- Carbamoyl phosphate synthetase I
Protein
Name=carbamoyl-phosphate synthetase 1, mitochondrial
caption=
Symbol=CPS1
AltSymbols=
HGNCid=2323
Chromosome=2
Arm=p
Band=
LocusSupplementaryData=
ECnumber=6.3.4.16
OMIM=608307
EntrezGene=1373
RefSeq=NM_001875
UniProt=P31327
PDB=Carbamoyl Phosphate Synthetase I ("E.coli": PDB|1jdb, EC number|6.3.5.5) is a
ligase enzyme located in themitochondria involved in the production of urea. Carbamoyl Phosphate Synthetase I (CPSI) transfers anammonia fromglutamine to a molecule ofbicarbonate that has been phosphorylated by a molecule of ATP. The resulting carbamate is then phosphorylated with another molecule ATP. The resulting molecule of carbamoyl phosphate leaves the enzyme.tructure of Carbamoyl Phosphate Synthetase I
CPSI is a heterodimer with a small subunit and a larger subunit with are about 382 and 1073 amino acid residues in sizeJames B. Thoden‡, Xinyi Hua, et al. “Carbamoyl-phosphate Synthetase: Creation of an Escape Route for Ammonia.” From the ‡Department of Biochemistry, University of Wisconsin, Madison, Wisconsin, 53706-1544 and the §Department of Chemistry, Texas A&M University, College Station, Texas 77843-3012. http://www.jbc.org/cgi/reprint/277/42/39722.pdf] . The small subunit contains one active site for the binding and deamination of glutamine to make ammonia and glutamate. The large subunit contains two active sites, one for the production of carboxyphosphate, and the other for the production of carbamoyl phosphateSUE GLENN POWERS, “Inhibition of Carbamyl Phosphate Synthetase by PI, P5-Di (adenosine 5’) - pentaphosphate EVIDENCE FOR TWO ATP BINDING SITES.” From the Department ofBiochemistry, Cornell University Medical College, New York, New York 10021. http://www.jbc.org/cgi/reprint/252/10/3558] [James B. Thoden, Hazel M. Holden, et al (1997). “Structure of Carbamoyl Phosphate Synthetase: A Journey of 96 Å from Substrate to Product.” Institute for Enzyme Research, Graduate School, and Department of Biochemistry, College of Agriculture, UniVersity of Wisconsin, Madison, Wisconsin 53705, and Department of Chemistry, Texas A&M UniVersity, College Station, Texas 77843. http://pubs.acs.org/cgi-bin/article.cgi/bichaw/1997/36/i21/pdf/bi970503q.pdf] . Within the large subunit there are two domains (B and C) each with an active site of the ATP-grasp family. Connecting the two subunits a tunnel of sorts which directs the ammonia from the small subunit to the large subunitJungwook Kim and Frank M. Raushel (2004). “Perforation of the Tunnel Wall in Carbamoyl Phosphate Synthetase Derails the Passage of Ammonia between Sequential Active Sites.” Department of Chemistry, Texas A&M UniVersity, P.O. Box 30012, College Station, Texas 77842-3012. http://pubs.acs.org/cgi-bin/article.cgi/bichaw/2004/43/i18/pdf/bi049945+.pdf] .
Mechanism of Carbamoyl Phosphate Synthetase I
The overall reaction that occurs in CPSI is:
2ATP + HCO3-- + Glutamine --> 2ADP + Carbamoyl phosphate +
glutamate +Pi This reaction can be thought of occurring in four distinct steps. 1. Bicarbonate is phosphorylated 2. Ammonia is taken off glutamine 3. The ammonia from glutamine attacks the carboxyphosphate resulting in carbamate 4. Carbamate is phosphorylated to give Carbamoyl phosphate
Of these four steps only step two, the deamination of glutamine to get ammonia is known to have actively participating amino acid residues, Cys269 and His353. The other three steps mostly utilize amino acid residue to form hydrogen bonds with substrates. A video of a simplified version of this mechanism is available [http://bcs.whfreeman.com/lehninger/pages/bcs-main.asp?v=chapter&s=18000&n=00010&i=18010.04&o=|00510|00520|00530|00540|00550|00PRS|00010|00020|00030|00040|00050|00060|00070|00080|00090|00100|00110|00120|01000|02000|03000|04000|05000|06000|07000|08000|09000|10000|11000|12000|13000|14000|15000|16000|17000|18000|19000|20000|21000|22000|23000|24000|25000|26000|27000|28000|99000|&ns=0 here]
Recent Mechanism Studies
It has been found that both ATP-binding sites in the large subunit of CPSI are structurally equivalent. A recent study has investigated the interlinking between these two domains (domain B and domain C) and has found evidence that they are coupled. This ATP-binding domain coupling works such that a molecule of ATP binding at one site (domain C) conformationally allows synthesis at the other domain (domain B). If this turns out to be true then the mechanism for carbamoyl phosphate synthesis is significantly altered. Instead of forming carbamoyl phosphate in step 5 (of the included mechanism below) by ejecting ADP it would be formed at step 4 by protonating the alcohol group and then kicking it off as water.MICHAEL KOTH*, BINNUR EROGLU, et al. “Novel mechanism for carbamoyl-phosphate synthetase: A nucleotide switch for functionally equivalent domains.” Department of Biology, Northeastern University, Boston, MA 02115 http://www.pnas.org/cgi/reprint/94/23/12348.pdf?ck=nck] .
Regulation
CPSI is allosterically regulated by purine and pyrimidine nucleotides where the former is allosterically activates the enzyme and the later allosterically inhibits CPSI. Also, it has been found that ornithine is an allosteric activator of CPSI. Increased levels of ammonia also activate CPSI while decreased levels of ATP inhibit CPSI activity. All allosteric binding sites are located in the large subunit of the enzymeALTON MEISTER. “MECHANISM AND REGULATION OF THE GLUTAMINE-DEPENDENT CARBAMYL PHOSPHATE SYNTHETASE OF ESCHERZCHZA COLI.” Department of Biochemistry, Cornell University Medical College, New York, New York 10021] .
Carbamoyl Phosphate Synthetase I and Metabolism
CPSI plays a vital role in protein and nitrogen metabolism. Once ammonia has been brought into the mitochondria via glutamine, or glutamate it is CPSI’s job to add the ammonia to bicarbonate along with a phosphate group to form carbamoyl phosphate. Carbamoyl phosphate is then put into the urea cycle to eventually create urea. Urea can then be transferred back to the
blood stream and to thekidneys for filtration and on to thebladder for excretionDavid Nelson and Michael Cox. “Principles of Biochemistry, fourth edition.” Pgs 666-669] .Health Problems related to Carbamoyl Phosphate Synthetase I
The main problem related to CPSI is genetically based. Sometimes the body doesn’t produce enough CPSI due to a mutation in the genetic code. When this happens the body can’t metabolize proteins and nitrogen as well and this can result in high levels of ammonia in the body. This is dangerous because ammonia is highly toxic to the body and especially the
nervous system and can result inretardation andseizures . For more information check out the article onCarbamoyl phosphate synthetase I deficiency .References
External links
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