Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms

Laurian Zuidmeer-Jongejan; Montserrat Fernández-Rivas; Marcel G. T. Winter; Jaap H. Akkerdaas; Colin Summers; Ans Lebens; André C. Knulst; Piet Schilte; Peter Briza; Gabriele Gadermaier; Ronald van Ree

doi:https://doi.org/10.1186/2045-7022-4

Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms

Laurian Zuidmeer-Jongejan, Montserrat Fernández-Rivas, Marcel G. T. Winter, Jaap H. Akkerdaas, Colin Summers, Ans Lebens, André C. Knulst, Piet Schilte, Peter Briza, Gabriele Gadermaier, Ronald van Ree

Research output: Contribution to journal › Article › Academic › peer-review

50 Citations (Scopus)

Abstract

Background: Oil body-associated allergens such as oleosins have been reported for important allergenic foods such as peanut, sesame and hazelnut. Here we investigate whether oil body associated proteins (OAPs) are linked with specific clinical phenotypes and whether they are represented in skin prick test (SPT) reagents. Methods: A hazelnut OAP fraction was characterized by mass-spectrometry (MS) to identify its major constituents. Polyclonal rabbit antibodies were generated against hazelnut OAPs. The presence of OAPs in commercially available hazelnut SPTs was studied by immunoblot and spiking experiments. OAP specific IgE antibodies were measured in sera from patients with a convincing history of hazelnut allergy by RAST (n = 91), immunoblot (n = 22) and basophil histamine release (BHR; n = 14). Results: Hazelnut OAPs were analysed by MS and found to be dominated by oleosins at similar to 14 and similar to 17 kDa, and a 27 kDa band containing oleosin dimers and unidentified protein. In 36/91 sera specific IgE against hazelnut OAPs was detected, and confirmed to be biologically active by BHR (n = 14). The majority (21/22) recognized the oleosin bands at 17 kDa on immunoblot, of which 11 exclusively. These OAP-specific IgE responses dominated by oleosin were associated with systemic reactions to hazelnut (OR 4.24; p = 0.015) and negative SPT (X-2 6.3, p = 0.012). Immunoblot analysis using OAP-specific rabbit antiserum demonstrated that commercial SPT reagents are virtually devoid of OAPs, sometimes (3/9) resulting in false-negative SPT. Spiking of SPT reagents with OAP restored serum IgE binding of these false-negative patients on immunoblot at mainly 17 kDa. Conclusion: Hazelnut allergens found in oil bodies dominated by oleosin are associated with more severe systemic reactions and negative SPT. Defatted diagnostic extracts are virtually devoid of these allergens, resulting in poor sensitivity for detection of IgE antibodies against these clinically relevant molecules

Original language	English
Pages (from-to)	4
Journal	Clinical and Translational Allergy
Volume	4
Issue number	1
DOIs	https://doi.org/10.1186/2045-7022-4
Publication status	Published - 2014

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https://doi.org/10.1186/2045-7022-4

Cite this

Zuidmeer-Jongejan, L., Fernández-Rivas, M., Winter, M. G. T., Akkerdaas, J. H., Summers, C., Lebens, A., Knulst, A. C., Schilte, P., Briza, P., Gadermaier, G., & van Ree, R. (2014). Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms. Clinical and Translational Allergy, 4(1), 4. https://doi.org/10.1186/2045-7022-4

@article{e8a169f952fa43be8675e1f04ac6a3d8,

title = "Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms",

abstract = "Background: Oil body-associated allergens such as oleosins have been reported for important allergenic foods such as peanut, sesame and hazelnut. Here we investigate whether oil body associated proteins (OAPs) are linked with specific clinical phenotypes and whether they are represented in skin prick test (SPT) reagents. Methods: A hazelnut OAP fraction was characterized by mass-spectrometry (MS) to identify its major constituents. Polyclonal rabbit antibodies were generated against hazelnut OAPs. The presence of OAPs in commercially available hazelnut SPTs was studied by immunoblot and spiking experiments. OAP specific IgE antibodies were measured in sera from patients with a convincing history of hazelnut allergy by RAST (n = 91), immunoblot (n = 22) and basophil histamine release (BHR; n = 14). Results: Hazelnut OAPs were analysed by MS and found to be dominated by oleosins at similar to 14 and similar to 17 kDa, and a 27 kDa band containing oleosin dimers and unidentified protein. In 36/91 sera specific IgE against hazelnut OAPs was detected, and confirmed to be biologically active by BHR (n = 14). The majority (21/22) recognized the oleosin bands at 17 kDa on immunoblot, of which 11 exclusively. These OAP-specific IgE responses dominated by oleosin were associated with systemic reactions to hazelnut (OR 4.24; p = 0.015) and negative SPT (X-2 6.3, p = 0.012). Immunoblot analysis using OAP-specific rabbit antiserum demonstrated that commercial SPT reagents are virtually devoid of OAPs, sometimes (3/9) resulting in false-negative SPT. Spiking of SPT reagents with OAP restored serum IgE binding of these false-negative patients on immunoblot at mainly 17 kDa. Conclusion: Hazelnut allergens found in oil bodies dominated by oleosin are associated with more severe systemic reactions and negative SPT. Defatted diagnostic extracts are virtually devoid of these allergens, resulting in poor sensitivity for detection of IgE antibodies against these clinically relevant molecules",

author = "Laurian Zuidmeer-Jongejan and Montserrat Fern{\'a}ndez-Rivas and Winter, {Marcel G. T.} and Akkerdaas, {Jaap H.} and Colin Summers and Ans Lebens and Knulst, {Andr{\'e} C.} and Piet Schilte and Peter Briza and Gabriele Gadermaier and {van Ree}, Ronald",

year = "2014",

doi = "https://doi.org/10.1186/2045-7022-4",

language = "English",

volume = "4",

pages = "4",

journal = "Clinical and Translational Allergy",

issn = "2045-7022",

publisher = "BioMed Central",

number = "1",

}

Zuidmeer-Jongejan, L, Fernández-Rivas, M, Winter, MGT, Akkerdaas, JH, Summers, C, Lebens, A, Knulst, AC, Schilte, P, Briza, P, Gadermaier, G & van Ree, R 2014, 'Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms', Clinical and Translational Allergy, vol. 4, no. 1, pp. 4. https://doi.org/10.1186/2045-7022-4

Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms. / Zuidmeer-Jongejan, Laurian; Fernández-Rivas, Montserrat; Winter, Marcel G. T. et al.
In: Clinical and Translational Allergy, Vol. 4, No. 1, 2014, p. 4.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - Oil body-associated hazelnut allergens including oleosins are underrepresented in diagnostic extracts but associated with severe symptoms

AU - Zuidmeer-Jongejan, Laurian

AU - Fernández-Rivas, Montserrat

AU - Winter, Marcel G. T.

AU - Akkerdaas, Jaap H.

AU - Summers, Colin

AU - Lebens, Ans

AU - Knulst, André C.

AU - Schilte, Piet

AU - Briza, Peter

AU - Gadermaier, Gabriele

AU - van Ree, Ronald

PY - 2014

Y1 - 2014

N2 - Background: Oil body-associated allergens such as oleosins have been reported for important allergenic foods such as peanut, sesame and hazelnut. Here we investigate whether oil body associated proteins (OAPs) are linked with specific clinical phenotypes and whether they are represented in skin prick test (SPT) reagents. Methods: A hazelnut OAP fraction was characterized by mass-spectrometry (MS) to identify its major constituents. Polyclonal rabbit antibodies were generated against hazelnut OAPs. The presence of OAPs in commercially available hazelnut SPTs was studied by immunoblot and spiking experiments. OAP specific IgE antibodies were measured in sera from patients with a convincing history of hazelnut allergy by RAST (n = 91), immunoblot (n = 22) and basophil histamine release (BHR; n = 14). Results: Hazelnut OAPs were analysed by MS and found to be dominated by oleosins at similar to 14 and similar to 17 kDa, and a 27 kDa band containing oleosin dimers and unidentified protein. In 36/91 sera specific IgE against hazelnut OAPs was detected, and confirmed to be biologically active by BHR (n = 14). The majority (21/22) recognized the oleosin bands at 17 kDa on immunoblot, of which 11 exclusively. These OAP-specific IgE responses dominated by oleosin were associated with systemic reactions to hazelnut (OR 4.24; p = 0.015) and negative SPT (X-2 6.3, p = 0.012). Immunoblot analysis using OAP-specific rabbit antiserum demonstrated that commercial SPT reagents are virtually devoid of OAPs, sometimes (3/9) resulting in false-negative SPT. Spiking of SPT reagents with OAP restored serum IgE binding of these false-negative patients on immunoblot at mainly 17 kDa. Conclusion: Hazelnut allergens found in oil bodies dominated by oleosin are associated with more severe systemic reactions and negative SPT. Defatted diagnostic extracts are virtually devoid of these allergens, resulting in poor sensitivity for detection of IgE antibodies against these clinically relevant molecules

AB - Background: Oil body-associated allergens such as oleosins have been reported for important allergenic foods such as peanut, sesame and hazelnut. Here we investigate whether oil body associated proteins (OAPs) are linked with specific clinical phenotypes and whether they are represented in skin prick test (SPT) reagents. Methods: A hazelnut OAP fraction was characterized by mass-spectrometry (MS) to identify its major constituents. Polyclonal rabbit antibodies were generated against hazelnut OAPs. The presence of OAPs in commercially available hazelnut SPTs was studied by immunoblot and spiking experiments. OAP specific IgE antibodies were measured in sera from patients with a convincing history of hazelnut allergy by RAST (n = 91), immunoblot (n = 22) and basophil histamine release (BHR; n = 14). Results: Hazelnut OAPs were analysed by MS and found to be dominated by oleosins at similar to 14 and similar to 17 kDa, and a 27 kDa band containing oleosin dimers and unidentified protein. In 36/91 sera specific IgE against hazelnut OAPs was detected, and confirmed to be biologically active by BHR (n = 14). The majority (21/22) recognized the oleosin bands at 17 kDa on immunoblot, of which 11 exclusively. These OAP-specific IgE responses dominated by oleosin were associated with systemic reactions to hazelnut (OR 4.24; p = 0.015) and negative SPT (X-2 6.3, p = 0.012). Immunoblot analysis using OAP-specific rabbit antiserum demonstrated that commercial SPT reagents are virtually devoid of OAPs, sometimes (3/9) resulting in false-negative SPT. Spiking of SPT reagents with OAP restored serum IgE binding of these false-negative patients on immunoblot at mainly 17 kDa. Conclusion: Hazelnut allergens found in oil bodies dominated by oleosin are associated with more severe systemic reactions and negative SPT. Defatted diagnostic extracts are virtually devoid of these allergens, resulting in poor sensitivity for detection of IgE antibodies against these clinically relevant molecules

U2 - https://doi.org/10.1186/2045-7022-4

DO - https://doi.org/10.1186/2045-7022-4

M3 - Article

C2 - 24484687

SN - 2045-7022

VL - 4

SP - 4

JO - Clinical and Translational Allergy

JF - Clinical and Translational Allergy

IS - 1

ER -