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Peptide ASQ

Anti-Peptide ASQ Products
- Mouse Anti-Peptide ASQ Recombinant Soluble TCR (clone (Tg4)-1) (scTCR-0875YC-S(P))
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- Epitope: ASQARPSQR + ACET(A1)
- MHC: H-2Aᵘ
- Mouse Anti-Peptide ASQ Recombinant Soluble TCR (clone (Tg4)-2) (scTCR-0876YC-S(P))
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- Epitope: ASQARPSQRHG + ACET(A1)
- MHC: H-2Aᵘ
- Mouse Anti-Peptide ASQ Recombinant Soluble TCR (clone (Tg4)-3) (scTCR-0877YC-S(P))
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- Epitope: ASQYRPSQR + ACET(A1)
- MHC: H-2Aᵘ
- Mouse Anti-Peptide ASQ Recombinant Soluble TCR (clone (Tg4)-4) (scTCR-0878YC-S(P))
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- Epitope: ASQYRPSQRHG + ACET(A1)
- MHC: H-2Aᵘ
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- Epitope: ASQARPSQR + ACET(A1)
- MHC: H-2Aᵘ
- Recombinant Mouse Anti-Peptide ASQ Soluble TCR (Tg4) (C-Cys) (VS-0622-YF4877)
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- Epitope: ASQARPSQR + ACET(A1)
- MHC: H-2Aᵘ
- Recombinant Mouse Anti-Peptide ASQ Soluble TCR (Tg4) (KIH) (VS-0622-YF7585)
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- Epitope: ASQARPSQR + ACET(A1)
- MHC: H-2Aᵘ
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For Research Use Only. Not For Clinical Use.
Background
EAE has been successfully treated with the immunodominant epitope of MBP, Ac1-11, as well as analogues in which position four is changed from the native lysine to an alanine (Ac1-11[4A]) or tyrosine (Ac1-11[4Y]). Ac1-11[4A] and Ac1-11[4Y] bind to the MHC with ∼50 and 1,500 times higher affinity than does Ac1-11, and both peptides stimulate most Ac1-11–specific T cells more efficiently than does Ac1-11. The affinities of these peptides for I-Au correlate with the half-lives of each of the peptides complexed to I-Aᵘ; Ac1-11/I-Aᵘ has an immeasurably short half-life, Ac1-11[4A] has a half-life of ∼10 min, and Ac1-11[4Y]/I-Au can be detected for as long as 10 h. The efficacy of treatment of EAE with these three peptides correlates with the affinity of the peptides for I-Aᵘ. The mechanism of this treatment may be due to anergy, deletion, a switch in Th subset, or a combination of these phenomena.