A method for altering the conformation of a first polypeptide Itgand or group of polypeptide ligands, each polypeptide ligand comprising at least two reactive groups separated by a loop sequence covalently linked to a molecular scaffold which forms covalent bonds with said reactive groups, to produce a second polypeptide ligand or group of polypeptide iigands, comprising assembling said second ligand or group of ligands from the polypeptrde(s) and structural scaffold of said first ligand or group of ligands, incorporating one of:
(a) altering at least one reactive group; or
(b) altering the nature of the molecular scaffold; or
(c) altering the bond between at least one reactive group and the molecular scaffold; or
(d) any combination of (a), (b) or (c).
A method according to claim 1, wherein the reactive group comprises a sulphur atom.
A method according to claim 2, wherein the reactive group is a cysteine or a methionine.
A method according to claim 2, wherein the reactive group is altered to cysteine, selenocysteine or methionine.
A method according to claim 1, wherein the altered molecular scaffold is asymmetric.
A method according to claim 5, wherein the molecular scaffold comprises two or more scaffold reactive groups which are capable of forming covalent bonds with the reactive groups on the polypeptides, and said two or more reactive groups are not identical.
A method according to claim 6, wherein one of said scaffold reactive groups is orthogonal.

A method any of the above claims wherein the scaffold reactive groups are selected from benzyiic halides, a-halocarboxylic acids and acryloyl moieties.
A method according to claim 1, wherein at least one bond between the molecular scaffold and the polypeptide are chemically modified after assembly of the polypeptide and the molecular scaffold.
A method according to claim 9, wherein at least one thio-ether linkage between the polypeptide and the molecular scaffold is oxidised to form a sulphoxide or a sulphone.
A method according to any preceding claim, wherein the first group of polypeptide variants is a first repertoire of polypeptide variants.
A method according to any preceding claim, wherein the second group of polypeptide variants is a second repertoire of polypeptide variants.
A method for generating a group or repertoire of diverse polypeptide ligands from a first polypeptide ligand comprising at least two reactive groups separated by a loop sequence covalently linked to a molecular scaffold which forms covalent bonds with said reactive groups, comprising assembling a group or repertoire of ligands from the polypeptide and scaffold of said first ligand or group of ligands, and incorporating one of:
a) altering at least one reactive group; or
b) altering the nature of the molecular scaffold; or
c) altering the bond between at least one reactive group and the molecular scaffold; or
d) any combination of (a), (b) or (c); or
e) modifying the sequence of the polypeptide, in combination with any one of (a) to (d).

14. A method for increasing the conformational diversity of a first repertoire of
polypeptide ligands, comprising a plurality of polypeptides comprising at least two reactive groups separated by a loop sequence cova)ent)y linked to a molecular scaffold which forms covalent bonds with said reactive groups, comprising assembling a second repertoire of peptide ligands from the polypeptides and scaffold of said first repertoire, incorporating one of:
(a) altering at least one reactive group; or
(b) altering the nature of the molecular scaffold; or
(c) altering the bond between at least one reactive group and the moJecular scaffold; or
(d) any combination of (a), (b) or (c).
(e) modifying the sequence of the polypeptide, in combination with any one of (a)to(d).
15. A method according to claim 14, wherein the second repertoire is assembled
from the polypeptides of the first repertoire, and at least two structurally diverse molecular scaffold species.
16. A method for providing a polypeptide ligand comprising a polypeptide covalently
linked to a molecular scaffold at three or more amino acid residues, comprising the steps of:
a. providing a first repertoire of polypeptides;
b. conjugating said polypeptides to a molecular scaffold which binds to the
polypeptides at two or more amino acid residues, to form a first repertoire of
polypeptide conjugates;
c. screening said first repertoire for binding against a target, and selecting
members of the first repertoire which bind to the target;
d. introducing further variation into the polypeptide ligands, in accordance with
claim 1, yielding a second repertoire of polypeptide conjugates; and
e. screening said second repertoire for improved binding to the target.

17. A method for selecting a peptide ligand having increased protease resistance,
comprising the steps of:
a. providing a first repertoire of polypeptides;
b. conjugating said polypeptides to a molecular scaffold which binds to the
polypeptides at two or more amino acid residues, to form a first repertoire of
polypeptide conjugates;
c. screening said first repertoire for binding against a target, and selecting
members of the first repertoire which bind to the target;
d. introducing further variation into the polypeptide ligands, in accordance with
the first aspect of the invention set forth above, yielding a second repertoire
of polypeptide conjugates;
e. subjecting the second repertoire to selection for protease resistance; and
f. optionally, screening said second repertoire for binding to the target.
18. A method according to any preceding claim, wherein one or more of the groups
or repertoires of polypeptides is encoded by one or more libraries of nucleic acid molecules.
19. A method according to any one of claims 1 to 18, wherein the screening of said
repertoires is performed using a genetic display system.
20. A method according to claim 22, wherein the genetic display system is phage
display.
21. A repertoire of peptide ligands, when produced by a method according to any
preceding claim.
22. A method according to any one of claims 1 to 17, wherein any of the groups or
repertoires is made from synthetic peptides.
23. A method of claim 22 wherein the second group or repertoire is made from
synthetic peptides.
24. A method according to claim 22, wherein said synthetic peptides are arrayed on
solid phase.

A group of peptide ligands, when produced by a method according to any one of claims 22 to 24
A polypeptide conjugate produced by a method according to any one of claims 1
to 20, comprising a polypeptide comprising at least two reactive groups each
separated by a loop sequence, covalently linked to a molecular scaffold
comprising at least two scaffold reactive groups which form covalent bonds with
said reactive groups, wherein at least two of said scaffold reactive groups are
different. ' *
A polypeptide Iigand according to claim 26, which has a molecular weight of less than 3000 Dalton.
A polypeptide Iigand according to claim 26 or claim 27,-wherein the length of the polypeptide loops subtended between any two adjacent points of attachment of the polypeptide to the molecular scaffold is between 0 and 9 amino acids, and the length of the polypeptide sequence between the first and last of said points of attachment is less than 27 amino acids.