Melittin-specific monoclonal and polyclonal IgE and IgG1 antibodies from mice.

King, Te Piao; Kochoumian, Loucia; Joslyn, Alison

doi:10.4049/jimmunol.133.5.2668

Cited by 24 publications

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Immunogenicity of dinitrocarboxyphenylated melittin: The influence of C‐terminal chain shortening, N‐terminal substitution and prolin insertion at positions 5 and 10

Zhao

Rolli

Schneider

1995

Journal of Peptide Science

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Peptides derived from the bee-venom melittin were fitted with the haptenic group dinitrocarboxyphenyl (Dncp) and tested in out-bred guinea pigs for immunogenicity by measuring the IgG anti-Dncp antibody response by ELISA. Dncp-conjugates comprising virtually the entire melittin proved to be strong immunogens producing antibody responses comparable to those of proteins. Weak responses were obtained with considerably shortened sequences. Conjugates with N-terminal Dncp gave markedly reduced antibody responses compared to peptides with C-terminal Dncp. An N-terminal biotinyl substituent abolished the immune response whereas N-terminal lauryl and caprylyl had little effect. Insertion of L-proline into a hexadecapeptide conjugate abolishing the possibility of helix formation gave an immunogen to which individual animals clearly responded on a low level. Oligomerisation, but not the cytolytic activity of melittin peptides, may contribute to the immunogenicities observed.

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Immunogenicity of dinitrocarboxyphenylated melittin: The influence of C‐terminal chain shortening, N‐terminal substitution and prolin insertion at positions 5 and 10

Zhao

Rolli

Schneider

1995

Journal of Peptide Science

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Immunogenicity Studies with Haptenated Melittin Peptides: Implication for Membrane Involvement during the Recognition Step

Curcio-Vonlanthen

Rolli

Schneider

1996

Journal of Peptide Science

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Melittin peptides carrying 2,4-dinitro-6-carboxyphenyl (Dncp) haptenic groups regularly evoked anti-hapten IgG responses in mice or guinea pigs when the hapten was C-terminally attached. Single haptens on the N-terminal helix in several positions gave poor or no responses in the early stages but adequate titres after prolonged immunization. Peptides with Dncp at the C-terminus as an invariant feature and a second Dncp in various positions along the peptide chain did not fail to produce adequate responses. The hampering effect is not due to a defect at the T-cell level but involves the recognition step on the B-cell. It is implied that the haptenic interaction with the paratope of the recognizing immunoglobulin on the B-cell involves the cell membrane in an important way. It is also suggested that late antibody responses should not be overlooked during the development of proteinaceous immunogens for vaccination.

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Structure-Function Relationships of Allergens

Zhang¹,

Mohapatra²

1996

Pollen Biotechnology

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Melittin-specific monoclonal and polyclonal IgE and IgG1 antibodies from mice.

Cited by 24 publications

References 0 publications

Immunogenicity of dinitrocarboxyphenylated melittin: The influence of C‐terminal chain shortening, N‐terminal substitution and prolin insertion at positions 5 and 10

Immunogenicity of dinitrocarboxyphenylated melittin: The influence of C‐terminal chain shortening, N‐terminal substitution and prolin insertion at positions 5 and 10

Immunogenicity Studies with Haptenated Melittin Peptides: Implication for Membrane Involvement during the Recognition Step

Structure-Function Relationships of Allergens

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