1253690-13-9

Basic information

• Product Name: Boc-D-Ser-Oipr
• Synonyms: Boc-D-Ser-Oipr;(R)-Isopropyl 2-((tert-butoxycarbonyl)amino)-3-hydroxypropanoate
• CAS NO: 1253690-13-9
• Molecular Formula: C11H21NO5
• Molecular Weight: 247.28814
• Mol File: 1253690-13-9.mol
• Article Data: 1

Chemical Properties

• Appearance: /
• CAS DataBase Reference: Boc-D-Ser-Oipr(CAS DataBase Reference)
• NIST Chemistry Reference: Boc-D-Ser-Oipr(1253690-13-9)
• EPA Substance Registry System: Boc-D-Ser-Oipr(1253690-13-9)

Safety Data

• Hazardous Substances Data: 1253690-13-9(Hazardous Substances Data)

Usage

General Description

Boc-D-Ser-Oipr is a chemical compound with the molecular formula C20H28N2O5. It is a derivative of the amino acid D-serine that has been modified with a tert-butoxycarbonyl (Boc) protecting group and an 2-(1H-1,2,4-triazol-1-yl)isopropyl (Oipr) moiety. Boc-D-Ser-Oipr is commonly used in the synthesis of peptides and peptidomimetics, serving as a building block for the creation of novel bioactive compounds with potential pharmaceutical applications. Its unique structure and properties make it a valuable tool for chemical research and drug development.

Upstream product

• 24424-99-5 di-tert-butyl dicarbonate 

Relevant articles and documents

Serine side chain-linked peptidomimetic conjugates of cyclic HPMPC and HPMPA: Synthesis and interaction with hPEPT1

Cidofovir (HPMPC), a broad spectrum antiviral agent, cannot be administered orally due to ionization of its phosphonic acid group at physiological pH. One prodrug approach involves conversion to the cyclic form (cHPMPC, 1) and esterification by the side chain hydroxyl group of a peptidomimetic serine. Transport studies in a rat model have shown enhanced levels of total cidofovir species in the plasma after oral dosing with l-Val-l-Ser-OMe cHPMPC, 2a. To explore the possibility that 2a and its three l/d stereoisomers 2b-d undergo active transport mediated by the peptide-specific intestinal transporter PEPT1, we performed radiotracer uptake and electrophysiology experiments applying the two-electrode voltage clamp technique in Xenopus laevis oocytes overexpressing human PEPT1 (hPEPT1, SLC15A1). 2a-d did not induce inward currents, indicating that they are not transported, but the stereoisomers with an l-configuration at the N-terminal valine (2a and 2b) potently inhibited transport of the hPEPT1 substrate glycylsarcosine (Gly-Sar). A "reversed" dipeptide conjugate, l-Ser-l-Ala-OiPr cHPMPC (4), also did not exhibit detectable transport, but completely abolished the Gly-Sar signal, suggesting that affinity of the transporter for these prodrugs is not impaired by a proximate linkage to the drug in the N-terminal amino acid of the dipeptide. Single amino acid conjugates of cHPMPC (3a and 3b) or cHPMPA (5, 6a and 6b) were not transported and only weakly inhibited Gly-Sar transport. The known hPEPT1 prodrug substrate valacyclovir (7) and its l-Val-l-Val dipeptide analogue (8) were used to verify coupled transport by the oocyte model. The results indicate that the previously observed enhanced oral bioavailability of 2a relative to the parent drug is unlikely to be due to active transport by hPEPT1. Syntheses of the novel compounds 2b-d and 3-6 are described, including a convenient solid-phase method to prepare 5, 6a and 6b.