Literature DB >> 23621498

A phase 1 study of heat/phenol-killed, E. coli-encapsulated, recombinant modified peanut proteins Ara h 1, Ara h 2, and Ara h 3 (EMP-123) for the treatment of peanut allergy.

R A Wood1, S H Sicherer, A W Burks, A Grishin, A K Henning, R Lindblad, D Stablein, H A Sampson.   

Abstract

BACKGROUND: Immunotherapy for peanut allergy may be limited by the risk of adverse reactions.
OBJECTIVE: To investigate the safety and immunologic effects of a vaccine containing modified peanut proteins.
METHODS: This was a phase 1 trial of EMP-123, a rectally administered suspension of recombinant Ara h 1, Ara h 2, and Ara h 3, modified by amino acid substitutions at major IgE-binding epitopes, encapsulated in heat/phenol-killed E. coli. Five healthy adults were treated with 4 weekly escalating doses after which 10 peanut-allergic adults received weekly dose escalations over 10 weeks from 10 mcg to 3063 mcg, followed by three biweekly doses of 3063 mcg.
RESULTS: There were no significant adverse effects in the healthy volunteers. Of the 10 peanut-allergic subjects [4 with intermittent asthma, median peanut IgE 33.3 kUA /l (7.2-120.2), and median peanut skin prick test wheal 11.3 mm (6.5-18)]; four experienced no symptoms; one had mild rectal symptoms; and the remaining five experienced adverse reactions preventing completion of dosing. Two were categorized as mild, but the remaining three were more severe, including one moderate reaction and two anaphylactic reactions. Baseline peanut IgE was significantly higher in the five reactive subjects (median 82.4 vs 17.2 kUA /l, P = 0.032), as was baseline anti-Ara h 2 IgE (43.3 versus 8.3, P = 0.036). Peanut skin test titration and basophil activation (at a single dilution) were significantly reduced after treatment, but no significant changes were detected for total IgE, peanut IgE, or peanut IgG4.
CONCLUSIONS: Rectal administration of EMP-123 resulted in frequent adverse reactions, including severe allergic reactions in 20%.
© 2013 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.

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Year:  2013        PMID: 23621498      PMCID: PMC3663889          DOI: 10.1111/all.12158

Source DB:  PubMed          Journal:  Allergy        ISSN: 0105-4538            Impact factor:   13.146


  23 in total

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3.  Allergenic characteristics of a modified peanut allergen.

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5.  Strain-dependent induction of allergic sensitization caused by peanut allergen DNA immunization in mice.

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6.  Persistent protective effect of heat-killed Escherichia coli producing "engineered," recombinant peanut proteins in a murine model of peanut allergy.

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7.  Oral gene delivery with chitosan--DNA nanoparticles generates immunologic protection in a murine model of peanut allergy.

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10.  Sublingual immunotherapy for peanut allergy: a randomized, double-blind, placebo-controlled multicenter trial.

Authors:  David M Fleischer; A Wesley Burks; Brian P Vickery; Amy M Scurlock; Robert A Wood; Stacie M Jones; Scott H Sicherer; Andrew H Liu; Donald Stablein; Alice K Henning; Lloyd Mayer; Robert Lindblad; Marshall Plaut; Hugh A Sampson
Journal:  J Allergy Clin Immunol       Date:  2013-01       Impact factor: 10.793

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