Biology:Nicotinamide ribonucleoside uptake transporters

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Short description: Family of transport proteins
Identifiers
SymbolPnuC
PfamPF04973
TCDB4.B.1
OPM superfamily377
OPM protein4qtn

The Nicotinamide Ribonucleoside (NR) Uptake Permease (PnuC) Family (TC# 4.B.1) is a family of transmembrane transporters that is part of the TOG superfamily.[1] Close PnuC homologues are found in a wide range of Gram-negative and Gram-positive bacteria, archaea and eukaryotes.[2]

Function

PnuC of Salmonella typhimurium and Haemophilus influenzae are believed to function cooperatively with NadR homologues, multifunctional proteins that together with PnuC, participate in NR phosphorylation, transport and transcriptional regulation.[3][4][5] NadR, a cytoplasmic protein that is partly membrane associated, contains one well conserved and one poorly conserved mononucleotide-binding consensus sequence (G-X4 GKS). It drives transport and may render transport responsive to internal pyridine nucleotide levels. While its N-terminal half functions as a repressor, its C-terminal half functions as an NR kinase in a putative group translocation process.[6]

PnuC of Haemophilus influenzae

The H. influenzae homologue has been shown to transport NR from the periplasm into the cytoplasm. Phosphorylation of NR by NadR is required for NR uptake. The ribonucleoside kinase (RNK) domain has both Walker A and Walker B motifs, responsible for ATP binding and phosphoryl transfer. In addition, a proposed LID domain was identified in RNK. LID domains have been found in other kinases, and these domains are regions which are able to move after substrate binding. They are responsible for coordination of three distinct conformations, an open state in the absence of substrate, a partially closed state after substrate binding, and a fully closed state when both substrates are present.

In H. influenzae, NR enters the NAD+ resynthesis pathway after phosphorylation to NMN, and subsequently, NAD+ is synthesized from NMN and ATP via an NMN adenylyl transferase activity.[7][8] NadR represents a multifunctional regulator/enzyme complex able to integrate several functions, such as enzymatic catalysis, transport, and transcriptional regulatory activities.

Other constituents required for uptake

The components of the H. influenzae pathway necessary for NAD+, NMN, and NR uptake have been determined. Merdanovic et al. characterized two enzymes, an outer membrane nucleotide phosphatase, and an NAD+ nucleotidase (NadN) located in the periplasm.[9][10][11] They showed that NAD+ and NMN cross the outer membrane mainly via the OmpP2 porin.[12]

Only NR can be utilized by the PnuC transport system located in the inner membrane.[13][14] The pnuC gene product is the protein that is responsible for the main flow of the NR substrate into the cytoplasm. The study of Merdanovic et al. suggests that the RNK activity of NadR determines NR transport and is negatively regulated by cytoplasmic NAD+ feedback inhibition. Therefore, NR uptake is under NadR feedback control.[4]

ATP, not the proton motive force, appears to be required for NR uptake. Thus, the driving force for NR uptake via PnuC is NR phosphorylation by NadR. A concerted group translocation mechanism can be considered whereby NadR facilitates the dissociation of NR from PnuC by phosphorylating it to NMN, thus preventing efflux of NR.

Transport reaction

The proposed transport reaction catalyzed by PnuC and NadR is:[2]

NR (out) + ATP (in) → NMN (in) + ADP (in).

Structure

PnuC of Salmonella typhimurium and Haemophilus influenzae are integral membrane proteins, 239 and 226 amino acyl residues (aas) in length, respectively, with 7 putative transmembrane α-helical segments.

The structure of NadR has been determined.[15] Mutations in the nadR gene which interfere with NR uptake occur in the C-terminal part of NadR.[16] A helix-turn-helix DNA binding domain present in NadR of S. enterica serovar Typhimurium [16] could not be found in the NadR homologue of H. influenzae. Therefore, it was proposed that in H. influenzae NadR has no regulatory function at the transcriptional level.[7] The structures of the human NR kinase 1 (2QL6_P) with nucleotide and nucleoside substrates bound have been solved.[17] It is structurally similar to Rossmann fold metabolite kinases.

PnuC has been shown to resemble SWEET porters in overall fold,[18] supporting the conclusion that these two families are members of the TOG superfamily.[1]

Crystal structures

NadR Protein from H. influenzae PDB: 1LW7

NR transporter PnuC PDB: 4QTN

References

  1. 1.0 1.1 "The transporter-opsin-G protein-coupled receptor (TOG) superfamily". The FEBS Journal 280 (22): 5780–800. November 2013. doi:10.1111/febs.12499. PMID 23981446. 
  2. 2.0 2.1 Saier, MH Jr.. "4.B.1 The Nicotinamide Ribonucleoside (NR) Uptake Permease (PnuC) Family". Saier Lab Bioinformatics Group / SDSC. http://www.tcdb.org/search/result.php?tc=4.B.1#ref3139. 
  3. "Regulation of NAD metabolism in Salmonella typhimurium: molecular sequence analysis of the bifunctional nadR regulator and the nadA-pnuC operon". Journal of Bacteriology 172 (8): 4187–96. August 1990. doi:10.1128/jb.172.8.4187-4196.1990. PMID 2198247. 
  4. 4.0 4.1 "Coupling of NAD+ biosynthesis and nicotinamide ribosyl transport: characterization of NadR ribonucleotide kinase mutants of Haemophilus influenzae". Journal of Bacteriology 187 (13): 4410–20. July 2005. doi:10.1128/JB.187.13.4410-4420.2005. PMID 15968050. 
  5. "NAD-dependent DNA-binding activity of the bifunctional NadR regulator of Salmonella typhimurium". Journal of Bacteriology 181 (2): 648–55. January 1999. doi:10.1128/JB.181.2.648-655.1999. PMID 9882682. 
  6. "Group-translocation: a consequence of enzyme-catalysed group-transfer". Nature 182 (4632): 372–3. August 1958. doi:10.1038/182372a0. PMID 13577842. Bibcode1958Natur.182..372M. 
  7. 7.0 7.1 "Ribosylnicotinamide kinase domain of NadR protein: identification and implications in NAD biosynthesis". Journal of Bacteriology 184 (24): 6906–17. December 2002. doi:10.1128/jb.184.24.6906-6917.2002. PMID 12446641. 
  8. "Utilization and metabolism of NAD by Haemophilus parainfluenzae". Journal of General Microbiology 134 (10): 2789–99. October 1988. doi:10.1099/00221287-134-10-2789. PMID 3254936. 
  9. "NadN and e (P4) are essential for utilization of NAD and nicotinamide mononucleotide but not nicotinamide riboside in Haemophilus influenzae". Journal of Bacteriology 183 (13): 3974–81. July 2001. doi:10.1128/JB.183.13.3974-3981.2001. PMID 11395461. 
  10. "NADP and NAD utilization in Haemophilus influenzae". Molecular Microbiology 35 (6): 1573–81. March 2000. doi:10.1046/j.1365-2958.2000.01829.x. PMID 10760156. 
  11. "Is a NAD pyrophosphatase activity necessary for Haemophilus influenzae type b multiplication in the blood stream?". International Journal of Medical Microbiology 291 (3): 219–25. August 2001. doi:10.1078/1438-4221-00122. PMID 11554562. 
  12. "Porin OmpP2 of Haemophilus influenzae shows specificity for nicotinamide-derived nucleotide substrates". The Journal of Biological Chemistry 278 (27): 24269–76. July 2003. doi:10.1074/jbc.M213087200. PMID 12695515. 
  13. "Nicotinamide ribosyl uptake mutants in Haemophilus influenzae". Infection and Immunity 71 (9): 5398–401. September 2003. doi:10.1128/iai.71.9.5398-5401.2003. PMID 12933892. 
  14. "PnuC and the utilization of the nicotinamide riboside analog 3-aminopyridine in Haemophilus influenzae". Antimicrobial Agents and Chemotherapy 48 (12): 4532–41. December 2004. doi:10.1128/AAC.48.12.4532-4541.2004. PMID 15561822. 
  15. "Crystal structure of Haemophilus influenzae NadR protein. A bifunctional enzyme endowed with NMN adenyltransferase and ribosylnicotinimide kinase activities". The Journal of Biological Chemistry 277 (36): 33291–9. September 2002. doi:10.1074/jbc.M204368200. PMID 12068016. 
  16. 16.0 16.1 "The bifunctional NadR regulator of Salmonella typhimurium: location of regions involved with DNA binding, nucleotide transport and intramolecular communication". FEMS Microbiology Letters 112 (2): 179–83. September 1993. doi:10.1016/0378-1097(93)90161-t. PMID 8405960. 
  17. "Nicotinamide riboside kinase structures reveal new pathways to NAD+". PLOS Biology 5 (10): e263. October 2007. doi:10.1371/journal.pbio.0050263. PMID 17914902. 
  18. "Pnu Transporters: Ain't They SWEET?". Trends in Biochemical Sciences 41 (2): 117–118. February 2016. doi:10.1016/j.tibs.2015.11.013. PMID 26692123. https://pure.rug.nl/ws/files/79384860/Pnu_Transporters_Ain_t_They_SWEET.pdf.