Patent ID: 11929151
Assignee: ADAPTIMMUNE LIMITED
Field: Measurement (Instruments)
Classification: CPC G | IPC G

Claim 0:
1. A method of treating a disease in a human subject, comprising:
administering a binding peptide that has been selected to bind to a target peptide presented by a human leukocyte antigen (HLA) and selected to prevent unwanted side effects in the subject, wherein the selecting to prevent unwanted side effects comprises the steps of:
(a) identifying at least one binding motif in the target peptide to which the binding peptide binds;
(b) searching for peptides that are present in the subject that comprise the at least one binding motif and that are not the target peptide (an off target peptide);
(c) testing binding of any such off target peptide to the binding peptide in vitro, wherein binding to one or more of such off target peptides predicts that the binding peptide has the potential to cross react in vivo, and
(d) selecting for administration a binding peptide that binds to the target peptide presented by HLA and is predicted to not have the potential to cross react with an off target peptide in the subject in vivo so as to cause unwanted side effects,
wherein the identifying at least one binding motif in step (a) comprises:
(a)(si) creating a series of mutants of the target peptide, each mutant having an amino acid residue at one position in the binding sequence thereof that is involved in binding to the binding peptide substituted for an alternative amino acid, such that over the series of mutants the amino acid residue in each position in the binding sequence is substituted for an alternative amino acid; and
testing each mutant in the series for its activity relative to the target peptide,
wherein an amino acid residue at a position within the binding sequence is identified as being part of the binding motif if the mutant in which the amino acid at that position is mutated to the alternative amino acid has a 50% or greater loss of activity relative to the target peptide, or
(a)(ii) creating a series of mutants, each mutant having an amino acid residue at one position in the binding sequence substituted for an alternative amino acid, such that over the series of mutants the amino acid residue in each position in the binding sequence is substituted for all alternative amino acids; and
testing each mutant in the series for its activity relative to the wild-type peptide,
wherein amino acid substitutions which result in a 50% or greater loss of activity relative to the target peptide are considered to be non-tolerated amino acids and not part of the binding motif and/or amino acid substitutions which do not result in a 50% or greater loss of activity relative to the target peptide are considered as part of the binding motif.