Engineered anti-inflammatory peptides inspired by mapping an evasin–chemokine interaction

Darlot, Benoit; Eaton, James R.O.; Geis-Asteggiante, Lucía; Yakala, Gopala K.; Karuppanan, Kalimuthu; Davies, Graham; Robinson, Carol V.; Kawamura, Akane; Bhattacharya, Shoumo

doi:10.1074/jbc.ra120.014103

Cited by 9 publications

(18 citation statements)

References 60 publications

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“…Furthermore, the linear peptide Ev4 Glu 14 –Asn 31 , derived from the Evasin-4 sequence, possesses nanomolar affinity to CCL5 on its own. Similar tight affinities have recently been shown for peptides derived from the N terminus of P672 and are potent binders of CCL8 ( 31 ). The N-terminal region of Evasin-4 embodies multiple tyrosines, which are proposed to mimic an N-terminal region of CC-chemokine receptors ( 32 ).…”

Section: Discussionsupporting

confidence: 80%

“…Development of chemokine-binding peptides and peptidomimetics based on Evasins may provide more perspectives ( 34 ). Recently, several peptides derived from C8-Evasin P672 were shown to effectively block inflammation because of binding to multiple CC-type chemokines ( 31 ). Ev4 Glu 14 –Asn 31 effectively inhibits CCL5-induced monocyte migration.…”

Section: Discussionmentioning

confidence: 99%

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Structural characterization of anti-CCL5 activity of the tick salivary protein evasin-4

Denisov

Ramirez-Escudero

Heinzmann

et al. 2020

Journal of Biological Chemistry

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Ticks, as blood sucking parasites, have developed a complex strategy to evade and suppress host immune responses during feeding. The crucial part of this strategy is expression of a broad family of salivary proteins, called Evasins, to neutralize chemokines responsible for cell trafficking and recruitment. However, structural information about Evasins is still scarce and little is known about the structural determinants of their binding mechanism to chemokines. Here, we studied the structurally uncharacterized Evasin-4, which neutralizes a broad range of CC-motif chemokines, including the chemokine CC-motif ligand 5 (CCL5) involved in atherogenesis. Crystal structures of Evasin-4 and E66S CCL5—an obligatory dimeric variant of CCL5—were determined to a resolution of 1.3-1.8 Å. The Evasin-4 crystal structure revealed an L-shaped architecture formed by an N- and C-terminal subdomain consisting of eight β-strands and an α-helix that adopts a substantially different position compared to closely related Evasin-1. Further investigation into E66S CCL5/Evasin-4 complex formation with NMR spectroscopy showed that residues of the N-terminus are involved in binding to CCL5. The peptide derived from the N-terminal region of Evasin-4 possessed nM affinity to CCL5 and inhibited CCL5 activity in monocyte migration assays. This suggests that Evasin-4 derivatives could be used as starting point for the development of anti-inflammatory drugs.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 99%

Structural characterization of anti-CCL5 activity of the tick salivary protein evasin-4

Denisov

Ramirez-Escudero

Heinzmann

et al. 2020

Journal of Biological Chemistry

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“…Although EVA-1 and EVA-4 have effectively diminished inflammation in the murine model of acute lung injury and myocardial infarction, respectively ( Russo et al., 2011 ; Braunersreuther et al., 2013 ), their application as drugs could be challenging due to the complex structures and difficult production (personal observation). However, it has recently been shown that short linear and cyclic peptides derived from the N -termini of EVA-P672 and EVA-4 retain binding and inhibitory activity comparable to full-length parent proteins ( Darlot et al., 2020 ; Denisov et al., 2020b ). Moreover, these peptides could be further modified and adjusted for neutralization of chemokines of interest.…”

Section: Evasinsmentioning

confidence: 99%

Immunomodulatory Proteins in Tick Saliva From a Structural Perspective

Denisov

Dijkgraaf

2021

Front. Cell. Infect. Microbiol.

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To feed successfully, ticks must bypass or suppress the host’s defense mechanisms, particularly the immune system. To accomplish this, ticks secrete specialized immunomodulatory proteins into their saliva, just like many other blood-sucking parasites. However, the strategy of ticks is rather unique compared to their counterparts. Ticks’ tendency for gene duplication has led to a diverse arsenal of dozens of closely related proteins from several classes to modulate the immune system’s response. Among these are chemokine-binding proteins, complement pathways inhibitors, ion channels modulators, and numerous poorly characterized proteins whose functions are yet to be uncovered. Studying tick immunomodulatory proteins would not only help to elucidate tick-host relationships but would also provide a rich pool of potential candidates for the development of immunomodulatory intervention drugs and potentially new vaccines. In the present review, we will attempt to summarize novel findings on the salivary immunomodulatory proteins of ticks, focusing on biomolecular targets, structure-activity relationships, and the perspective of their development into therapeutics.

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“…Due to its broad CC chemokine-binding spectrum, Evasin-4 is considered the most suitable candidate for therapeutic development (86). More recently, Evasin-inspired artificial peptides dramatically reduced inflammation in vivo by targeting multiple chemokines (87). These peptides might therefore provide a route to the development of new anti-inflammatory therapeutics for chronic autoimmune diseases such as rheumatoid arthritis and inflammatory diseases such as atherosclerosis.…”

Section: Recruitment Of Blood-borne Innate Immune Cellsmentioning

confidence: 99%

“…These peptides might therefore provide a route to the development of new anti-inflammatory therapeutics for chronic autoimmune diseases such as rheumatoid arthritis and inflammatory diseases such as atherosclerosis. Moreover, the mechanism of action of these peptides suggests that they might also be useful in acute infectious diseases such as influenza or COVID-19, where exuberant cytokine responses are thought to be at least partially responsible for tissue injury (87).…”

Section: Recruitment Of Blood-borne Innate Immune Cellsmentioning

confidence: 99%

Tick Salivary Compounds for Targeted Immunomodulatory Therapy

et al. 2020

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Immunodeficiency disorders and autoimmune diseases are common, but a lack of effective targeted drugs and the side-effects of existing drugs have stimulated interest in finding therapeutic alternatives. Naturally derived substances are a recognized source of novel drugs, and tick saliva is increasingly recognized as a rich source of bioactive molecules with specific functions. Ticks use their saliva to overcome the innate and adaptive host immune systems. Their saliva is a rich cocktail of molecules including proteins, peptides, lipid derivatives, and recently discovered non-coding RNAs that inhibit or modulate vertebrate immune reactions. A number of tick saliva and/or salivary gland molecules have been characterized and shown to be promising candidates for drug development for vertebrate immune diseases. However, further validation of these molecules at the molecular, cellular, and organism levels is now required to progress lead candidates to clinical testing. In this paper, we review the data on the immunopharmacological aspects of tick salivary compounds characterized in vitro and/or in vivo and present recent findings on non-coding RNAs that might be exploitable as immunomodulatory therapies.

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Engineered anti-inflammatory peptides inspired by mapping an evasin–chemokine interaction

Cited by 9 publications

References 60 publications

Structural characterization of anti-CCL5 activity of the tick salivary protein evasin-4

Structural characterization of anti-CCL5 activity of the tick salivary protein evasin-4

Immunomodulatory Proteins in Tick Saliva From a Structural Perspective

Tick Salivary Compounds for Targeted Immunomodulatory Therapy

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