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A natural CCL5/RANTES variant antagonist for CCR1 and CCR3
Authors:Corinne Capoulade-Métay  Ahidjo Ayouba  Anfumbom Kfutwah  Kavita Lole  Stéphane Pêtres  Yasmine Dudoit  Philippe Deterre  Elisabeth Menu  Françoise Barré-Sinoussi  Patrice Debré  Ioannis Theodorou
Institution:(1) INSERM U543, CHU Pitié-Salpêtrière, 91 Boulevard de l’Hôpital, 75013 Paris, France;(2) Centre Pasteur du Cameroun, Yaoundé, Cameroon;(3) Unité de Régulation des Infections Rétrovirales, Institut Pasteur, Paris, France;(4) Plateforme protéomique, Institut Pasteur, Paris, France;(5) National Institute of Virology, Pune, India
Abstract:The N-terminal domain of the chemokine CCL5/regulated upon activation normal T cell expressed and secreted (RANTES) has been shown to be critical for its biological activity on leukocytes. Several N-terminus-modified CCL5/RANTES derivatives, such as N-Terminal truncated CCL5/RANTES, Met-RANTES, and amino-oxypentane (AOP)-RANTES exhibited antagonist or partial agonist functions when investigated on the properties of their receptors CCR1, CCR3, and CCR5. Studying 95 African samples from Cameroon, we found a naturally occurring variant of CCL5/RANTES containing a missense mutation located in the first amino acid of the secreted form (S24F). S24F binds CCR1, CCR3, and CCR5 and triggers receptor down-modulation comparable to CCL5/RANTES. Moreover, in CCR5 positive cells, S24F elicits cellular calcium mobilization equivalent to that obtained with CCL5/RANTES. By contrast, S24F does not provoke any response in CCR1 and CCR3 positive cells. As CCL5/RANTES is able to attract different subtypes of leukocytes into inflamed tissue and intervenes in a wide range of allergic and autoimmune diseases, the discovery of this natural N-terminus-modified CCL5/RANTES analogue exhibiting differential effects on CCL5/RANTES receptors, opens up additional perspectives for therapeutic intervention.Nucleotide sequence data reported is available in the DDBJ/EMBL/GenBank databases under the accession number: DQ230537.
Keywords:Chemokines  Chemokine receptors  Variant  Ca2+ mobilization
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