Individually dosed omalizumab facilitates peanut oral immunotherapy in peanut allergic adolescents

Background Peanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of stopping OIT. In placebo‐controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut....

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Published inClinical and experimental allergy Vol. 49; no. 10; pp. 1328 - 1341
Main Authors Brandström, Josef, Vetander, Mirja, Sundqvist, Ann‐Charlotte, Lilja, Gunnar, Johansson, S. G. O., Melén, Erik, Sverremark‐Ekström, Eva, Nopp, Anna, Nilsson, Caroline
Format Journal Article
LanguageEnglish
Published England Wiley Subscription Services, Inc 01.10.2019
Subjects
Adolescents
Allergens
Allergies
anaphylaxis
Ara h 1 antigen
Ara h 2 antigen
basophil
Clinical trials
Dosage
Food allergies
food allergy
Hypersensitivity
Immunoglobulin E
Immunoglobulin G
Immunotherapy
Monoclonal antibodies
omalizumab
oral immunotherapy
paediatrics
Patients
paediatrics
anaphylaxis
omalizumab
oral immunotherapy
basophil
food allergy
Online AccessGet full text
ISSN0954-7894
1365-2222
1365-2222
DOI10.1111/cea.13469

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Abstract Background Peanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of stopping OIT. In placebo‐controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut. Objective We hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD‐sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab. Methods This is the 2nd part of a one‐armed open phase‐2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step‐wise withdrawal of omalizumab, based on clinical symptoms and CD‐sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD‐sens and allergen‐binding activity (ABA) and IgE‐ab, IgG‐ab and IgG4‐ab to peanut and its components were measured during the study. Results All 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full‐dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE‐ab to peanut components Ara h 1‐3 and CD‐sens to peanut were significantly lower among successfully treated patients and IgG4‐ab to peanut, Ara h 2 and 6 increased significantly more during treatment. Conclusions and clinical relevance This study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up‐dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased. Clinical trials registration: ClinicalTrials.gov; NCT02402231. EudraCT; 2012‐005625‐78.
AbstractList Peanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause of stopping OIT. In placebo-controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut.BACKGROUNDPeanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause of stopping OIT. In placebo-controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut.We hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD-sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab.OBJECTIVEWe hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD-sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab.This is the 2nd part of a one-armed open phase-2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step-wise withdrawal of omalizumab, based on clinical symptoms and CD-sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD-sens and allergen-binding activity (ABA) and IgE-ab, IgG-ab and IgG4-ab to peanut and its components were measured during the study.METHODSThis is the 2nd part of a one-armed open phase-2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step-wise withdrawal of omalizumab, based on clinical symptoms and CD-sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD-sens and allergen-binding activity (ABA) and IgE-ab, IgG-ab and IgG4-ab to peanut and its components were measured during the study.All 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full-dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE-ab to peanut components Ara h 1-3 and CD-sens to peanut were significantly lower among successfully treated patients and IgG4-ab to peanut, Ara h 2 and 6 increased significantly more during treatment.RESULTSAll 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full-dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE-ab to peanut components Ara h 1-3 and CD-sens to peanut were significantly lower among successfully treated patients and IgG4-ab to peanut, Ara h 2 and 6 increased significantly more during treatment.This study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up-dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased.CONCLUSIONS AND CLINICAL RELEVANCEThis study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up-dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased.ClinicalTrials.gov; NCT02402231. EudraCT; 2012-005625-78.CLINICAL TRIALS REGISTRATIONClinicalTrials.gov; NCT02402231. EudraCT; 2012-005625-78.
Peanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause of stopping OIT. In placebo-controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut. We hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD-sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab. This is the 2nd part of a one-armed open phase-2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step-wise withdrawal of omalizumab, based on clinical symptoms and CD-sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD-sens and allergen-binding activity (ABA) and IgE-ab, IgG-ab and IgG4-ab to peanut and its components were measured during the study. All 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full-dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE-ab to peanut components Ara h 1-3 and CD-sens to peanut were significantly lower among successfully treated patients and IgG4-ab to peanut, Ara h 2 and 6 increased significantly more during treatment. This study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up-dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased. ClinicalTrials.gov; NCT02402231. EudraCT; 2012-005625-78.
Background Peanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of stopping OIT. In placebo‐controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut. Objective We hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD‐sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab. Methods This is the 2nd part of a one‐armed open phase‐2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step‐wise withdrawal of omalizumab, based on clinical symptoms and CD‐sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD‐sens and allergen‐binding activity (ABA) and IgE‐ab, IgG‐ab and IgG4‐ab to peanut and its components were measured during the study. Results All 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full‐dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE‐ab to peanut components Ara h 1‐3 and CD‐sens to peanut were significantly lower among successfully treated patients and IgG4‐ab to peanut, Ara h 2 and 6 increased significantly more during treatment. Conclusions and clinical relevance This study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up‐dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased. Clinical trials registration: ClinicalTrials.gov; NCT02402231. EudraCT; 2012‐005625‐78.
BackgroundPeanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of stopping OIT. In placebo‐controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut.ObjectiveWe hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD‐sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab.MethodsThis is the 2nd part of a one‐armed open phase‐2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step‐wise withdrawal of omalizumab, based on clinical symptoms and CD‐sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD‐sens and allergen‐binding activity (ABA) and IgE‐ab, IgG‐ab and IgG4‐ab to peanut and its components were measured during the study.ResultsAll 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full‐dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE‐ab to peanut components Ara h 1‐3 and CD‐sens to peanut were significantly lower among successfully treated patients and IgG4‐ab to peanut, Ara h 2 and 6 increased significantly more during treatment.Conclusions and clinical relevanceThis study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up‐dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased.Clinical trials registration: ClinicalTrials.gov; NCT02402231. EudraCT; 2012‐005625‐78.
Background: Peanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause of stopping OIT. In placebo-controlled trials, omalizumab has been shown to facilitate allergen immunotherapy and increase tolerance to peanut. Objective: We hypothesized that by combining omalizumab with pOIT, and monitor treatment effects with basophil allergen threshold sensitivity tests (CD-sens), peanut allergic patients could safely initiate pOIT and thereafter slowly withdraw omalizumab. Methods: This is the 2nd part of a one-armed open phase-2 study where peanut allergic adolescents (n = 23) started pOIT after an individualized omalizumab treatment. The pOIT dose was increased from 280 to 2800 mg peanut protein in 8 weeks followed by an individualized step-wise withdrawal of omalizumab, based on clinical symptoms and CD-sens levels. pOIT continued for 12 weeks followed by an open peanut challenge. Peanut CD-sens and allergen-binding activity (ABA) and IgE-ab, IgG-ab and IgG4-ab to peanut and its components were measured during the study. Results: All 23 patients successfully reached the 2800 mg maintenance dose. Moderate/systemic allergic reactions were rare while receiving full-dose omalizumab. Eleven of 23 (48%) successfully continued with pOIT after omalizumab was stopped. Compared to treatment failures, median baseline IgE-ab to peanut components Ara h 1-3 and CD-sens to peanut were significantly lower among successfully treated patients and IgG4-ab to peanut, Ara h 2 and 6 increased significantly more during treatment. Conclusions and clinical relevance: This study indicates that omalizumab is an effective adjunctive therapy for initiation and rapid up-dosing of pOIT; however, adverse events from pOIT become more frequent as omalizumab doses are decreased.
Author Vetander, Mirja
Brandström, Josef
Sundqvist, Ann‐Charlotte
Sverremark‐Ekström, Eva
Nopp, Anna
Lilja, Gunnar
Melén, Erik
Johansson, S. G. O.
Nilsson, Caroline
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  orcidid: 0000-0003-3679-6699
  surname: Brandström
  fullname: Brandström, Josef
  email: josef.brandstrom@sll.se
  organization: Karolinska Institutet
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  givenname: Mirja
  surname: Vetander
  fullname: Vetander, Mirja
  organization: Karolinska Institutet
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  givenname: Ann‐Charlotte
  surname: Sundqvist
  fullname: Sundqvist, Ann‐Charlotte
  organization: Södersjukhuset
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  givenname: Gunnar
  surname: Lilja
  fullname: Lilja, Gunnar
  organization: Karolinska Institutet
– sequence: 5
  givenname: S. G. O.
  surname: Johansson
  fullname: Johansson, S. G. O.
  organization: Karolinska Institutet
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  givenname: Erik
  surname: Melén
  fullname: Melén, Erik
  organization: Karolinska Institutet
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  givenname: Eva
  surname: Sverremark‐Ekström
  fullname: Sverremark‐Ekström, Eva
  organization: Stockholm University
– sequence: 8
  givenname: Anna
  orcidid: 0000-0003-1389-8676
  surname: Nopp
  fullname: Nopp, Anna
  organization: Karolinska Institutet
– sequence: 9
  givenname: Caroline
  surname: Nilsson
  fullname: Nilsson, Caroline
  organization: Karolinska Institutet
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ContentType Journal Article
Copyright 2019 John Wiley & Sons Ltd
2019 John Wiley & Sons Ltd.
Copyright © 2019 John Wiley & Sons Ltd
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IsPeerReviewed true
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Issue 10
Keywords paediatrics
anaphylaxis
omalizumab
oral immunotherapy
basophil
food allergy
Language English
License 2019 John Wiley & Sons Ltd.
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Notes Funding information
Data Availability Statement
Data available on request due to privacy/ethical restrictions.
This work was supported by Swedish Asthma and Allergy Association, Stockholm City Council, Sachs's Children and Youth Hospital, Center for Allergy Research (Karolinska Institutet), Hesselman's Foundation, Frimurare Barnhuset Foundation (Freemasons of Sweden), Konsul Th C Bergh's Foundation, research grant in memory of Kerstin Hejdenberg, Samariten Foundation, Her Royal Highness Crown Princess Lovisa's research fund, Mjölkdroppen Foundation, ÅkeWiberg's Foundation and Torsten Söderberg's foundation. MV is a postdoctoral researcher funded by the Karin and Sten Mörtstedt Initiative on Anaphylaxis. The funding sources had no role in planning, designing or execution of this study, neither did they have any role in collecting, analysing and reporting of data and results.
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Snippet Background Peanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of...
Peanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause of stopping...
BackgroundPeanut oral immunotherapy (pOIT) has showed good short‐term outcomes, but allergic reactions may prevent effective up‐dosing and is a major cause of...
Background: Peanut oral immunotherapy (pOIT) has showed good short-term outcomes, but allergic reactions may prevent effective up-dosing and is a major cause...
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StartPage 1328
SubjectTerms Adolescents
Allergens
Allergies
anaphylaxis
Ara h 1 antigen
Ara h 2 antigen
basophil
Clinical trials
Dosage
Food allergies
food allergy
Hypersensitivity
Immunoglobulin E
Immunoglobulin G
Immunotherapy
Monoclonal antibodies
omalizumab
oral immunotherapy
paediatrics
Patients
Title Individually dosed omalizumab facilitates peanut oral immunotherapy in peanut allergic adolescents
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