Risk assessment in anaphylaxis: Current and future approaches

F. Estelle R. Simons; Anthony J. Frew; Ignacio J. Ansotegui; Bruce S. Bochner; David B.K. Golden; Fred D. Finkelman; Donald Y.M. Leung; Jan Lotvall; Gianni Marone; Dean D. Metcalfe; Ulrich Müller; Lanny J. Rosenwasser; Hugh A. Sampson; Lawrence B. Schwartz; Marianne van Hage; Andrew F. Walls

doi:10.1016/j.jaci.2007.05.001

Risk assessment in anaphylaxis: Current and future approaches

F. Estelle R. Simons, Anthony J. Frew, Ignacio J. Ansotegui, Bruce S. Bochner, David B.K. Golden, Fred D. Finkelman, Donald Y.M. Leung, Jan Lotvall, Gianni Marone, Dean D. Metcalfe, Ulrich Müller, Lanny J. Rosenwasser, Hugh A. Sampson, Lawrence B. Schwartz, Marianne van Hage, Andrew F. Walls

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

239 Scopus citations

Abstract

Risk assessment of individuals with anaphylaxis is currently hampered by lack of (1) an optimal and readily available laboratory test to confirm the clinical diagnosis of an anaphylaxis episode and (2) an optimal method of distinguishing allergen-sensitized individuals who are clinically tolerant from those at risk for anaphylaxis episodes after exposure to the relevant allergen. Our objectives were to review the effector mechanisms involved in the pathophysiology of anaphylaxis; to explore the possibility of developing an optimal laboratory test to confirm the diagnosis of an anaphylaxis episode, and the possibility of improving methods to distinguish allergen sensitization from clinical reactivity; and to develop a research agenda for risk assessment in anaphylaxis. Researchers from the American Academy of Allergy, Asthma & Immunology and the European Academy of Allergology and Clinical Immunology held a PRACTALL (Practical Allergy) meeting to discuss these objectives. New approaches being investigated to support the clinical diagnosis of anaphylaxis include serial measurements of total tryptase in serum during an anaphylaxis episode, and measurement of baseline total tryptase levels after the episode. Greater availability of the test for mature β-tryptase, a more specific mast cell activation marker for anaphylaxis than total tryptase, is needed. Measurement of chymase, mast cell carboxypeptidase A3, platelet-activating factor, and other mast cell products may prove to be useful. Consideration should be given to measuring a panel of mediators from mast cells and basophils. New approaches being investigated to help distinguish sensitized individuals at minimum or no risk from those at increased risk of developing anaphylaxis include measurement of the ratio of allergen-specific IgE to total IgE, determination of IgE directed at specific allergenic epitopes, measurement of basophil activation markers by using flow cytometry, and assessment of allergen-specific cytokine responses. Algorithms have been developed for risk assessment of individuals with anaphylaxis, along with a research agenda for studies that could lead to an improved ability to confirm the clinical diagnosis of anaphylaxis and to identify allergen-sensitized individuals who are at increased risk of anaphylaxis.

Original language	English (US)
Pages (from-to)	S2-S24
Journal	Journal of Allergy and Clinical Immunology
Volume	120
Issue number	1 SUPPL.
DOIs	https://doi.org/10.1016/j.jaci.2007.05.001
State	Published - Jul 2007
Externally published	Yes

Keywords

Anaphylaxis
FcεRI
IgE
allergens
basophil
food allergy
histamine
insect venom allergy
mast cell
mast cell carboxypeptidase
tryptase

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.1016/j.jaci.2007.05.001

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Simons, F. E. R., Frew, A. J., Ansotegui, I. J., Bochner, B. S., Golden, D. B. K., Finkelman, F. D., Leung, D. Y. M., Lotvall, J., Marone, G., Metcalfe, D. D., Müller, U., Rosenwasser, L. J., Sampson, H. A., Schwartz, L. B., van Hage, M., & Walls, A. F. (2007). Risk assessment in anaphylaxis: Current and future approaches. Journal of Allergy and Clinical Immunology, 120(1 SUPPL.), S2-S24. https://doi.org/10.1016/j.jaci.2007.05.001

Simons, FER, Frew, AJ, Ansotegui, IJ, Bochner, BS, Golden, DBK, Finkelman, FD, Leung, DYM, Lotvall, J, Marone, G, Metcalfe, DD, Müller, U, Rosenwasser, LJ, Sampson, HA, Schwartz, LB, van Hage, M & Walls, AF 2007, 'Risk assessment in anaphylaxis: Current and future approaches', Journal of Allergy and Clinical Immunology, vol. 120, no. 1 SUPPL., pp. S2-S24. https://doi.org/10.1016/j.jaci.2007.05.001

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abstract = "Risk assessment of individuals with anaphylaxis is currently hampered by lack of (1) an optimal and readily available laboratory test to confirm the clinical diagnosis of an anaphylaxis episode and (2) an optimal method of distinguishing allergen-sensitized individuals who are clinically tolerant from those at risk for anaphylaxis episodes after exposure to the relevant allergen. Our objectives were to review the effector mechanisms involved in the pathophysiology of anaphylaxis; to explore the possibility of developing an optimal laboratory test to confirm the diagnosis of an anaphylaxis episode, and the possibility of improving methods to distinguish allergen sensitization from clinical reactivity; and to develop a research agenda for risk assessment in anaphylaxis. Researchers from the American Academy of Allergy, Asthma & Immunology and the European Academy of Allergology and Clinical Immunology held a PRACTALL (Practical Allergy) meeting to discuss these objectives. New approaches being investigated to support the clinical diagnosis of anaphylaxis include serial measurements of total tryptase in serum during an anaphylaxis episode, and measurement of baseline total tryptase levels after the episode. Greater availability of the test for mature β-tryptase, a more specific mast cell activation marker for anaphylaxis than total tryptase, is needed. Measurement of chymase, mast cell carboxypeptidase A3, platelet-activating factor, and other mast cell products may prove to be useful. Consideration should be given to measuring a panel of mediators from mast cells and basophils. New approaches being investigated to help distinguish sensitized individuals at minimum or no risk from those at increased risk of developing anaphylaxis include measurement of the ratio of allergen-specific IgE to total IgE, determination of IgE directed at specific allergenic epitopes, measurement of basophil activation markers by using flow cytometry, and assessment of allergen-specific cytokine responses. Algorithms have been developed for risk assessment of individuals with anaphylaxis, along with a research agenda for studies that could lead to an improved ability to confirm the clinical diagnosis of anaphylaxis and to identify allergen-sensitized individuals who are at increased risk of anaphylaxis.",

keywords = "Anaphylaxis, FcεRI, IgE, allergens, basophil, food allergy, histamine, insect venom allergy, mast cell, mast cell carboxypeptidase, tryptase",

author = "Simons, {F. Estelle R.} and Frew, {Anthony J.} and Ansotegui, {Ignacio J.} and Bochner, {Bruce S.} and Golden, {David B.K.} and Finkelman, {Fred D.} and Leung, {Donald Y.M.} and Jan Lotvall and Gianni Marone and Metcalfe, {Dean D.} and Ulrich M{\"u}ller and Rosenwasser, {Lanny J.} and Sampson, {Hugh A.} and Schwartz, {Lawrence B.} and {van Hage}, Marianne and Walls, {Andrew F.}",

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AU - Ansotegui, Ignacio J.

AU - Bochner, Bruce S.

AU - Golden, David B.K.

AU - Finkelman, Fred D.

AU - Leung, Donald Y.M.

AU - Lotvall, Jan

AU - Marone, Gianni

AU - Metcalfe, Dean D.

AU - Müller, Ulrich

AU - Rosenwasser, Lanny J.

AU - Sampson, Hugh A.

AU - Schwartz, Lawrence B.

AU - van Hage, Marianne

AU - Walls, Andrew F.

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N2 - Risk assessment of individuals with anaphylaxis is currently hampered by lack of (1) an optimal and readily available laboratory test to confirm the clinical diagnosis of an anaphylaxis episode and (2) an optimal method of distinguishing allergen-sensitized individuals who are clinically tolerant from those at risk for anaphylaxis episodes after exposure to the relevant allergen. Our objectives were to review the effector mechanisms involved in the pathophysiology of anaphylaxis; to explore the possibility of developing an optimal laboratory test to confirm the diagnosis of an anaphylaxis episode, and the possibility of improving methods to distinguish allergen sensitization from clinical reactivity; and to develop a research agenda for risk assessment in anaphylaxis. Researchers from the American Academy of Allergy, Asthma & Immunology and the European Academy of Allergology and Clinical Immunology held a PRACTALL (Practical Allergy) meeting to discuss these objectives. New approaches being investigated to support the clinical diagnosis of anaphylaxis include serial measurements of total tryptase in serum during an anaphylaxis episode, and measurement of baseline total tryptase levels after the episode. Greater availability of the test for mature β-tryptase, a more specific mast cell activation marker for anaphylaxis than total tryptase, is needed. Measurement of chymase, mast cell carboxypeptidase A3, platelet-activating factor, and other mast cell products may prove to be useful. Consideration should be given to measuring a panel of mediators from mast cells and basophils. New approaches being investigated to help distinguish sensitized individuals at minimum or no risk from those at increased risk of developing anaphylaxis include measurement of the ratio of allergen-specific IgE to total IgE, determination of IgE directed at specific allergenic epitopes, measurement of basophil activation markers by using flow cytometry, and assessment of allergen-specific cytokine responses. Algorithms have been developed for risk assessment of individuals with anaphylaxis, along with a research agenda for studies that could lead to an improved ability to confirm the clinical diagnosis of anaphylaxis and to identify allergen-sensitized individuals who are at increased risk of anaphylaxis.

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KW - mast cell carboxypeptidase

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Risk assessment in anaphylaxis: Current and future approaches

Abstract

Keywords

ASJC Scopus subject areas

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