2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE
2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE Basic information
- Product Name:
- 2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE
- Synonyms:
-
- 2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE
- 2-Adamantanecarbonyl-Arg-Phe-NH2
- RF 9
- 1-Adamantanecarbonyl-Arg-Phe-NH2
- 1-Adamantanecarbonyl-Arg-Phe-NH2 trifluoroacetate salt
- RF9 trifluoroacetate salt
- RD9
- L-Phenylalaninamide, N2-(tricyclo[3.3.1.13,7]dec-1-ylcarbonyl)-L-arginyl-
- CAS:
- 876310-60-0
- MF:
- C26H38N6O3
- MW:
- 482.62
- Mol File:
- 876310-60-0.mol
2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE Chemical Properties
- Density
- 1.42±0.1 g/cm3(Predicted)
- storage temp.
- Store at -20°C
- solubility
- H2O: soluble20mg/mL
- pka
- 14.53±0.20(Predicted)
- form
- solid
- color
- White
2-ADAMANTANECARBONYL-ARG-PHE-NH2 TRIFLUOROACETATE Usage And Synthesis
Uses
RF9 is an NPFF1 and NPFF2 receptor inhibitor as well as RFRP-3 antagonist.
Definition
ChEBI: RF9 is a dipeptide formed from L-arginine and L-phenylalaninamide residues in which a hydrogen attached to the nitrogen of the alpha-amino group of the arginine residue has been replaced by a 1-adamantanecarbonyl group. It has been reported to be a potent and selective antagonist of neuropeptide FF (NPFF) receptors, but more recently found to be an agonist at both NPFF1R and the kisspeptin receptor (KISS1R). It has a role as a neuropeptide FF receptor antagonist, a neuropeptide FF receptor agonist and a kisspeptin receptor agonist. It is functionally related to an Arg-Ala.
Biological Activity
ki: 58 nm for npff1; 75 nm for npff2rf 9 is a neuropeptide ff receptors antagonist.neuropeptide ff (npff) has been isolated originally from bovine brain through its cross-reaction with antibodies to the molluscan cardioexcitory peptide fmrf-nh2, which possesses the similar c-terminal sequence. recent studies shows that npff belongs to a neuropeptide family including two g protein-coupled receptors (npff1 and npff2) and two precursors (pro-npffa and pro-npffb). both in vitro and in vivo studies have indicated that npff involves in a variety of biological actions.
in vitro
rf9 was found as a potent and selective npff receptor antagonist. rf9 was shown to be able to selectively bind to recombinant npff1 or npff2 receptors expressed in cho or cos-1 cell and could also in vitro antagonize the agonism induced by npff and npvf in the functional assays [1].
in vivo
aminal in vivo study showed rf9 (30 nmol) injection failed to induce significant effect, but rf9 could completely antagonize the hypothermia of npff after cerebral administration in mice. additionally, rf9 (30 nmol) co-injected in the third ventricle reduced the hypothermia induced by morphine or nociceptin/orphanin [2].
storage
Store at -20°C
References
[1] fang q,wang yq,he f,guo j,guo j,chen q,wang r. inhibition of neuropeptide ff (npff)-induced hypothermia and anti-morphine analgesia by rf9, a new selective npff receptors antagonist. regul pept.2008 apr 10;147(1-3):45-51.
[2] wang yq,guo j,wang sb,fang q,he f,wang r. neuropeptide ff receptors antagonist, rf9, attenuates opioid-evoked hypothermia in mice. peptides.2008 jul;29(7):1183-90.
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