| Literature DB >> 21683593 |
Nan Zhao1, Yao Ma, Shengmei Zhang, Xin Fang, Zhenglun Liang, Gang Liu.
Abstract
A series of new muramyl dipeptide (MDP) mimics were designed and synthesized via a solid-phase synthetic route. Their adjuvant activities were evaluated ex vivo for investigation of the synergism of the S(28-39) peptide, which is an MHC class I binding epitope of recombinant hepatitis B surface antigen (HBsAg) for both humans and mice. Several compounds without the carbohydrate moiety exerted better adjuvanticity than the MDP-C that has been reported by our laboratory previously. A primary screening test revealed that compounds 6, 14 and 16 exhibited stronger adjuvanticity compared with other MDP mimics.Entities:
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Year: 2011 PMID: 21683593 PMCID: PMC7126364 DOI: 10.1016/j.bmcl.2011.05.056
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823
Figure 1Structures of MDP and MDP-C.
Figure 2Structural diversity of MDP mimics.
Scheme 1Reagents and conditions: (a) HOBt, DIC, and DMF, rt, 3 h; (b) 20% piperidine/DMF, rt, 20 min, two times; (c) Fmoc-protected amino acids, HOBt, DIC, and DMF, rt, 3 h; (d) o-nitro benzoic acid derivatives, HOBt, DIC, and DMF, rt, 3 h; (e) 2 M SnCl2, NMM, and DMF, rt, 12 h; (f) organic aldehyde, NaH3BCN, AcOH, and DMF; 40 °C, 36 h; (g) 95% TFA/H2O, rt, 1 h.
SAR investigation of twenty new MDP mimics
| Compd. | R1 | R2 | R3 | R4 | IFN-γ SFCs/4 × 105 splenocytes |
|---|---|---|---|---|---|
| Cl | H | H | 212.5 ± 19 | ||
| H | H | H | 224.0 ± 24 | ||
| H | H | 164.0 ± 26 | |||
| Cl | H | 14.3 ± 7 | |||
| Cl | H | H | 122.5 ± 15 | ||
| Cl | H | 316.0 ± 20 | |||
| CH3O | CH3O | H | 186.8 ± 47 | ||
| CH3O | CH3O | 185.8 ± 49 | |||
| H | H | 102.0 ± 37 | |||
| H | H | 173.3 ± 21 | |||
| H | H | 116.3 ± 22 | |||
| H | H | H | 139.5 ± 9 | ||
| CH3O | CH3O | H | 144.3 ± 30 | ||
| Cl | H | 317.0 ± 46 | |||
| H | H | H | 31.8 ± 11 | ||
| H | H | 304.3 ± 17 | |||
| H | H | 130.3 ± 10 | |||
| CH3O | CH3O | 117.8 ± 9 | |||
| Cl | H | 125.3 ± 9 | |||
| CH3O | CH3O | 125.3 ± 29 |
HBsAg-specific IFN-γ ELISPOT responses after immunization with various MDP mimics + HBsAg MHC I restricted peptide S28–39. BALB/c mice were immunized subcutaneously on day 0 and boosted on day 7 with S28–39 (100 μg in 100 μL of PBS) and the various MDP mimics (100 μg in 100 μL of PBS), or S28–39 alone. MDP-C was used as a positive control. Mice were sacrificed 7 days after the last immunization and splenocytes were collected. Isolated splenocytes were tested for HBsAg MHC I restricted peptide S28–39-specific IFN-γ secretion using the ELISPOT assay. Data were expressed as mean ± SEM.
p <0.05 versus S28–39 alone.
p <0.01 versus S28–39 alone.
p <0.01 versus MDP-C.