the cell as a form of regulation.  Yang et al. showed that the structure
 +
of the C-terminal domain overlaps significantly with the structure of SerA, a known amino acid-binding ACT domain from ''E. coli''. However, the glycine that is critical for the binding of amino acids in these ACT domains has been substituted in MgtC with a tyrosine, likely abolishing any potential amino acid binding activity
===Potential for Chelation===
===Potential for Chelation===

Revision as of 12:45, 9 April 2015

This Sandbox is Reserved from 02/09/2015, through 05/31/2016 for use in the course "CH462: Biochemistry 2" taught by Geoffrey C. Hoops at the Butler University. This reservation includes Sandbox Reserved 1051 through Sandbox Reserved 1080.
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MgtC: A Virulence Factor From Mycobacterium tuberculosis

C-terminal Domain of Mg2+ transport P-type ATPase C (PDB: 2LQJ)

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References

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