Abstract

The build-up of greenhouse gases in our atmosphere has, and will continue to, lead to a steady increase in the global temperature. A way to halt the further atmospheric accumulation of greenhouses gases, particularly carbon dioxide, is through manipulation of the natural carbon-sequestering mechanisms of aquatic cyanobacteria. One significant factor limiting carbon sequestration in these organisms is the low bioavailability of iron. For the acquisition of bicarbonate and iron, cyanobacteria employ high-affinity ATP-binding cassette (ABC) transporters. These ABC transporters are composed of a periplasmic solute-binding lipoprotein, a cytoplasmic-membrane spanning permease, and an ATPase that powers solute transport. A combination of x-ray crystallography, biochemical and molecular biology techniques will be used to examine both the molecular basis of substrate specificity and transport regulation in the bicarbonate CmpABCD, and the ferric iron FutABC transporters of Synechocystis sp PCC 6803. X-ray crystal structures of the CmpA, CmpC and CmpD proteins will be pursued, as well as a biochemical characterization of the unique multi-domain CmpC protein that is involved in the regulation of bicarbonate uptake. Both thermodynamic and enzymatic techniques will be employed to investigate the interactions between the ATPase domains of CmpC and CmpD. The FutABC transporter will be used to ask the question of whether the membrane permease and ATPase components of ABC transporters plays a role in solute recognition. The solute-binding specificity of the ferric-binding protein FutA1 will be altered in order to test whether the FutBC machinery can accept alternate metal ions. These experiments will involve genetic manipulation of Synechocystis for the purpose of testing metal ion acquisition through FutBC. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Postdoctoral Individual National Research Service Award (F32)
Project #
1F32GM078800-01
Application #
7155354
Study Section
Special Emphasis Panel (ZRG1-F04B-A (20))
Program Officer
Flicker, Paula F
Project Start
2006-09-29
Project End
2008-09-28
Budget Start
2006-09-29
Budget End
2007-09-28
Support Year
1
Fiscal Year
2006
Total Cost
$45,976
Indirect Cost

  Institution

Name
Donald Danforth Plant Science Center
Department
Type
DUNS #
044193006
City
St. Louis
State
MO
Country
United States
Zip Code
63132

  Publications

Martens, Eric C; Koropatkin, Nicole M; Smith, Thomas J et al. (2009) Complex glycan catabolism by the human gut microbiota: the Bacteroidetes Sus-like paradigm. J Biol Chem 284:24673-7
Koropatkin, Nicole; Martens, Eric C; Gordon, Jeffrey I et al. (2009) Structure of a SusD homologue, BT1043, involved in mucin O-glycan utilization in a prominent human gut symbiont. Biochemistry 48:1532-42
Koropatkin, Nicole M; Martens, Eric C; Gordon, Jeffrey I et al. (2008) Starch catabolism by a prominent human gut symbiont is directed by the recognition of amylose helices. Structure 16:1105-15
Koropatkin, Nicole; Randich, Amelia M; Bhattacharyya-Pakrasi, Maitrayee et al. (2007) The structure of the iron-binding protein, FutA1, from Synechocystis 6803. J Biol Chem 282:27468-77
Koropatkin, Nicole M; Koppenaal, David W; Pakrasi, Himadri B et al. (2007) The structure of a cyanobacterial bicarbonate transport protein, CmpA. J Biol Chem 282:2606-14