نتایج جستجو برای: peptide analogues

تعداد نتایج: 185427  

Mohammad Mazidi Mostafa Gandomkar Mostafa Goudarzi Reza Najafi Seyed Esmaeil Sadat Ebrahimi

  Introduction: Over expression of selected peptide receptors in human tumors has been shown to represent clinically relevant targets for cancer diagnosis and therapy. The aim of this work was to investigate Neuropeptide Y (NPY) as a new radiopharmaceutical for diagnosis of breast cancer. Methods: A neuropeptide Y analogues with Y1 receptor preference and agonistic p...

Journal: :Proceedings of the National Academy of Sciences of the United States of America 1994
G Guichard N Benkirane G Zeder-Lutz M H van Regenmortel J P Briand S Muller

Three analogues of the model peptide of sequence IRGERA corresponding to the COOH-terminal residues 130-135 of histone H3 were synthesized, and their antigenicity, immunogenicity, and resistance to trypsin were compared to those of the natural L-peptide. The three analogues correspond to the D-enantiomer, containing only D-residues, and two retro-peptides containing NH-CO bonds instead of natur...

Journal: :Journal of immunology 1998
L R Soares P L Orr M R Garovoy G Benichou

Recent studies using synthetic altered peptide ligands (Analogues) have led to the fine dissection of TCR-mediated T cell functions elicited by Ag recognition. Certain Analogues behave as full agonists of the antigenic peptide while others are partial agonists in that they only trigger selected T cell functions. Additionally, peptide Analogues can behave as antagonists by inhibiting functions o...

Journal: :Annals of the New York Academy of Sciences 2004
Eric P Krenning Dik J Kwekkeboom Roelf Valkema Stanislas Pauwels Larry K Kvols Marion De Jong

On their plasma membranes, cells express receptor proteins with high affinity for regulatory peptides, such as somatostatin. Changes in the density of these receptors during disease, for example, overexpression in many tumors, provide the basis for new imaging methods. The first peptide analogues successfully applied for visualization of receptor-positive tumors were radiolabeled somatostatin a...

Journal: :Journal of immunology 1999
Y Men I Miconnet D Valmori D Rimoldi J C Cerottini P Romero

Previous studies have shown that substitution of single amino acid residues in human Melan-A immunodominant peptides Melan-A27-35 and Melan-A26-35 greatly improved their binding and the stability of peptide/HLA-A*0201 complexes. In particular, one Melan-A peptide analogue was more efficient in the generation of Melan-A peptide-specific and melanoma-reactive CTL than its parental peptide in vitr...

Journal: :The Biochemical journal 1991
J C Kermode R J Freer E L Becker

The characteristics of binding to the chemotactic receptors on rabbit peritoneal neutrophils were examined for seven formyl peptide analogues. These receptor-binding characteristics were compared with the abilities of the analogues to induce the biological responses of degranulation and chemotaxis. Five of the analogues showed distinct functional heterogeneity in their receptor-binding patterns...

Journal: :Molecules 2017
Anna Lucia Tornesello Luigi Buonaguro Maria Lina Tornesello Franco Maria Buonaguro

Many synthetic peptides have been developed for diagnosis and therapy of human cancers based on their ability to target specific receptors on cancer cell surface or to penetrate the cell membrane. Chemical modifications of amino acid chains have significantly improved the biological activity, the stability and efficacy of peptide analogues currently employed as anticancer drugs or as molecular ...

Journal: :The Journal of biological chemistry 1978
J R Feramisco E G Krebs

Analogues of the synthetic substrate Leu-Arg-Arg-Ala-Ser-Leu-Gly in which the serine is replaced by other amino acids inhibited the activity of the catalytic subunit of cyclic AMP-dependent protein kinase from beef skeletal muscle (Peak I). All of the analogues were competitive with respect to peptide substrate but apparent Ki values varied depending on the particular amino acid that was substi...

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