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2. List of contributors

Author

Amie Adkin, Timothy E.H. Allen, Felipe Alves de Almeida, Lucia E. Anelich, Mark Arnold, Sandrine Auger, Tessa Avermaete, Craig Baker-Austin, Forrest L. Bayer, Kiran N. Bhilegaonkar, Xiaoyu Bi, W. Marty Blom, Alan R. Boobis, Marija Boskovic, Hans Bouwmeester, Gary Bowering, Ioannis S. Boziaris, Christopher J. Breen, Hugo Brouwer, Ian Brown, Robert L. Buchanan, Elna M. Buys, Jane M. Caldwell, Elena Canellas, Deisy Guimarães Carneiro, Karin Carstensen, Brayan R.H. Cervantes-Huamán, Roger Clemens, Luca Cocolin, Samuel M. Cohen, David Coles, Alessia Cossettini, Natália Cruz-Martins, György Csikó, Michelle Danyluk, Wageh Sobhy Darwish, Barbara De Coninck, Christina A. Mireles DeWitt, B.C. Dlamini, John Doe, Simon Douglas Kelly, Eleonora Dupouy, Gerhard Eisenbrand, James A. Elegbeleye, Pablo Estévez, Ricardo Franco-Duarte, Leonardo Luiz de Freitas, Nigel French, Lynn J. Frewer, Yuqi Fu, Shoji Fukushima, Ana Gago-Martinez, Alejandro Dorado Garcia, Steven M. Gendel, Anne Gerardi, Anuradha Ghosh, Milica Glisic, Samuel Benrejeb Godefroy, Nigel J. Gooderham, Gerard Govers, Tomasz Grenda, F. Peter Guengerich, Sandrine Guillou, Steve Gutsell, Muriel Guyard-Nicodème, Nabila Haddad, Ndaindila N.K. Haindongo, Christie L. Harman, Thomas Hartung, A. Wallace Hayes, Graham Head, Stephen S. Hecht, Jeljer Hoekstra, Louwrens Hoffman, Olivier Honnay, Geert Houben, Jan Jetten, Shan Jin, Karen Job, Snehal Kadam, Shraddha Karanth, Agnes Karmaus, Manos Karvounis, Fumiko Kasuga, Karishma S. Kaushik, Marc C. Kennedy, John G. Keogh, Wannes Keulemans, Nida Khan, Michael E. Knowles, Dimitra Kogiannou, Serhii Kolesnyk, Rahul P. Kolhe, Timm Konold, Zoi Kotsiri, Matt Krug, Krzysztof Kwiatek, Youngjoo Kwon, Francesca Latronico, José M. Leao, Jeffrey T. LeJeune, Wenjing Li, Matthew J. Linman, Rebeca López-García, Thomas Luechtefeld, Bernadene Magnuson, Louise Manning, Nikos Manouselis, Marisa Manzano, Marco Marin, María Salomé Mariotti, Jaime Martinez-Urtaza, Lynn M. McMullen, Cronan McNamara, Angel Medina, N.N. Mehlomakulu, Jyotigna M. Mehta, Marjolein Meijerink, J. David Miller, E.N. Clare Mills, Stephen C. Mitchell, Angelo Moretto, Desmond T. Mugadza, Keya Mukherjee, Francis Z. Naab, Hanspeter Naegeli, Maristela S. Nascimento, Ivan Nastasijevic, Maarten Nauta, Lev Neretin, Cristina Nerín, Victor Ntuli, Elena G. Olson, John O’Brien, Sakshi Painuli, Efstratia Panteleli, Mihalis Papakonstantinou, Foteini F. Parlapani, Ewelina Patyra, Franco Pedreschi, Sandrine Pigat, Bert Popping, Morten Poulsen, Abani K. Pradhan, Peter Pressman, Mykola Prodanchuk, Monika Przeniosło-Siwczyńska, Ans Punt, Alfons Ramel, Abderahman Rejeb, Katherine Rich, Steven C. Ricke, Ivonne M.C.M. Rietjens, George Rigos, Carolina Ripolles-Avila, Francesco Rizzotto, Célia Fortuna Rodrigues, José Juan Rodríguez-Jerez, Martin Rose, Thomas J. Rosol, Joyjit Saha, Tor Savidge, Eyassu Seifu, Prabhakar Semwal, Thulani Sibanda, Sik Yu So, Susana Socolovsky, Giannis Stoitsis, Katelynn Stull, Marta H. Taniwaki, Sean V. Taylor, Lesa A. Thompson, Zeynal Topalcengiz, George T. Tzotzos, Michaela van den Honert, Femke L.N. Van Oijen, Maria Cristina Dantas Vanetti, Apostolos Vantarakis, Paula Vera, Jasmina Vidic, Priya Vizzini, Rosemary H. Waring, Qinglong Wu, Khaldoon Zaid-Kaylani, and Tjitske Anna Zwart

Published
2023
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3. Poor understanding of allergen labelling by allergic and non‐allergic consumers

Author

Yvette F. M. Linders, Leo Lentz, Bregje Holleman, Anouska D. Michelsen-Huisman, Geert F. Houben, André C. Knulst, Harmieke van Os-Medendorp, W. Marty Blom, Huub van den Bergh, Liselotte M. van Dijk, and Kitty C.M. Verhoeckx

Subjects
Allergy, Food Safety, business.industry, Immunology, Health literacy, Original Articles, Allergens, medicine.disease, Food safety, medicine.disease_cause, humanities, Allergen, Food, Food Labeling, Food allergy, Environmental health, Labelling, Non allergic, medicine, Humans, Immunology and Allergy, Original Article, business, Risk assessment, Food Hypersensitivity
Abstract

Background Understanding consumers’ interpretation of allergy information is crucial for effective food safety policies. We evaluated consumer understanding of allergy information on foods in controlled, experimental studies. Method Using 18 packaged foods, we evaluated consumer understanding of information about allergens in two experiments: First, a comparison of foods with no stated allergen versus allergen as a stated ingredient versus a precautionary allergen label (PAL); second, a comparison of three common variants of PAL. In each experiment, consumers with and without self‐reported food allergy were asked to estimate the risk of allergic reaction and to rate the comprehensibility of the allergen information. In the second experiment, consumers were also asked which form of PAL they preferred. Results Risk of reaction was assessed as high and low for foods with the allergen stated as ingredient, or without any mention of allergen. However, risk assessment for PAL varied and was judged as higher by non‐allergic than allergic participants (82% vs. 58%, p, Food labels are a crucial source of information for allergic consumers, but despite ingredient declaration legislation, allergic reactions frequently occur. We evaluated common allergy information on foods in two controlled experimental studies. Allergic consumers attribute lower risks to products with PAL than consumers without FA, different risks are attributed to different PAL wordings especially by consumers with higher levels of Health Literacy, and less than 50% of participants judge allergy information to be clear. Better allergy information is called for.

Published
2021
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4. The population threshold for soy as an allergenic food – Why did the Reference Dose decrease in VITAL 3.0?

Author

René W.R. Crevel, W. Marty Blom, Joost Westerhout, Joseph L. Baumert, Geert F. Houben, Benjamin C. Remington, Steve L. Taylor, and Simon Brooke-Taylor

Subjects
Reference dose, education.field_of_study, business.industry, Population, 04 agricultural and veterinary sciences, Appropriate use, 040401 food science, Cross contact, 03 medical and health sciences, 0404 agricultural biotechnology, 0302 clinical medicine, 030228 respiratory system, Infant formula, Medicine, Food science, business, education, Allergen labeling, Soy protein, Agricultural crops, Food Science, Biotechnology
Abstract

Background. Soy is globally recognized as a commonly allergenic food. The VITAL (Voluntary Incidental Trace Allergen Labeling) Scientific Expert Panel (VSEP) of the Allergen Bureau of Australia & New Zealand used data on minimal reactive doses in low-dose clinical challenges of soy-allergic individuals to elaborate and propose the first Reference Dose for soy at 1.0 mg soy protein (based on the lower 95% confidence interval of the ED05) in 2014 to guide use of precautionary allergen labeling (PAL). These data were taken from clinical challenges with soy flour or soy-based infant formula. More recently, the VSEP has examined additional data including data from challenges conducted with soy milk and used a new statistical model averaging approach to propose a new Reference Dose for soy at 0.5 mg soy protein (based on the ED01). Questions have arisen about the lowering of the soy Reference Dose and the appropriate use of this new Reference Dose in risk management for soy residues especially relating to the adventitious presence of soy in other grains, legumes and pulses emanating from agricultural comingling. Scope and approach. Several factors may have contributed to the lowering of the Reference Dose for soy including the use of the ED01 vs. the previous use of the 95% lower confidence interval of the ED05, the use of model averaging and multiple parametric statistical models, and the incorporation of additional data including the soy milk challenge data. Soy milk may differ from other forms of soy as a challenge material. The background data were examined in greater detail in an attempt to unravel the causative factor(s) behind the lowering of the soy Reference Dose. The use of the new soy Reference Dose for allergen management of the adventitious presence of soy in other agricultural crops was examined in terms of risk to soy-allergic consumers. Key finding and conclusions. The Reference Dose for soy in VITAL 3.0 decreased to 0.5 mg soy protein primarily because it was based on the ED01 rather than the 95% lower confidence interval of the ED05. Clinical data suggest that some soy-allergic individuals may react to soy milk but can tolerate soy flour and other soy-based foods. Perhaps, soy milk may be a more potent form of soy because of its minimal processing. But, with the current data available, there is no evidence to conclude that soy milk responders as a whole group display a relevantly different ED-distribution. The new soy Reference Dose impacts risk assessments for agricultural comingling, a form of cross contact that can be challenging to control on a national or international basis. The potential risks posed by agricultural comingling should be carefully examined in light of the new Reference Dose for soy protein.

Published
2021
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6. Accidental food‐allergic reactions are associated with higher costs and more sick leave but not with quality of life

Author

André C. Knulst, Thuy-My Le, Harmieke van Os-Medendorp, Astrid Versluis, Geert F. Houben, Anouska D. Michelsen-Huisman, and W. Marty Blom

Subjects
0301 basic medicine, Adult, Male, Immunology, MEDLINE, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Quality of life (healthcare), Cost of Illness, Food allergy, Clinical history, Economic cost, Environmental health, medicine, Research Letter, Immunology and Allergy, Humans, Positive serology, Aged, Netherlands, business.industry, Health Care Costs, Middle Aged, medicine.disease, Research Letters, 030104 developmental biology, 030228 respiratory system, Accidental, Sick leave, Quality of Life, Female, Sick Leave, business, Food Hypersensitivity
Abstract

The prevalence of IgE-mediated food allergy diagnosed by clinical history and positive serology in adults across Europe ranges from 0.3-6% (1). Almost half of the food allergic adults are confronted with accidental allergic reactions yearly (2). Especially moderate and severe reactions require medical consultation and treatment, which can have a high impact on economic costs (3).

Published
2021

7. Updated threshold dose-distribution data for sesame

Author

Paul J. Turner, Magdalena Gretzinger, Nandinee Patel, Helen A. Brough, R. Sharon Chinthrajah, Motohiro Ebisawa, Arnon Elizur, Jennifer J. Koplin, Rachel L. Peters, Natasha Purington, Anna Nowak‐Wegrzyn, Sarah Saf, Hugh A. Sampson, Joost Westerhout, W. Marty Blom, Joseph L. Baumert, Geert F. Houben, and Benjamin C. Remington

Subjects
Science & Technology, Allergy, 1107 Immunology, Immunology, Immunology and Allergy, Humans, Life Sciences & Biomedicine, Sesamum
Published
2022

8. Reproducibility of food challenge to cow’s milk: a systematic review with individual participant data meta-analysis

Author

Paul J. Turner, Nandinee Patel, Dianne E. Campbell, Hugh A. Sampson, Mayu Maeda, Toshio Katsunuma, Joost Westerhout, W. Marty Blom, Joseph L. Baumert, Geert F. Houben, Benjamin C. Remington, and Medical Research Council (MRC)

Subjects
Allergy, Immunology, thresholds, Reproducibility of Results, Proteins, Allergens, cow’s milk, food challenge, Milk, 1107 Immunology, precautionary allergen labeling, anaphylaxis, eliciting dose, Immunology and Allergy, Animals, Humans, Cattle, Female, Milk Hypersensitivity, Randomized Controlled Trials as Topic
Abstract

Background: Cow’s milk (CM) is an increasingly common cause of severe allergic reactions, but there is uncertainty with respect to severity of reactions at low level CM exposure, as well as the reproducibility of reaction thresholds. Objective: To undertake an individual participant data (IPD) meta-analysis of studies reporting double-blind, placebo-controlled food challenges (DBPCFC) in CM, to determine the rate of anaphylaxis to low level exposures and the reproducibility of reaction thresholds. Methods: Systematic review and individual participant data (IPD) meta-analysis of studies reporting relevant data. Authors were contacted to provide additional data and/or clarifications as needed. Risk of bias was assessed using the National Institute for Clinical Excellence methodological checklists. Results: 34 studies were included, representing data from over 1000 participants. The cumulative ED01 and ED05 (cumulative doses causing objective symptoms in 1% and 5% of the at-risk allergic population) were 0.3 (95%CI 0.2-0.5) and 2.9 (95%CI 1.6-5.4) mg, respectively. At meta-analysis, 4.8% (95%CI 2.0-10.9%) and 4.8% (95%CI 0.7-27.1%) of individuals reacting to ≤5mg and ≤0.5mg of CM protein (respectively) had anaphylaxis (minimal heterogeneity, I 2 =0%). 110 individuals subsequently underwent a repeat DBPCFC: the intra-individual variation in reaction threshold was limited to a ½-log change in 80% (95%CI 65-89%) of participants. Two individuals initially tolerated 5mg CM protein but then reacted to this dose at a subsequent challenge, although neither had anaphylaxis. Conclusions: Around 5% of CM-allergic individuals reacting to an ED01 or ED05 exposure might have anaphylaxis to that dose. This equates to 5 and 24 anaphylaxis events per 10,000 patients exposed to an ED01 or ED05 dose respectively, in the broader CM-allergic population. The vast majority of these anaphylactic reactions would be at the more mild end of the spectrum of anaphylaxis severity, responding to single dose of epinephrine.

Published
2022

9. Peanut Can Be Used as a Reference Allergen for Hazard Characterization in Food Allergen Risk Management: A Rapid Evidence Assessment and Meta-Analysis

Author

M. Hazel Gowland, Natasha Purington, Nandinee Patel, Dianne E. Campbell, Arnon Elizur, María Cristina López, Sebastien La Vieille, Hugh A. Sampson, Anthony E.J. Dubois, Eva Södergren, Motohiro Ebisawa, Benjamin C. Remington, Sabine Schnadt, E. N. Clare Mills, Barbara Ballmer-Weber, Helen A. Brough, R. Sharon Chinthrajah, Geert F. Houben, André C. Knulst, W. Marty Blom, Gustavo Alberto Polenta, Paul Turner, Jonathan Hourihane, Stephen L Taylor, Simon Brooke-Taylor, Jennifer Gerdts, Maria Said, René W.R. Crevel, Joseph L. Baumert, Hongbing Chen, Groningen Research Institute for Asthma and COPD (GRIAC), Medical Research Council (MRC), National Institute for Health Research, University of Zurich, and Turner, Paul J

Subjects
ORAL TOLERANCE INDUCTION, CLINICAL REACTIVITY, Arachis, IGE ANTIBODIES, PFAS, Pollen food allergy syndrome, WHEAT ALLERGY, medicine.disease_cause, DOUBLE-BLIND, Allergen, Dosis de Referencia, Food Labeling, immune system diseases, Alérgenos, COWS MILK ALLERGY, Immunology and Allergy, Risk management, Randomized Controlled Trials as Topic, ED, Eliciting dose, Threshold, 10177 Dermatology Clinic, Hazard, humanities, Eliciting Dose, Dosis Provocadora, Meta-analysis, CROSS-REACTIVITY, ED01, Amount of allergen expected to cause objective symptoms in 1% of the population with that allergy, 2723 Immunology and Allergy, ED05, Amount of allergen expected to cause objective symptoms in 5% of the population with that allergy, Alergia Alimentaria, THRESHOLD DOSE DISTRIBUTIONS, Eliciting dose, Food Hypersensitivity, Precautionary allergen labeling, Food Allergies, 610 Medicine & health, Legislation, Cacahuete, Maní, PAL, Precautionary allergen labeling, Risk Assessment, WHO, World Health Organization, Reference Dose, Food allergy, Environmental health, FC, Food challenge, medicine, Humans, Precautionary Allergen Labeling, Review and Feature Article, Reacciones Anafilácticas, Anaphylaxis, HENS EGG, EIA, Exercise-induced anaphylaxis, Reference dose, CI, Confidence interval, business.industry, CHALLENGE-PROVEN, Evidence-based medicine, Allergens, medicine.disease, Etiquetado Preventivo de Alérgenos, Umbral, Groundnuts, Metanálisis, respiratory tract diseases, Peanut, FAO, Food and Agriculture Organization, business, DBPCFC, Double-blind, placebo-controlled food challenge, Anaphylactic Reactions, Meta-Analysis
Abstract

Regional and national legislation mandates the disclosure of “priority” allergens when present as an ingredient in foods, but this does not extend to the unintended presence of allergens due to shared production facilities. This has resulted in a proliferation of precautionary allergen (“may contain”) labels (PAL) that are frequently ignored by food-allergic consumers. Attempts have been made to improve allergen risk management to better inform the use of PAL, but a lack of consensus has led to variety of regulatory approaches and nonuniformity in the use of PAL by food businesses. One potential solution would be to establish internationally agreed “reference doses,” below which no PAL would be needed. However, if reference doses are to be used to inform the need for PAL, then it is essential to characterize the hazard associated with these low-level exposures. For peanut, there are now published data relating to over 3000 double-blind, placebo-controlled challenges in allergic individuals, but a similar level of evidence is lacking for other priority allergens. We present the results of a rapid evidence assessment and meta-analysis for the risk of anaphylaxis to a low-level allergen exposure for priority allergens. On the basis of this analysis, we propose that peanut can and should be considered an exemplar allergen for the hazard characterization at a low-level allergen exposure. Resumen: La legislación regional y nacional exige la divulgación de alérgenos "prioritarios" cuando están presentes como ingrediente en los alimentos, pero esto no se extiende a la presencia involuntaria de alérgenos debido a instalaciones de producción compartidas. Esto ha dado lugar a una proliferación de etiquetas de precaución para alérgenos ("pueden contener") (PAL) que los consumidores alérgicos a los alimentos suelen ignorar. Se han hecho intentos para mejorar la gestión del riesgo de alérgenos para informar mejor el uso de PAL, pero la falta de consenso ha llevado a una variedad de enfoques regulatorios y a la falta de uniformidad en el uso de PAL por parte de las empresas alimentarias. Una posible solución sería establecer “dosis de referencia” acordadas internacionalmente, por debajo de las cuales no se necesitaría PAL. Sin embargo, si se van a utilizar dosis de referencia para informar la necesidad de PAL, entonces es esencial caracterizar el peligro asociado con estas exposiciones de bajo nivel. Para el maní, ahora hay datos publicados relacionados con más de 3000 desafíos doble ciego controlados por placebo en individuos alérgicos, pero falta un nivel similar de evidencia para otros alérgenos prioritarios. Presentamos los resultados de una evaluación rápida de la evidencia y un metanálisis del riesgo deanafilaxia a una exposición a alérgenos de bajo nivel para alérgenos prioritarios. Sobre la base de este análisis, proponemos que el cacahuete puede y debe considerarse un alérgeno ejemplar para la caracterización del peligro en una exposición a un alérgeno de bajo nivel. Instituto de Investigación de Tecnología de Alimentos Fil: Turner, Paul J. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Patel, Nandinee. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Ballmer-Weber, Barbara K. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Ballmer-Weber, Barbara K. Clínica de Dermatología y Alergología. Kantonsspital; Suiza. Fil: Baumert, Joe L. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Blom, W. Marty. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Brooke-Taylor, Simon. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Brough, Helen. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Brough, Helen. King's College London. Departamento de Alergia Pediátrica; Reino Unido. Fil: Campbell, Dianne E. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Campbell, Dianne E. Tecnologías DBV. Montrouge; Francia. Fil: Chen, Hongbing. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Chinthrajah, R. Sharon. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Crevel, René W.R. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Dubois, Anthony E.J. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Ebisawa, Motohiro. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Elizur, Arnon. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Elizur, Arnon. Universidad de Tel Aviv. Facultad de Medicina Sackler. Departamento de Pediatría; Israel. Fil: Gerdts, Jennifer D. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Gowland, M. Hazel. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Houben, Geert F. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Hourihane, Jonathan O.B. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Knulst, André C. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: La Vieille, Sébastien. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: López, María Cristina. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Mills, E.N. Clare. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Polenta, Gustavo Alberto. Instituto Nacional de Tecnología Agropecuaria (INTA). Instituto de Investigación Tecnología de Alimentos; Argentina. Fil: Polenta, Gustavo Alberto. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Purington, Natasha. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Said, María. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Sampson, Hugh A. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Sampson, Hugh A. Escuela de Medicina Icahn. División de Alergia e Inmunología Pediátricasen. Nueva York. Estados Unidos de América. Fil: Schnadt, Sabine. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Södergren, Eva. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Södergren, Eva. ThermoFisher Scientific; Suecia. Fil: Taylor, Stephen L. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Remington, Benjamin C. Imperial College London. Instituto Nacional del Corazón y los Pulmones; Reino Unido. Fil: Remington, Benjamin C. Grupo BV. Consultoría Remington; Holanda.

Published
2022

10. Deriving individual threshold doses from clinical food challenge data for population risk assessment of food allergens

Author

Benjamin C. Remington, Joost Westerhout, Jennifer J. Koplin, Thuy My Le, Hugh A. Sampson, W. Marty Blom, Wayne G. Shreffler, Matthew Greenhawt, René W.R. Crevel, Geert F. Houben, Montserrat Fernandez-Rivas, Jonathan O'b Hourihane, Katrina J. Allen, Anthony E.J. Dubois, Joseph L. Baumert, Barbara Ballmer-Weber, Astrid G. Kruizinga, Steve L. Taylor, Paul Turner, University of Zurich, Blom, W Marty, and Groningen Research Institute for Asthma and COPD (GRIAC)

Subjects
Male, no observed adverse effect level-lowest observed adverse effect level derivation, double-blind, placebo-controlled food challenge, Administration, Oral, CHILDREN, food challenge, placebo-controlled food challenge, DOUBLE-BLIND, threshold, eliciting dose, Immunology and Allergy, Decision-making, Risk management, education.field_of_study, Biological Variation, Individual, 10177 Dermatology Clinic, risk assessment, Child, Preschool, no observed adverse effect level–lowest observed adverse effect level derivation, 2723 Immunology and Allergy, Female, Risk assessment, Food Hypersensitivity, medicine.medical_specialty, Resource (biology), EUROPE, Maximum Tolerated Dose, Clinical Decision-Making, Population, Immunology, 610 Medicine & health, PEANUT, DIAGNOSIS, risk management, Double-Blind Method, Population Groups, Food allergy, Environmental health, medicine, Journal Article, Humans, education, No-Observed-Adverse-Effect Level, 2403 Immunology, decision-making process, business.industry, Public health, Infant, Allergens, Placebo Effect, medicine.disease, Food, Immunization, Population Risk, business
Abstract

Background: Food allergies are a significant public health issue, and the only effective management option currently available is strict avoidance of all foods containing the allergen. In view of the practical impossibility of limiting risks to zero, quantitative allergen risk assessment and management strategies are needed. Objective: We sought to develop appropriate methods for informing population-based risk assessments and risk management programs to benefit all stakeholders but particularly patients with food allergy. Methods: Individual thresholds for food allergens (maximum tolerable doses and minimum eliciting doses) can ideally be established through double-blind, placebo-controlled food challenges. If double-blind, placebo-controlled food challenge data are not available, data from widely used open food challenges using predefined objective criteria can also provide useful data regarding minimum eliciting doses. For more than 20 years, the Netherlands Organisation for Applied Scientific Research and the Food Allergy Research and Resource Program at the University of Nebraska-Lincoln have been collecting individual maximum tolerable doses and minimum eliciting doses that produce objective symptoms from published and unpublished clinical data to better refine knowledge regarding the sensitivity of the population to food allergens. Results: In this article we provide in-depth insights into the methodology applied by the Netherlands Organisation for Applied Scientific Research and Food Allergy Research and Resource Program to derive individual maximum tolerable doses and minimum eliciting doses for objective symptoms from clinical food challenge data. More than 90 examples for determining individual allergic thresholds are presented. Conclusion: With the methodology presented in this article, we aim to stimulate harmonization and transparency in quantitative food allergen risk assessment and risk management programs, encouraging their wider adoption. © 2019 American Academy of Allergy, Asthma & Immunology

Published
2019

11. Evidence‐based approaches to the application of precautionary allergen labelling: Report from two iFAAM workshops

Author

Audrey DunnGalvin, Lynne Regent, Sabine Schnadt, Moira Austin, Stephen L Taylor, Astrid G. Kruizinga, E. N. Clare Mills, Graham Roberts, Joseph L. Baumert, Siân Astley, W. Marty Blom, Michael Walker, Chun Han Chan, Kate Grimshaw, and René W.R. Crevel

Subjects
0301 basic medicine, medicine.medical_specialty, Allergy, Food industry, Immunology, medicine.disease_cause, Education, 03 medical and health sciences, 0302 clinical medicine, Allergen, Food Labeling, Food allergy, Environmental health, Labelling, medicine, Animals, Humans, Immunology and Allergy, May contain, Risk management, Risk Management, business.industry, Public health, digestive, oral, and skin physiology, Allergens, medicine.disease, humanities, 030104 developmental biology, Precautionary labelling, 030228 respiratory system, Business, Risk assessment, Food Analysis, Food Hypersensitivity
Abstract

Food allergy is a major public health concern with avoidance of the trigger food(s) being central to management by the patient. Food information legislation mandates the declaration of allergenic ingredients; however, the labelling of the unintentional presence of allergens is less defined. Precautionary allergen labelling (PAL) was introduced by the food industry to help manage and communicate the risk of reaction from the unintended presence of allergens in foods. In its current form, PAL is counterproductive for consumers with food allergies as there is no standardised approach to applying PAL. Foods with a PAL often do not contain the identified food allergen while some products without a PAL contain quantities of common food allergens that are capable of inducing an allergic reaction. Integrated Approaches to Food Allergen and Allergy Risk Management (iFAAM) was an EU-funded project that aimed to improve the management of food allergens by the food industry for the benefit of people with food allergies. Within iFAAM, a clinically validated tiered risk assessment approach for food allergens was developed. Two cross-stakeholder iFAAM workshops were held on 13th -14th December 2016 and 19th -20th April 2018. One of the objectives of these workshops was to develop a proposal to make PAL effective for consumers. This paper describes the outcomes from these workshops. This provides the basis for the development of more informative and transparent labelling that will ultimately improve management and well-being in consumers with food allergy. This article is protected by copyright. All rights reserved.

Published
2019
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12. Updated full range of Eliciting Dose values for Cow's milk for use in food allergen risk assessment

Author

W. Marty Blom, Joost Westerhout, Joseph L. Baumert, Marie Y. Meima, Paul J. Turner, Motohiro Ebisawa, Noriyuki Yanagida, Benjamin C. Remington, Geert F. Houben, and J P Moulton Charitable Foundation

Subjects
General Medicine, Allergens, Milk Proteins, Toxicology, Risk Assessment, Eliciting Dose, Milk, Allergenic food, Risk management, Food allergy, Food allergen, Animals, Cattle, Female, Milk Hypersensitivity, 0908 Food Sciences, Food Hypersensitivity, Food Science
Abstract

Access to Eliciting Doses (ED) for allergens enables advanced food allergen risk assessment. Previously, the full ED range for 14 allergenic foods, including milk, and recommendations for their use were provided (Houben et al., 2020). Additional food challenge studies with cow's milk-allergic patients added 247 data points to the original dataset. Using the Stacked Model Averaging statistical method for interval-censored data on the 697 individual NOAELs and LOAELs for milk generated an updated full ED distribution. The ED01 and ED05, the doses at which 1% and 5% of the milk-allergic population would be predicted to experience any objective allergic reaction, were 0.3 and 3.2 mg milk protein for the discrete and 0.4 mg and 4.3 mg milk protein for the cumulative dose distribution, respectively. These values are slightly higher but remain within the 95% confidence interval of previously published EDs. We recommend using the updated EDs for future characterization of risks of exposure of milk-allergic individuals to milk protein. This paper contributes to the discussion on the Reference Dose for milk in the recent Ad hoc Joint FAO/WHO Expert Consultation on Risk Assessment of Food Allergens. It will also benefit harmonization of food allergen risk assessment and risk management globally.

Published
2022
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13. Allergen quantitative risk assessment within food operations: Concepts towards development of practical guidance based on an ILSI Europe workshop

Author

Benjamin C. Remington, Joseph Baumert, W. Marty Blom, Luca Bucchini, Neil Buck, René Crevel, Fleur De Mooij, Simon Flanagan, James Hindley, Bushra Javed, Despoina Angeliki Stavropoulou, Myrthe W. van den Dungen, Marjan van Ravenhorst, Si Wang, and Michael Walker

Subjects
Food Science, Biotechnology
Published
2022
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14. Suitability of low-dose, open food challenge data to supplement double-blind, placebo-controlled data in generation of food allergen threshold dose distributions

Author

Anthony E.J. Dubois, Steve L. Taylor, Benjamin C. Remington, Geert F. Houben, Astrid G. Kruizinga, W. Marty Blom, Joost Westerhout, Joseph L. Baumert, and Groningen Research Institute for Asthma and COPD (GRIAC)

Subjects
Male, medicine.medical_specialty, Adolescent, Immunology, Dose-Response Relationship, Immunologic, Information Storage and Retrieval, Placebo, Double blind, Placebos, Corylus, Double-Blind Method, Internal medicine, medicine, Immunology and Allergy, Humans, Peanut Hypersensitivity, Food allergens, Child, Egg Hypersensitivity, Risk Management, business.industry, Low dose, Infant, Allergens, Threshold dose, Child, Preschool, Female, Nut Hypersensitivity, RISK-ASSESSMENT, Milk Hypersensitivity, business, Food Hypersensitivity
Published
2021

15. Allergen risk assessment: Food intake levels of the general population represent those of food allergic patients

Author

Anouska D. Michelsen-Huisman, Geert F. Houben, Anne M van Dijk, Harmieke van Os-Medendorp, Carina M. Rubingh, W. Marty Blom, André C. Knulst, Sabina Bijlsma, and Astrid G. Kruizinga

Subjects
Male, Food intake, Population, Toxicology, medicine.disease_cause, Risk Assessment, Food group, Cohort Studies, 03 medical and health sciences, 0404 agricultural biotechnology, Allergen, Environmental health, medicine, Humans, Matched sample, education, Risk management, 030304 developmental biology, 0303 health sciences, education.field_of_study, Adult patients, business.industry, digestive, oral, and skin physiology, 04 agricultural and veterinary sciences, General Medicine, Allergens, 040401 food science, Female, Risk assessment, business, Food Hypersensitivity, Food Science
Abstract

Unintentional intake of allergens through food products poses a daily risk for allergic patients. Models estimating the risk of reactions mostly use intake data from general population surveys. Our study evaluates the comparability of food intake levels in the general population to those in the food allergic population. Data were collected by a 24-h recall method on 2 non-consecutive days in 38 cow's milk and/or hen's egg and 35 peanut and/or tree nut allergic adult patients. All products were assigned to food groups previously developed for allergen risk assessment. Food intake distributions from the allergic populations and a matched sample from the Dutch National Food Consumption Survey were compared, and risk assessments were performed. Food intake data was obtained for 92% of the food groups. Comparison of the intake showed no statistically significant differences between either of the two allergic populations and the general population. Consequently, only small variations in estimated risks were found, that would not result in different risk management decisions. In conclusion, food intake data from the general population can be used for food allergen risk assessment and will not lead to a relevant under- or overestimation of the risk for the food allergic population.

Published
2020

16. Risk of shared equipment in restaurants for consumers with peanut allergy: a simulation for preparing Asian foods: A simulation for preparing Asian foods

Author

Benjamin C, Remington, W Marty, Blom, Boris, Bassa, and Stef J, Koppelman

Subjects
Restaurants, Arachis, Immune Tolerance, Equipment Contamination, Food Contamination, Cooking, Allergens, Cooking and Eating Utensils, Risk Assessment, Plant Proteins
Abstract

Allergic reactions to meals consumed outside the home are common and can be severe and sometimes fatal.To quantify the risk reduction potentially achieved by increasing an individual's threshold sensitivity to peanut (such as by means of immunotherapy) in scenarios of peanut exposure through shared kitchen materials in a restaurant setting.Three versions of popular peanut-containing sauces were selected to represent common ingredients used in Asian cooking. Different combinations of utensils, equipment, sauces, and test conditions were prepared by a professional chef, with or without common cleaning procedures, to represent normal daily practice. Residue amounts of peanut-containing material on kitchen equipment and utensils were measured and used for quantitative risk assessment to model the risk reduction associated with increasing an individual's threshold.Shared utensils had mean residue amounts of 23 to 1519 mg peanut protein (no cleaning) and 3 to 82 mg peanut protein (after water rinse). Shared woks and pans had up to 20 mg peanut protein after rinsing. Individuals who reach a threshold of 300 mg peanut protein have a predicted relative risk reduction of 94.9% to greater than 99.99% with brief cleaning. With no cleaning, relative risk reductions were 63.5% to 91.1% for individuals with a baseline threshold of less than or equal to 100 mg peanut protein who reach a threshold of 300 mg peanut protein, increasing to 91% to 99.7% when reaching a threshold value of 1000 mg peanut protein.In all shared kitchen material scenarios that we studied, achieving an eliciting dose of 300 or 1000 mg peanut protein seems clinically relevant for the peanut-allergic population.

Published
2020

17. Accidental allergic reactions in food allergy: Causes related to products and patient's management

Author

Harmieke van Os-Medendorp, W. Marty Blom, Astrid Versluis, Hubert P.J.M. Noteborn, Jacqueline J.M. Castenmiller, Anouska D. Michelsen-Huisman, Astrid G. Kruizinga, André C. Knulst, and Geert F. Houben

Subjects
Adult, Male, Adolescent, Immunology, Young Adult, 03 medical and health sciences, 0404 agricultural biotechnology, 0302 clinical medicine, Patient Education as Topic, Food Labeling, Food allergy, Environmental health, Humans, Immunology and Allergy, Medicine, Prospective Studies, Letters to the Editor, Letter to the Editor, Aged, business.industry, 04 agricultural and veterinary sciences, Middle Aged, medicine.disease, 040401 food science, 030228 respiratory system, Accidental, Female, Self Report, business, Food Hypersensitivity, Follow-Up Studies
Published
2018
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18. Assessing food allergy risks from residual peanut protein in highly refined vegetable oil

Author

Astrid G. Kruizinga, W. Marty Blom, René W.R. Crevel, Ben Remington, Carina M. Rubingh, and Geert F. Houben

Subjects
Arachis, Refined peanut oil, Food Contamination, Toxicology, Residual, Risk Assessment, 03 medical and health sciences, 0404 agricultural biotechnology, 0302 clinical medicine, Food allergy, Labelling, medicine, Humans, Plant Oils, Peanut Hypersensitivity, Food science, Health risk, Plant Proteins, Chemistry, food and beverages, 04 agricultural and veterinary sciences, General Medicine, Clinical literature, medicine.disease, 040401 food science, Vegetable oil, 030228 respiratory system, Food products, Food Science
Abstract

Refined vegetable oils including refined peanut oil are widely used in foods. Due to shared production processes, refined non-peanut vegetable oils can contain residual peanut proteins. We estimated the predicted number of allergic reactions to residual peanut proteins using probabilistic risk assessment applied to several scenarios involving food products made with vegetable oils. Variables considered were: a) the estimated production scale of refined peanut oil, b) estimated cross-contact between refined vegetable oils during production, c) the proportion of fat in representative food products and d) the peanut protein concentration in refined peanut oil. For all products examined the predicted risk of objective allergic reactions in peanut-allergic users of the food products was extremely low. The number of predicted reactions ranged depending on the model from a high of 3 per 1000 eating occasions (Weibull) to no reactions (LogNormal). Significantly, all reactions were predicted for allergen intakes well below the amounts reported for the most sensitive individual described in the clinical literature. We conclude that the health risk from cross-contact between vegetable oils and refined peanut oil is negligible. None of the food products would warrant precautionary labelling for peanut according to the VITAL® programme of the Allergen Bureau. © 2017 Elsevier Ltd

Published
2017
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19. Threshold Dose Distribution in Walnut Allergy

Author

W. Marty Blom, Rob J.B. Klemans, Steve L. Taylor, André C. Knulst, Joseph L. Baumert, Mark A. Blankestijn, Geert F. Houben, and Benjamin C. Remington

Subjects
Adult, Male, Risk, Allergy, medicine.medical_specialty, Walnut, No-observed-adverse-effect level, Food industry, Population, Administration, Oral, Juglans, Toxicology, 03 medical and health sciences, 0404 agricultural biotechnology, 0302 clinical medicine, Food Labeling, Food allergy, Journal Article, medicine, Humans, Immunology and Allergy, Prospective Studies, Adverse effect, education, education.field_of_study, business.industry, 04 agricultural and veterinary sciences, Allergens, Eliciting doses, medicine.disease, 040401 food science, Surgery, Allergen thresholds, Lowest-observed-adverse-effect level, Threshold dose, 030228 respiratory system, Threshold dose distributions, Female, Immunization, Nut Hypersensitivity, business
Abstract

Background In food allergy, eliciting doses (EDs) of foods on a population level can improve risk management and labeling strategies for the food industry and regulatory authorities. Previously, data available for walnut were unsuitable to determine EDs. Objective The objective of this study was to determine EDs for walnut allergic adults and to compare with previously established threshold data for peanut and tree nuts. Methods Prospectively, adult subjects with a suspected walnut allergy underwent a low-dose double-blind, placebo-controlled food challenge. Individual no observed and lowest observed adverse effect levels were determined and log-normal, log-logistic, and Weibull models were fit to the data. Estimated ED values were calculated for the ED5, ED10, and ED50, the dose respectively predicted to provoke an allergic reaction in 5%, 10%, and 50% of the walnut allergic population. Results Fifty-seven subjects were challenged and 33 subjects were confirmed to be walnut allergic. Objective symptoms occurred in 20 of the positive challenges (61%). The cumulative EDs in the distribution models ranged from 3.1 to 4.1 mg for the ED05, from 10.6 to 14.6 mg walnut protein for the ED10, and from 590 to 625 mg of walnut protein for the ED50. Conclusions Our data indicate that population EDs for walnut are slightly higher compared with those for peanut and hazelnut allergy. Currently available data indicate that the ED values for hazelnut could be used as a conservative temporary placeholder when implementing risk management strategies for other tree nuts where little or no food challenge data are available.

Published
2017
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20. Using data from food challenges to inform management of consumers with food allergy: A systematic review with individual participant data meta-analysis

Author

Daniel C. Adelman, Joseph L. Baumert, W. Marty Blom, Ross A.R. Yarham, E. N. Clare Mills, R. Sharon Chinthrajah, Hugh A. Sampson, Bushra Javed, Nandinee Patel, Katherine Anagnostou, Paul Turner, Benjamin C. Remington, Alexander D. Smith, Natasha Purington, and Dianne E. Campbell

Subjects
medicine.medical_specialty, Allergen immunotherapy, Allergy, LOAEL, Lowest observed adverse effect level, Arachis, Immunology, Peanut allergy, Population, Administration, Oral, medicine.disease_cause, Food Allergy and Gastrointestinal Disease, DBPCFC, Double-blind placebo-controlled food challenge, Allergen, Recurrence, oral food challenge, Food allergy, Internal medicine, FC, Food challenge, medicine, Animals, Humans, Immunology and Allergy, Peanut Hypersensitivity, education, Anaphylaxis, education.field_of_study, ED, Eliciting dose, IPD, Individual participant data, Oral food challenge, business.industry, thresholds, Reproducibility of Results, peanut allergy, Allergens, PRACTALL, Practical Allergy, medicine.disease, Desensitization, Immunologic, Food, precautionary allergen labeling, ED01, Amount of allergen expected to cause objective symptoms in 1% of the population with that allergy, AIT, Allergen immunotherapy, ED05, Amount of allergen expected to cause objective symptoms in 5% of the population with that allergy, business, Eliciting dose, WAO, World Allergy Organization, Food Hypersensitivity
Abstract

Background Eliciting doses (EDs) (eg, ED01 or ED05 values, which are the amounts of allergen expected to cause objective symptoms in 1% and 5% of the population with an allergy, respectively) are increasingly being used to inform allergen labeling and clinical management. These values are generated from food challenge, but the frequency of anaphylaxis in response to these low levels of allergen exposure and their reproducibility are unknown. Objective Our aim was to determine (1) the rate of anaphylaxis in response to low-level peanut exposure and (2) the reproducibility of reaction thresholds (and anaphylaxis) at food challenge. Methods We conducted a systematic review and individual participant data meta-analysis of studies that reported at least 50 individuals with peanut allergy reacting to peanut at double-blind, placebo-controlled food challenge (DBPCFC) and were published between January 2010 and September 2020. Risk of bias was assessed by using National Institute for Clinical Excellence methodologic checklists. Results A total of 19 studies were included (covering a total of 3151 participants, 534 of whom subsequently underwent further peanut challenge). At individual participant data meta-analysis, 4.5% (95% CI, 1.9% to 10.1%) of individuals reacted to 5 mg or less of peanut protein with anaphylaxis (moderate heterogeneity [I2 = 57%]). Intraindividual thresholds varied by up to 3 logs, although this variation was limited to a half-log change in 71.2% (95% CI, 56.2% to 82.6%) of individuals. In all, 2.4% (95% CI, 1.1% to 5.0%) of patients initially tolerated 5 mg of peanut protein but then reacted to this dose at subsequent challenge (low heterogeneity [I2 = 16%]); none developed anaphylaxis. Conclusion Around 5% of individuals reacting to an ED01 or ED05 level of exposure to peanut might develop anaphylaxis in response to that dose. This equates to 1 and 6 anaphylaxis events per 2500 patients exposed to an ED01 or ED05 dose, respectively, in the broader population of individuals with peanut allergy., Graphical abstract

Published
2021
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21. Methods to determine the risk of unintended allergen presence related to the dispersion of allergenic food particles in food production areas

Author

Steven L. Taylor, W. Marty Blom, Marie Y. Meima, Joseph L. Baumert, Marie-Claude Robert, Niels B. Lucas Luijckx, Benjamin C. Remington, Brett Jeffery, and Geert F. Houben

Subjects
Test facility, business.industry, 010401 analytical chemistry, 04 agricultural and veterinary sciences, medicine.disease_cause, medicine.disease, 040401 food science, 01 natural sciences, 0104 chemical sciences, Toxicology, 0404 agricultural biotechnology, Allergen, Food particles, Allergic symptoms, Food allergy, medicine, Food processing, Environmental science, Particle, business, Dispersion (chemistry), Food Science, Biotechnology
Abstract

Allergenic food particles (typically ~0.5–5 mm) may unintentionally end up in food products during production and can pose a risk for the allergic consumer. A single particle can provoke allergic symptoms in an allergic consumer when the dose of allergenic protein exceeds minimal eliciting doses. However, there is a lack of fundamental knowledge and research regarding allergenic particle behavior in food production and the resulting probability of their unintended presence in food products. In this study, the behavior of various types of particles encompassing a range of sizes and shapes (i.e. mustard seeds, sesame seeds, hazelnut pieces, walnut pieces and decoration pearls) was observed under controlled laboratory conditions and in a food production test facility. The main behavioral endpoints studied were rebound height and distance from and distribution around the rebound point. We found that the most determining particle characteristic for behavior was particle shape (spherical vs. non-spherical). In the laboratory, spherical mustard seeds showed an average rebound height of at least 3-fold higher than the non-spherical shaped sesame seeds, walnut pieces and hazelnut pieces. The distance from the rebound point after dropping was also considerably larger for mustard seeds, i.e. regularly up to 150 cm, while the majority of sesame seeds, walnut pieces and hazelnut pieces showed a distance from the rebound point of up to 30 cm, 7 cm and 4 cm, respectively. Experimental results from the test facility were in line with the results of the experiments in the laboratory, and provided additional insights in particle behavior for specific factory characteristics such as a moving belt. The experiments led to a concept for the definition of risk zones around a particle application and handling point, and can ultimately support efficient design of a production line and area and the application of tailored risk management measures with the goal to limit allergenic particle cross contamination.

Published
2021
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22. A systematic comparison of food intake data of the United States and the Netherlands for food allergen risk assessment

Author

Geert F. Houben, Marie Y. Meima, Joost Westerhout, W. Marty Blom, Astrid G. Kruizinga, and Benjamin C. Remington

Subjects
Population, Toxicology, Risk Assessment, Food group, 03 medical and health sciences, 0404 agricultural biotechnology, Food allergy, Environmental health, medicine, Animals, Product (category theory), education, Risk management, Netherlands, 030304 developmental biology, 0303 health sciences, education.field_of_study, business.industry, digestive, oral, and skin physiology, Comparability, Feeding Behavior, 04 agricultural and veterinary sciences, General Medicine, Allergens, medicine.disease, 040401 food science, United States, Geography, Survey data collection, Risk assessment, business, Food Analysis, Food Hypersensitivity, Food Science
Abstract

National population-based food consumption surveys are used in food allergen risk assessment. It would be beneficial if food intake data is interchangeable between countries to bridge potential gaps present in national survey data, which is only possible when risk assessment outcomes for comparable food product groups between countries are fairly similar. Additionally, merged food intake data would enable risk assessments that cover scenarios for various countries, if based on the most critical situation. Therefore, we systematically compared risk assessment outcomes for a broad range of food groups based on United States and Dutch population food consumption survey data. We calculated risks for 14 allergenic foods for 9 concentrations (1-10,000 ppm) to assess comparability. Depending on the assumed allergen concentration, risk assessment outcomes for 20% (10 out of 49) food groups differed considerably. We consider the number of potentially relevant risk differences too high to conclude that food intake data from the US and The Netherlands can be used interchangeably. To allow risk assessments that cover scenarios for several countries, we recommend development and use of a food intake dataset based on the highest intake levels for each food group of the involved countries to facilitate risk management efforts and harmonization.

Published
2021
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23. Cofactors in allergic reactions to food: physical exercise and alcohol are the most important

Author

Harmieke van Os-Medendorp, Geert F. Houben, André C. Knulst, W. Marty Blom, Astrid Versluis, and Astrid G. Kruizinga

Subjects
0301 basic medicine, medicine.medical_specialty, Allergy, business.industry, Immunology, Alcohol, Physical exercise, medicine.disease, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, 030228 respiratory system, chemistry, Food allergy, Allergic symptoms, Internal medicine, Physical therapy, Immunology and Allergy, Medicine, Outpatient clinic, Limited evidence, business, Alcohol consumption
Abstract

Introduction Involvement of cofactors, like physical exercise, alcohol consumption and use of several types of medication, are associated with more severe food allergic symptoms. However, there is limited evidence on how often cofactors play a role in food allergic reactions. The study aimed to get more insight into the frequency of exposure to cofactors and how often cofactors are associated with more severe symptoms in food allergic patients. Methods A questionnaire was completed by patients visiting the Allergology outpatient clinic. Patients with food allergy were included. Outcome measures were the frequency of medication use of medication groups that might act as cofactor and the frequency that physical exercise, alcohol consumption and use of analgesics are associated with more severe food allergic symptoms. Results Four hundred ninety-six patients were included in the study. The frequency with which patients used one or more types of medication that might act as cofactors was 7.7%: antacids/acid neutralizing medication (5%), NSAIDs (2%), beta blockers (0.6%), angiotensin-converting enzyme inhibitors (0.6%), and angiotensin receptor blockers (0.2%). Of all patients, 13% reported more severe symptoms to food after involvement of one or more of the cofactors: physical exercise (10%), alcohol consumption (5%), and use of analgesics (0.6%). Sixty-five percent did not know if these cofactors caused more severe symptoms; 22% reported that these cofactors had no effect. Conclusions Only a small percentage of patients (7.7%) used medication that might aggravate food allergic reactions. Physical exercise and alcohol consumption were the most frequently reported cofactors, but occurring still in only 10% or less.

Published
2016
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24. Full range of population Eliciting Dose values for 14 priority allergenic foods and recommendations for use in risk characterization

Author

Joost Westerhout, Geert F. Houben, Steve L. Taylor, Benjamin C. Remington, Astrid G. Kruizinga, W. Marty Blom, Matthew W. Wheeler, Marie Y. Meima, and Joseph L. Baumert

Subjects
Population, Context (language use), Toxicology, medicine.disease_cause, Risk Assessment, Article, Allergen, Food allergy, Allergic symptoms, Environmental health, medicine, Humans, Food allergens, education, Risk management, No-Observed-Adverse-Effect Level, education.field_of_study, Dose-Response Relationship, Drug, business.industry, General Medicine, Allergens, medicine.disease, business, Risk assessment, Food Hypersensitivity, Food Science
Abstract

Previously, we published selected Eliciting Dose (ED) values (i.e. ED01 and ED05 values) for 14 allergenic foods, predicted to elicit objective allergic symptoms in 1% and 5%, respectively, of the allergic population (Remington et al., 2020). These ED01 and ED05 values were specifically presented and discussed in the context of establishing Reference Doses for allergen management and the calculation of Action Levels for Precautionary Allergen Labeling (PAL). In the current paper, we publish the full range of ED values for these allergenic foods and provide recommendations for their use, specifically in the context of characterizing risks of concentrations of (unintended) allergenic proteins in food products. The data provided in this publication give risk assessors access to full population ED distribution information for 14 priority allergenic foods, based on the largest threshold database worldwide. The ED distributions were established using broad international consensus regarding suitable datapoints and methods for establishing individual patient's NOAELs and LOAELs and state of the art statistical modelling. Access to these ED data enables risk assessors to use this information for state-of-the-art food allergen risk assessment. This paper contributes to a harmonization of food allergen risk assessment and risk management and PAL practices.

Published
2020
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25. Risk of shared equipment in restaurants for consumers with peanut allergy: a simulation for preparing Asian foods

Author

Boris Bassa, W. Marty Blom, Stef J. Koppelman, and Benjamin C. Remington

Subjects
Pulmonary and Respiratory Medicine, Relative risk reduction, education.field_of_study, business.industry, Threshold limit value, Immunology, Population, Peanut allergy, food and beverages, medicine.disease, Toxicology, 03 medical and health sciences, 0302 clinical medicine, 030228 respiratory system, Daily practice, Immunology and Allergy, Medicine, 030212 general & internal medicine, business, Risk assessment, education
Abstract

Background Allergic reactions to meals consumed outside the home are common and can be severe and sometimes fatal. Objective To quantify the risk reduction potentially achieved by increasing an individual’s threshold sensitivity to peanut (such as by means of immunotherapy) in scenarios of peanut exposure through shared kitchen materials in a restaurant setting. Methods Three versions of popular peanut-containing sauces were selected to represent common ingredients used in Asian cooking. Different combinations of utensils, equipment, sauces, and test conditions were prepared by a professional chef, with or without common cleaning procedures, to represent normal daily practice. Residue amounts of peanut-containing material on kitchen equipment and utensils were measured and used for quantitative risk assessment to model the risk reduction associated with increasing an individual’s threshold. Results Shared utensils had mean residue amounts of 23 to 1519 mg peanut protein (no cleaning) and 3 to 82 mg peanut protein (after water rinse). Shared woks and pans had up to 20 mg peanut protein after rinsing. Individuals who reach a threshold of 300 mg peanut protein have a predicted relative risk reduction of 94.9% to greater than 99.99% with brief cleaning. With no cleaning, relative risk reductions were 63.5% to 91.1% for individuals with a baseline threshold of less than or equal to 100 mg peanut protein who reach a threshold of 300 mg peanut protein, increasing to 91% to 99.7% when reaching a threshold value of 1000 mg peanut protein. Conclusion In all shared kitchen material scenarios that we studied, achieving an eliciting dose of 300 or 1000 mg peanut protein seems clinically relevant for the peanut-allergic population.

Published
2020
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26. Updated population minimal eliciting dose distributions for use in risk assessment of 14 priority food allergens

Author

Steve L. Taylor, Benjamin C. Remington, Marie Y. Meima, Joseph L. Baumert, Geert F. Houben, Astrid G. Kruizinga, Matthew W. Wheeler, W. Marty Blom, and Joost Westerhout

Subjects
Allergy, Arachis, Population, Juglans, Biology, Toxicology, medicine.disease_cause, Risk Assessment, Article, Sesamum, 03 medical and health sciences, 0404 agricultural biotechnology, Fish meal, Allergen, Food allergy, medicine, Animals, Humans, Nuts, education, 030304 developmental biology, 0303 health sciences, education.field_of_study, Oral food challenge, 04 agricultural and veterinary sciences, General Medicine, Allergens, medicine.disease, 040401 food science, Shrimp, Milk, Risk assessment, Food Hypersensitivity, Food Science
Abstract

Food allergy and allergen management are important global public health issues. In 2011, the first iteration of our allergen threshold database (ATDB) was established based on individual NOAELs and LOAELs from oral food challenge in roughly 1750 allergic individuals. Population minimal eliciting dose (EDp) distributions based on this dataset were published for 11 allergenic foods in 2014. Systematic data collection has continued (2011–2018) and the dataset now contains over 3400 data points. The current study provides new and updated EDp values for 14 allergenic foods and incorporates a newly developed Stacked Model Averaging statistical method for interval-censored data. ED01 and ED05 values, the doses at which 1%, and respectively 5%, of the respective allergic population would be predicted to experience any objective allergic reaction were determined. The 14 allergenic foods were cashew, celery, egg, fish, hazelnut, lupine, milk, mustard, peanut, sesame, shrimp (for crustacean shellfish), soy, walnut, and wheat. Updated ED01 estimates ranged between 0.03 mg for walnut protein and 26.2 mg for shrimp protein. ED05 estimates ranged between 0.4 mg for mustard protein and 280 mg for shrimp protein. The ED01 and ED05 values presented here are valuable in the risk assessment and subsequent risk management of allergenic foods. © 2020

Published
2020
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27. Defining the targets for the assessment of IgE-mediated allergenicity of new or modified food proteins

Author

Geert F. Houben, Anne Constable, Ricardo Assunção, Ben Remington, Charlotte Bernhard Madsen, Emilia Vassilopoulou, Paula Alvito, Thomas Stroheker, Christiane Kruse Fæste, Jana Žiarovská, Kitty C.M. Verhoeckx, Thuy My Le, W. Marty Blom, and René W.R. Crevel

Subjects
Risk, Immunoglobulin E/metabolism, Computer science, Decision Making, Population, RAPID - Risk Analysis for Products in Development, Assessment, Toxicology, Health outcomes, Risk Assessment, 03 medical and health sciences, 0404 agricultural biotechnology, Ige mediated, Life, Food allergy, Journal Article, medicine, Humans, education, Risk management, 030304 developmental biology, Nutrition, Risk Management, 0303 health sciences, education.field_of_study, ImpARAS, business.industry, Proteins, 04 agricultural and veterinary sciences, General Medicine, Allergens, Immunoglobulin E, medicine.disease, 040401 food science, Method development, Allergens/adverse effects, 3. Good health, Segurança Alimentar, Risk analysis (engineering), Food, Allergenicity, Dietary Proteins, Food Hypersensitivity/immunology, business, Risk assessment, Food Hypersensitivity, Dietary Proteins/adverse effects, Food Science
Abstract

Many food innovations rely on the introduction and use of new or modified proteins. New or modified food proteins may lead to major health risks due to their inherent potential to cause food allergy. Currently, the pre-market allergenicity assessment for new or modified food proteins and protein sources relies on methods for identifying allergenic hazards based on characteristics of known allergens. However, there is no general consensus on the allergenicity parameters to use and the criteria that should apply for the evaluation and decisions to be made. In this paper, we propose that the strategy for allergenicity risk assessment of new or modified food proteins and the methodologies applied should be governed by the risk management questions to be answered, reflected in the information needed by risk managers to enable their informed decision making. We generated an inventory of health outcome-related assessment parameters and criteria potentially important for risk management decision-making and we discuss the implications of selecting different optional criteria (e.g. cut-off values) for what could be accepted as safe with regards to the health outcomes in the (at risk) population. The impact of these various options on both method development and risk management practices was investigated. The work presented in this paper as well as the publication of it were part of and made possible by EU COST Action 1402 ImpARAS: Improving Allergy Risk Assessment Strategy for New Food Proteins (http://imparas.eu). Paula Alvito and Ricardo Assunção acknowledge the support from National Institute of Health, Dr. Ricardo Jorge and CESAM through the Fundação para a Ciência e a Tecnologia [UID/AMB/50017/2013], through national funds, and the co-funding by the FEDER [POCI-01- 0145-FEDER-00763], within the PT2020 Partnership info:eu-repo/semantics/publishedVersion

Published
2019

28. Sensitivity analysis to derive a food consumption point estimate for deterministic food allergy risk assessment

Author

Charlotte Bernhard Madsen, Joseph L. Baumert, Geert F. Houben, René W.R. Crevel, Stephen L Taylor, Benjamin C. Remington, Astrid G. Kruizinga, Amélie Crépet, W. Marty Blom, and Luca Bucchini

Subjects
Percentile, Databases, Factual, Population, Context (language use), Food Contamination, Toxicology, Risk Assessment, Food group, 03 medical and health sciences, 0404 agricultural biotechnology, Food allergy, Environmental health, Medicine, Humans, education, 030304 developmental biology, 0303 health sciences, Reference dose, education.field_of_study, Probabilistic risk assessment, business.industry, digestive, oral, and skin physiology, 04 agricultural and veterinary sciences, General Medicine, medicine.disease, 040401 food science, Food, business, Risk assessment, Food Hypersensitivity, Food Science
Abstract

One of the input parameters in food allergy risk assessment is the amount of a given food consumed at an eating occasion. There is no consensus on how to use food consumption data when assessing the risk from unintended allergen presence in food products. A sensitivity analysis was performed to establish the optimal food consumption estimate for a deterministic food allergy risk assessment. Exposure was calculated for consumption percentiles (50th percentile, P50 to maximum) using the iFAAM consumption database in conjunction with an allergen concentration range from 1 to 1000 ppm. The resulting allergen intakes were compared to the allergic population reference doses proposed by Taylor et al. (2014) for 10 major allergenic foods. Optimal consumption percentiles were defined as those which predicted an intake below the relevant reference dose and met the defined acceptable risk level confirmed by probabilistic risk assessments. Analysis showed that, for 99% of the food groups, the P50 consumption met our criteria, while the P75 did so for 100% of the food groups. We suggest that the P75 is the optimal point estimate for use in deterministic food allergy risk assessment. It meets the safety objective and is adequately conservative for a public health context.

Published
2018

29. Potential cofactors in accidental food allergic reactions are frequently present but may not influence severity and occurrence

Author

Geert F. Houben, Anouska D. Michelsen-Huisman, Jacqueline J.M. Castenmiller, Hubert P.J.M. Noteborn, André C. Knulst, W. Marty Blom, Harmieke van Os-Medendorp, and Astrid Versluis

Subjects
0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Alcohol Drinking, Population, Immunology, Physical exercise, Severity of Illness Index, Cofactor, 03 medical and health sciences, 0302 clinical medicine, Food allergy, Risk Factors, Internal medicine, medicine, Immunology and Allergy, Humans, Longitudinal Studies, Prospective Studies, Prospective cohort study, education, Exercise, Asthma, Aged, education.field_of_study, food allergy, exercise, biology, business.industry, alcohol, cofactor, Middle Aged, medicine.disease, 030104 developmental biology, 030228 respiratory system, Accidental, biology.protein, Population study, Female, accidental reaction, business, Food Hypersensitivity, Follow-Up Studies
Abstract

Background: Cofactors, such as physical exercise and alcohol intake, might be associated with the severity or occurrence of food allergic reactions. Objective: To gain insight into the frequency of presence of potential cofactors in accidental food allergic reactions in adults and to what extent these factors influence the severity and occurrence of allergic reactions. Methods: A prospective cohort study was conducted, with a 1-year follow-up in adult patients with a physician-diagnosed food allergy. Patients were required to fill in a questionnaire after every accidental allergic reactions to food over a 1-year period. The primary outcome measure was the frequency that potential cofactors were present in these allergic reactions. Results: A total of 157 patients were included, of which 46% reported a total of 153 reactions during a 1-year follow-up period. In 74% of the reactions, ≥1 potential cofactor was reported to be present: tiredness (38%), alcohol intake (16%), stress (14%), symptoms of pollinosis (16%), symptoms of asthma (9%), sickness/flu (3%), physical exercise (3%) and use of analgesics (2%). More than one potential cofactor was reported in almost half of all reactions (47%). There was no significant difference in the presence of these factors between mild, moderate and severe reactions (P = 0.522). In the total study population, 9% of the patients used medication that might act as cofactor (antacids, angiotensin receptor blockers [ARBs], beta blockers and angiotensin-converting enzyme inhibitors [ACEIs]) on a daily basis, which however did not influence the occurrence of reactions. Furthermore, 38% daily used allergy-suppressing medication. Conclusions: Although factors suggested to be cofactors were frequently present during accidental food allergic reactions, we found no evidence for an association between the potential cofactors examined and reaction severity, in a population where most reactions were of mild to moderate severity.

Published
2018

30. Abstracts from the Food Allergy and Anaphylaxis Meeting 2016

Author

Georgios Rentzos, Esben Eller, Annick Mercenier, Magna Correia, Pedro Moreira, Linda Verrill, Mário Morais-Almeida, Frauke Schocker, Carsten Bindslev-Jensen, Ulrike Lehnigk, Andreas Frey, Lars Verschuren, Anna-Lena Bramstång Björk, Lene Heise Garvey, Elena Molina, Katrine L. Bøgh, J. L. van der Velde, Montserrat Alvaro, Phil Padfield, Niamh Brosnan, Nelly Gourdon-Dubois, Christian Harwanegg, Manuel Branco Ferreira, Songül Yürek, Amyra Ali Azamar Jácome, Rashid Amin, José Ramón Fernández Lorenzo, Kirsten Beyer, Florin-Adrian Secureanu, Charlotte Bernhard Madsen, Julie Galand, Claudia Pföhler, Rabea Reinert, Heinz Fehrenbach, Anton Hartmann, Maria Salas, Arne Homann, Rand Arnaout, Sarah Lindsley, Nerea Sarmiento Carrera, Patrícia Padrão, Berber Vlieg-Boerstra, Alkerta Ibranji, Benoît Sterling, Maria Auxiliadora Guerrero, Maria L. Baeza, Maurizio Tamburrini, Eva Untersmayr, Tanja Cirkovic Velickovic, Farrukh Sheikh, Sarah Kuntz, Sara Martínez, Kriti Gupta, Maria de Lurdes Torre, Yvonne Vergouwe, Ross Yarham, Faisal R. Bakhsh, Marta Vazquez-Ortiz, João Marcelino, Tullio Frediani, Ricardo Prata, Anna Kaarina Kukkonen, Gustavo Soldateli, Ines Mrakovčić-Šutić, Elodie Drumez, Cristina Ornelas, Maria Vazquez de La Torre, Renata Barros, Agata Szymkiewicz, Aneta Tomaszewska, Stefanie Rohwer, Charlotte Eisenmann, Adriana Muntean, Matteo Moretti, Johanna P. M. van der Valk, Birgit Quinting, Stefan Kabasser, David Gillick, Michał Przybyszewski, Grzegorz Sergiejko, Antonio Jorge Cabral, Alba Pablos-Tanarro, Robert Elfont, Marit Reitsma, Roxana Silvia Bumbăcea, Nelson Rosario, Maria Livia Bernardi, Cristiane N. Santos, Christian Radauer, Sandra Denery-Papini, Geert F. Houben, Nicolette W. de Jong, Marta Anda, Alexander Rohrbach, Teodorikez Wilfox Jimenez-Rodriguez, María Teresa Villalba, Karine Patient, Harmieke van Os-Medendorp, Kathrin Scherer, Marta Goñi Esarte, Svetlan Dermendzhiev, Jossie Garthoff, Michelle M. Epstein, Catherine Bertholet, Bruna Pultrini Aquilante, Didier G. Ebo, Roberta Aina, Jorge Kalil, Petri Kulmala, Lars K. Poulsen, Barbara Ballmer, H. Mary-Lene de Zeeuw-Brouwer, Karin Hoffman-Sommergruber, Winfried Leeman, Anne Miles, Nehad Gomaa, Maria Teresa Costantino, Evelyne Mangodt, Maria Konstantakopoulou, Rosa Jimenez, Attilio Francesco Speciani, Helga Magnusdottir, Inmaculada Sánchez-Machín, H. Kaddouri, Raquel Perez, Astrid Versluis, Anthony E. J. Dubois, Anja Koren Jeverica, Zdenka Barićev-Novaković, Joost Westerhout, A.M. Plaza, Júlio Oliveira, Pierre Lukas, Oksana Matsyura, Giuseppe Pingitore, Mira Silar, Huub F. J. Savelkoul, Urszula Samolinska-Zawisza, Chantal Brossard, Ana Reis Ferreira, Reiko Teshima, Serena Perna, Mariola Dietrich, Dirk Verhoeven, Fiona Kenna, Paloma Poza-Guedes, Cristobalina Mayorga, Pilar Hernandez, Roberto Bernardini, Roberto Berni Canani, Maria Francesca Patria, Mariana Vieru, Julie Locklear, Esther van Twuijver, Marina A. Kiseleva, H. Kim A. Brand, Gabriele Schulz, Ileana-Maria Ghiordanescu, Nikolaos G. Papadopoulos, Danijela Apostolovic, Maria del Mar Folqué, Eva Lasa, Mohammad Al Bahkali, Arianna Dondi, Sofia Kostoudi, Simon Rosenberg, Véronique Nève, Rumyana Yankova, Barbara Ballmer-Weber, Maria Jose Goikoetxea, María José Barasona Villarejo, Teija Dunder, Tina Vesel, Elisa Gritti, Marianne van Hage, Laure Castan, Etienne Beaudouin, Margherita Di Costanzo, Natalia Ukleja-Sokołowska, Matthew Sperrin, Paul Turner, Saskia Albroscheit, Rebeca Lopez, Sonja Posega Devetak, Francisca Palomares, Laetitia Sellam, Jennifer Hammond, Astrid G. Kruizinga, Konrad Furmanczyk, Patricia Macchiaverni, Olga Pakholchuk, I V Vorozhko, Ania Carsin, Aleksandar Bulog, Joris Mens, Bianca Balbino, James P. Hindley, Jaap H. Akkerdaas, Jonathan Hourihane, Hilde Cnossen, Tatyana A Popova, Rupert Schlags, Natalia Nenasheva, A. Ehrenberg, Sigurveig T. Sigurdardottir, Anna Iliopoulou, Clara Ippolito, Piotr Samel-Kowalik, Paloma Campo, Gador Bogas, Constantinos Pitsios, Sarah Grosche, Karla Leversia Borjas Aguilar, Amena Warner, Birgit Kalb, Lénaïck Dupuis, Harry J. Wichers, Diana Silva, Gabriele Piuri, Linus Grabenhenrich, Emanuel Sarinho, M. Eleonore Pettersson, Rodrigo Barderas, Gary Stiefel, E. N. Clare Mills, Lali Saginadze, Ruta Dubakiene, Francesca Cipriani, Mindy Tsai, Marina Themisb, Michela Ciancamerla, Rebecca Knibb, Ruperto González-Pérez, Marina Peredelskaya, André C. Knulst, Irene Berends, S N Denisova, Montserrat Fernandez-Rivas, Paolo Maria Matricardi, Daniel Sampaio, Giorgio Bedogni, Sira Miquel, Koen Smit, Stefania Arasi, Sylvia Osscini, Justine Courtois, Cristina Deaconu, Srdan Banac, Kirsten Hansen, Jennette Higgs, Charlotte Hands Plovdiv, Carlotta Povesi Dascola, Noe Ontiveros, Rik Schrijvers, Carla Mastrorilli, Maria Passioti, Sebastian Tschirner, Bjorn R. Ludviksson, Joana Caiado, Daniel Corbacho, Sophie Nutten, Agustin Madroñero, Marina Suárez Vergara, Boudewjin J. Kollen, Catherine J Nock, Johanna Rost, Agnieszka Lipiec, Skadi Kull, Geert Houben, Carlo Caffarelli, Jordi Roca-Ferrer, Bolesław Samoliński, Isabelle Cleach, Colette Larré, Aideen Byrne, Corinne Herouet-Guicheney, Jonas Lidholm, Vera Assmann, W. Marty Blom, Adriano Mari, Adam T. Fox, Giuseppe Crisafulli, Afke M. M. Schins, Anastasia Papadopoulou, Flávio Sano, Richard Cooke, Franziska Ruëff, L Jorjoliani, Rebekah Sayers, Anne-Marie Kochuyt, Borja Bartalomé, Anne Moneret-Vautrin, Juan Carlos Julia, Jelena Mihailovic, Katarzyna Pyrz, Kollen Boudewijn, Margherita Varini, Paolo Giordani, Claudia Alessandri, Johanna van der Valk, Antoine Deschildre, Mariam Tskhakaia, Rosina López-Fandiño, Omar Kheroua, Nicolette J. T. Arends, Alina Zbróg, Chung-Hsiung Huang, Andrea Wangorsch, Ulf Bengtsson, Jim Langridge, Dasha Roa-Medellín, Jose Ignacio Larco, Bert Popping, Ana Prieto del Prado, José Antonio Bácter Martos, Rita Nocerino, Sophia Watts, Elisa Haroun, Danilo Villalta, Lee A. Gethings, María Ángeles Algaba Mármol, Ewa Gawrońska-Ukleja, Cornelia Jansen, André Moreira, V A Revyakina, Robert Zacniewski, Xavier Domingo Miró, Francesco Macrì, Mayra de Barros Dorna, Akanksha Sharma, Stephen J. Till, Ali Almontasheri, Chrystyna Kalicinsky, Robbert Sutorius, Akila Rekima, Mark A. Blankestijn, Nicolette Arends, Chiara Pistoletti, Merima Bublin, Manuel Pereira-Barbosa, Reyna Simon, Martin Karjalainen, Sam Mehr, Tushar Banerjee, Carmen Riggioni, Bertrand Evrard, Antonio Carlos Pastorino, Lidia Ilènko, Nikolaos Douladiris, Miguel Vieira, Erik Wambre, Francisco Cabrera-Chavez, Nikos G. Papadopoulos, Piotr Humeniuk, Gert van Duijn, Francesco Zinno, Young-Ae Lee, Lisa Tuppo, Hans de Groot, Léon M.J. Knippels, Pawel Dubiela, Henrik Fomsgaard Kjaer, Andrea Vereda, Djamel Saidi, Kok Loong Ue, Henk Van Loveren, Maria Jose Rodriguez, Marta Lomikovska, Elodie Michaud, Josefina Cernadas, Carmen Ponce, Marysia Recto, Frances Smith, Hassan Al-Dhekri, Shinobu Sakai, Thomas Eiwegger, Ana Rodolfo, Diego Peroni, Nikki Edelbroek, Waltraud Suer, Jenny van Odijk, Irena Nedelea, Borja Bartolomé, Lauren Lissner, Marjeta Sedmak, Annette Jamin, Italo De Vitis, Bo Pontoppidan, Annabelle Capt, Diego G. Peroni, Susana Rodrigues, Juan Carlos López-Rodríguez, David Endesfelder, Lesya Besh, Danila Zennaro, Charlotte G. Mortz, Kati Palosuo, María José Torres, Esozia Arroabarren, Lynne Regent, Laura Valdesoiro Navarrete, Ana Molina, Agha Rehan Khaliq, Phil Couch, Ana Miranda, Thomas Marichal, Riccardo Asero, Denise Borges, Dikla Pivko Levy, Miriam Palacios, Mireille Eb, Stephen J. Galli, Karin Hoffmann-Sommergruber, Anna Gudrun Vidarsdottir, Ifigenia Sfika, André Wolterbeek, Mauro Calvani, Edward F. Knol, Joyce A. M. Emons, Anne-Marie Oomkes-Pilon, Montserrat Bosque García, Daniel Lozano-Ojalvo, Filip Raciborski, Deirdre Galloway, Nanna Juel-Berg, Margareta Brandt Gertmo, Cornelia Bergmayr, Rob Klemans, Juliane Gregersen, Yolanda Meijer, Bettina Brix, Susanne Lau, Karine Adel-Patient, Hanneke van der Kleij, Mareike Price, Jean-Louis Mege, Lizalet Oosthuizen, Agurtzane Bilbao, Indre Butiene, Antonino Romano, Colin Barber, Rosana Camara Agondi, Nour Baïz, Soraya Ainad Tabet, Peter Korošec, Laurian Jongejan, Francine C. van Erp, José Pedro Moreira Silva, Nandinee Patel, Jaime Lozano, Prescilla V. Jeurink, Artur Walkiewicz, Bryan M. Harvey, Tiina J. Kauppila, Aida Semic-Jusufagic, Marianna Murdjeva, Miren Arteaga, Y. Bouferkas, Geunwoong Noh, Henny G. Otten, Sabine Dölle, Christopher Munro, O Dominguez, Gerard H. Koppelman, Leonieke N. van Veen, Vasti Iancu, Georg Mitterer, Patrizia Polverino de Laureto, Juliane Schulz, Ewa Ternesten Hasseus, Caroline Zimmermann, Ivona Barcievic-Jones, Shira Benor, Susanne Schwarz, Eun Ha Jang, Josefina Rodrigues Cernadas, Tadej Avcin, Joseph L. Baumert, Pernille Winther, Stéphane Leteurtre, Gabriela Canto, Louise J Michaelis, Jorge Alvarez, Gabriel Gastaminza, Michela Carola Speciani, Rute Gonçalves, Leire Dopazo, Evgen Benedik, Susanne C. Diesner, Luc S. De Clerck, A. Wesley Burks, Maurits S. van Maaren, Salvatore Tripodi, Philippe Aubert, Kamel Eddine El Mecherfi, Aline B. Sprikkelman, Ana Prieto, Margitta Worm, Edyta Krzych, Maja Krstic, Iride Dello Iacono, Melanie Cap, Alf Weimann, Maria Nassiri, Niels Röckendorf, Vladyslava Barzylovych, Marcia C. Mallozi, Pierre Bruhns, Jeanette Fisker Trandbohus, Ekaterini Papadopoulou, Vicente Albendiz, Timothy Watts, Uta Jappe, Javier Moreno, Maria Carmen Verga, Beatriz Secades Barbado, Carmen Di Scala, Roy Gerth van Wijk, Vladimir Mićović, Esther Barrionuevo, Giampaolo Ricci, Luisa Galindo, Ana Paula Beltran Moschione Castro, Oona Mustonen, Jia Yin, Lucia Caminiti, Jorge Esparza-Gordillo, N Adamia, Anna-Maija Hanni, Romy Gadisseur, Stefano Luccioli, Regina Treudler, Rosetta Ferrara, M. Guendouz, Jaakko Yrjänä, Philipp Starkl, Premendra D. Dwivedi, Javier Cuesta-Herranz, Johan Garssen, Ekaterini Goudouris, Sridevi Muralidharan, Kate Grimshaw, Carolina Sanchez Aranda, Ioana Maris, Manzoor Ahmed, Hajime Karasuyama, Stephanie Claus, Chantal Agabriel, Karen English, Dorien Van Ginkle, Eleonora Savi, Loredana Chini, Ine I. Decuyper, Sabine Schnadt, Valérie Trendelenburg, Jean-Luc Fauquert, Maurizio Mennini, Nikolaos Mikos, Ana Célia Costa, Steve L. Taylor, A. A. Schoemaker, Sara Abián, Margo M. Hagendorens, Andrea Di Rienzo Businco, Melina Makatsori, Eugénia Matos, Lucy Walker, Nikolaos A. Kitsioulis, David Alejandro Mendoza Hernández, Maria Starkhammar, Djordje Filipovic, Aine Adams, Mukul Das, Sonsoles Intente-Herrero, Natalia Blanca López, Marek L. Kowalski, Diana Deleanu, Bernard P. Mahon, Jean-Michel Wal, Lucia Decastelli, Mihaela Popescu, Aimee Lou Nano, Eva Batanero, Tong-Rong Jan, Yolanda Puente, Jacek Borowicz, Aimée Dorkenoo, J. Östling, Mashary Altamimi, Michel Neunlist, Zerrin Yalvaç, Sonia Ricò, Wentong Xue, Linda Cosenza, David C. A. Candy, Robert D. Voyksner, Montserrat De Prada, Abdulhadi Al-Qahtani, Sébastien Holvoet, Wolf-Meinhard Becker, Meropi D. Kontogianni, Bruno Pereira, F. Pineau, Eva Corbet, Kirsten Mehlig, Rosella De Poi, Jolanda H. M. van Bilsen, José Luís Plácido, Hans-Jørgen Malling, Chia-Chi Wang, Philip Couch, Kerrie Kirk, Agata Michalska, Sylke Rietz, Mariya Ivanovska, Victor Matheu-Delgado, Carl Hamsten, Francisca Gómez, Neusa Falbo Wandalsen, Mika J. Mäkelä, Tatyana Sentsova, Kristian Bravin, Philippe Delahaut, Hervé Bernard, Leonor Carneiro-Leão, Michele Miraglia del Giudice, Elena D. Kuvshinova, Jochen Behrends, Caroline Klingebiel, Meta Accetto, Claire Mills, Mariona Pascal, Miguel García Domínguez, Huan Rao, Carmen Saviana Ganea, Umberto Pelosi, Stefano Pattini, Bodo Niggemann, Annamaria Bianchi, Laura Martín-Pedraza, Anna Selby, Cristina Bueno, Stefan Vieths, Luis Felipe Ensina, Florin-Dan Popescu, Antonio Fernandez, Soren Wille, Erna Van Hoeyveld, Carina Kelleher, Athina L. Van Gasse, Anders Blom Jensen, Zorica Zivkovic, Moshe Ben-Shoshan, Sara Pereiro Fernández, Ronald van Ree, Antima Banerjee, Pablo Merida, Mandy Ziegert, Barbara Wróblewska, Morten Christensen, Gador Gomez, Pablo San Segundo-Acosta, Khaled Messaoudi, Anne-Sofie Ravn Ballegaard, Mikael Kuitunen, David Luyt, Vito Sabato, Nesrine Zaabat, Svitlana Zubchenko, Julien Labreuche, Elin Lustig, Katharina Blumchen, Guillaume Pouessel, Ana Fiandor, Stéphanie Lejeune, Paola Dignetti, Helen Brown, Anastasia Cirisano, Evangelia Kompoti, Anna Sokolova, Mercedes Escarrer Jaume, Shan Deng, Dirceu Solé, Chiara Fiamingo, Alessandro Travaglini, Nicolas Gaudenzio, Zbigniew Bartuzi, Antonia Rojas, Roberta Olcese, Nanju Alice Lee, Sandra Brandhoff, Lucien F. Harthoorn, Anna Maria Szyc, Andrea Costanzi, Sabine Pfeifer, Emiliano De Dominicis, Chiara Rafaiani, Yin-Hua Cheng, Elida Nikolla, Ignacio García Núñez, Diego Faggian, Lieve Coorevits, Ayelet Rimon, Erika Jensen-Jarolim, Jacqueline J.M. Castenmiller, Kristin Verbeke, Sean Bennett, Paraskevi Xepapadaki, Glauce Hiromi Yonamine, Anna Wawrzeńczyk, Rusudan Karseladze, Emmanouil Manousakis, Fiona Ward, Ivana Filipovic, Marie Bodinier, Viviana Moschese, Pedro Giavina Bianchi, Alice Coimbra, Alena Berger, Anton A. Shekhetov, Monica Maćków, Philippe Egenmann, Oscar Asensio, Lidia Hanna Markiewicz, Chun-Wei Tung, Zsolt Szépfalusi, Jan Knol, Frits Koning, Carolina S. Aranda, Annick Bastiaensen, Giovanni Battista Pajno, Leticia Pérez-Rodríguez, Ewout W. Steyerberg, Riccardo Sibilano, Valérie Verhasselt, Roberta Lupi, Lukasz Sokolowski, Adam Wawrzeńczyk, Dimitris I. Mitsias, Andreia Forno, Antoine Magnan, Christian Schwager, Ioanna Manolaraki, Alessandro Fiocchi, Tanja Rouhani Rankouhi, Carla Jones, Ana Pereira, Hannah M. Kansen, Michael Clausen, D. Bignardi, Assad M. Butt, Julie C. Locklear, Katrine Lindholm Bøgh, Valery Muhortnich, María Teresa Giner, Juan Miguel Garcia, Maria Luisa Somoza, Raditsa Sokolova, Maria Pasioti, Mirjana Zupancic, Joana Vitte, Duncan Brown, Arnaldo Porto, M. Turfkruyer, Lau Fabricius Larsen, Filipe Benito-Garcia, Mayra Coutinho Andrade, Meltem Ugras, Ingrid Sutic, Rand K. Arnaout, Etienne Cavalier, Marta Neto, Grégory Bouchaud, Elena Varin, Bushra Javed, Carla Camerotto, Monica Bronkowska, Cristiano Caruso, Luís Amaral, Jackeline F. Motta, Sahar Elshorbagi, Cornelis K. van der Ent, Alexandra Rodrigues, Silvia Peveri, Juan Heber Castellanos, Muriel Totis, Joan Bartra, Gjustina Loloci, Ivana Giangrieco, Ekaterina Khaleva, Joaquín Navarro, Kayoko Matsunaga, Jlenia Fresta, Jonathan O'b Hourihane, Sabina Bijlsma, Ana Rodriguez-Fernandez, Rosita Aitoro, Daniela Manila Bianchi, Rosa Jimenez-Feijoo, Mario Plebani, Marleen T. J. Van Ampting, Anthony E.J. Dubois, Clémence Mordacq, Simone Frediani, Martin Chapman, Helena Larramona, Fabrícia Carolino, Yanne Boloh, Ivona Baricevic-Jones, Mathilde Claude, Caroline Thumerelle, Päivi Vähäsarja, Mareen R. Datema, Abdullah Alfhaid, Diana Perez Alzate, Laura Santos-Diez, Graham King, Maria Teresa Guerra Perez, Jean-Marie Renaudin, Frieke Kuper, Josué Alejandro Huertas Guzmán, Harry Wichers, Thomas Keil, A. Haddi, Jennifer Santos, Regina Selb, Aida del Campo García, Maria Basagaña, Valentino Pavišić, Angela Simpson, Chris H. Bridts, Susana Piedade, Silvia Gallina, Isabella Pali-Schöll, Inês Pádua, Margaretha A. Faber, Frédéric de Blay, Luís Câmara Pestana, Ben Remington, Anna S. Pelkonen, Sandra Lucarelli, Ivana Šutić, Olivier Tranquet, Montserrat López Onieva, Antonio Amoroso, Paola Minale, Katia Basello, George Du Toit, Daniela Adriano, Adnan Custovic, Zbikowska-Gotz M, Domingo Barber, Inmaculada Doña, Christine Breynaert, Hanan Sharif, Manon M. Oude Nijhuis, Sandra Denery, Bertine M. J. Flokstra-de Blok, Rinkesh Kumar Gupta, Pieter-Jan de Kam, Dianne E. Campbell, Carmen M. D'Amelio, Nunzia Maiello, Ingo Marenholz, José María Ignacio García, Helen Lindqvist, Lilian Moraes, Cleonir Lui de Moraes Beck, Eunice Dias de Castro, Cono Casale, Barbara Majkowska-Wojciechowska, Maria Petrodimopoulou, Andrea Mikkelsen, Hub P. J. M. Noteborn, Hulya Ercan Saricoban, Moira Austin, Martinus Løvik, Graham Roberts, Isabella Annesi-Maesano, Aeilko H. Zwinderman, Sigrun H. Lund, Anouska D. Michelsen-Huisman, Fernando Bandrés Sánchez-Cruz, Francisco Javier Ruano, Valérie Liabeuf, Eman Madbouly, Pasquale Comberiati, Maria Isabel Garcimartin, Stephan Scheurer, Inna A. Larkova, Jean Tratt, Renata Rodrigues Cocco, Younes Belabbas, Lorella Paparo, Elizabeth Griffiths, Gian Lodovico Rapaccini, Audrey Dunn Galvin, Zizi Cojocariu, Isidor Hutteger, Claire Claverie, S.M. Nedelska, Anna Kuklinska-Pijanka, Jenny Badas, Mónica Piquer, Iztok Devetak, A.K.F. Gushken, Frans Timmermans, Adriana Machinena, Francisco Javier Monteseirin, Amaranta Traversa, Fátima Cabral Duarte, Tomaž Poredoš, Peter Meyer, Cristina Arêde, Rosa Muñoz-Cano, Barbara Pfitzner, Alejandro Joral, Juan Carlos Daza, Laurent L. Reber, Olga Chernyak, and Maria Antonetta Ciardiello

Subjects
Pulmonary and Respiratory Medicine, Allergy, medicine.medical_specialty, 030504 nursing, business.industry, Immunology, RC581-607, medicine.disease, Meeting Abstracts, 03 medical and health sciences, 0302 clinical medicine, Food allergy, 030225 pediatrics, Family medicine, medicine, Immunology and Allergy, Immunologic diseases. Allergy, 0305 other medical science, business, Anaphylaxis
Published
2017
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31. Sensitization to Cor a 9 or Cor a 14 has a strong impact on the distribution of thresholds to hazelnut

Author

W. Marty Blom, Suzanne G.M.A. Pasmans, Rob J.B. Klemans, Carina M. Rubingh, Ben Remington, Geert F. Houben, Carla A.F.M. Bruijnzeel-Koomen, Els van Hoffen, André C. Knulst, L. J. Masthoff, Yolanda Meyer, and Dermatology

Subjects
Adult, Male, Young Adult, 03 medical and health sciences, Corylus, Sex Factors, 0302 clinical medicine, 030225 pediatrics, Statistics, medicine, Humans, Immunology and Allergy, Distribution (pharmacology), Child, Sensitization, Netherlands, Plant Proteins, Skin Tests, No-Observed-Adverse-Effect Level, business.industry, Age Factors, Allergens, Antigens, Plant, Immunoglobulin E, medicine.anatomical_structure, 030228 respiratory system, Child, Preschool, Female, Immunization, Nut Hypersensitivity, business
Published
2018
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32. Risk assessment of peanut protein traces found in refined peanut oil

Author

Geert F. Houben, René W.R. Crevel, Astrid G. Kruizinga, and W. Marty Blom

Subjects
Pulmonary and Respiratory Medicine, Reference dose, education.field_of_study, business.industry, Refined peanut oil, Immunology, Peanut allergy, Population, food and beverages, medicine.disease, Consumer safety, Ice cream, Labelling, Oral Presentation, Immunology and Allergy, Medicine, Food science, business, Risk assessment, education
Abstract

Highly refined peanut oil is considered to pose a risk to people with peanut allergy.[1] Although that risk has not been characterised, but controlled clinical challenges suggest it is negligible. A consequence is that the risk from cross contact between other refined vegetable oils and refined peanut oil during production must be assessed in order to assure consumer safety. Use of these refined vegetable oils in consumer food products potentially leads to very small amounts of peanut proteins in the final product. However, it is not clear yet if these amounts could reach levels that are relevant for public health. Allergen risk assessment using probabilistic techniques enables quantitative estimation of the risk after the consumption of a product that unintendedly contains an allergen. Several scenarios were defined for the unintended allergen levels in food products based on the estimated production scale of refined peanut oil in the UK, estimated figures for cross-contact and the peanut protein concentration in refined peanut oil. The consumption of 12 food products, selected for their high contribution to fat consumption including biscuits, margarine, ice cream and fried food, was combined with the peanut dose distribution. Food consumption data were derived from the National Diet and Nutrition Survey in the UK, and the Dutch National Food Consumption Survey. Peanut dosedistribution data were the same as used for the scientific review of VITAL® (Voluntary Incidental Trace Allergen Labelling).[2] We estimated that the amounts and distributions of peanut proteins posed a risk of objective allergic reactions in 0.03 to 0.6% of the peanut-allergic consumer population. The concentrations of peanut protein in selected food products would be below the limit of detection of current analytical methods and in all the scenarios examined, which included worst-case, the amounts consumed were below the VITAL reference dose for peanut. On that basis, the health risk is very small and none of those products would warrant precautionary labelling.

Published
2015
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33. Regional Loss of the Mitochondrial Membrane Potential in the Hepatocyte Is Rapidly Followed by Externalization of Phosphatidylserines at That Specific Site during Apoptosis

Author

W. Marty Blom, Hans de Bont, and J. Fred Nagelkerke

Subjects
Apoptosis, Phosphatidylserines, Cycloheximide, Mitochondrion, Biology, Biochemistry, Membrane Potentials, chemistry.chemical_compound, Adenosine Triphosphate, medicine, Animals, Rats, Wistar, Molecular Biology, Protein Synthesis Inhibitors, Membrane potential, chemistry.chemical_classification, Microscopy, Confocal, Microscopy, Video, ATP synthase, Intracellular Membranes, Cell Biology, Rotenone, Molecular biology, Mitochondria, Rats, Killer Cells, Natural, medicine.anatomical_structure, Enzyme, chemistry, Hepatocyte, Hepatocytes, biology.protein
Abstract

The spatio-temporal relationship between a decrease in the mitochondrial membrane potential (MMP) and externalization of phosphatidylserines (PS) during induction of apoptosis was investigated in single freshly isolated hepatocytes. Apoptosis was induced in the hepatocytes in three different ways: attack by activated Natural Killer cells, exposure to ATP, or exposure to the inhibitor of protein synthesis cycloheximide. Fluorescence microscopy showed staining of externalized PS at those areas where the staining for MMP was lost whereas in other areas the mitochondria remained intact for longer periods of time, indicating coupling between local loss of MMP and local PS exposure. To discriminate whether the decrease in MMP itself or a decrease in ATP induced PS externalization, hepatocytes were treated with rotenone, which resulted in a rapid collapse of cellular ATP but left the MMP intact for a much longer period. Addition of fructose prevented the decrease of ATP to approximately 30% and also delayed the collapse of the MMP. This indicates that ATP was needed for the maintenance of the MMP probably via reverse action of the ATP synthase. In a subsequent study hepatocytes were incubated with Natural Killer cells for induction of apoptosis followed by addition of rotenone to deplete ATP. Under these conditions the PS staining co-localized with mitochondrial MMP indicating that PS externalization does not require a collapse in MMP. Moreover, exposure of PS was evenly distributed over the whole plasma membrane. In conclusion, we propose that after an apoptotic stimulus some mitochondria start to loose their MMP, which results in cessation of ATP production and perhaps even consumption of ATP. This results in an overall decrease in cellular ATP. ATP-consuming enzyme reactions most distal from still intact mitochondria will be most sensitive to such a decrease. Apparently the translocase that keeps phosphatidylserines inward-oriented is such a sensitive enzyme.

Published
2003
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34. Specific IgE to Jug r 1 has no additional value compared with extract-based testing in diagnosing walnut allergy in adults

Author

W. Marty Blom, Mark A. Blankestijn, Joseph L. Baumert, Rob J.B. Klemans, André C. Knulst, Henny G. Otten, Carla A.F.M. Bruijnzeel-Koomen, Steve L. Taylor, and Geert F. Houben

Subjects
Allergy, biology, business.industry, Immunology, Immunoglobulin E, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, 030228 respiratory system, biology.protein, medicine, Immunology and Allergy, 030212 general & internal medicine, business, Value (mathematics)
Published
2017
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35. Remodeling of the actin cytoskeleton of target hepatocytes and NK cells during induction of apoptosis

Author

J. Fred Nagelkerke, Irma Meijerman, Hans de Bont, Hans van der Meulen, W. Marty Blom, Gerard J. Mulder, and Peter J. K. Kuppen

Subjects
Male, Cell, Arp2/3 complex, Apoptosis, Major histocompatibility complex, Immune system, Structural Biology, Tumor Cells, Cultured, medicine, Animals, Humans, Rats, Wistar, Killer Cells, Lymphokine-Activated, Cytoskeleton, Actin, biology, Dendrites, Cell Biology, Actin cytoskeleton, Actins, Coculture Techniques, Rats, Cell biology, medicine.anatomical_structure, Hepatocytes, biology.protein, Interleukin-2, Calcium
Abstract

Natural Killer cells are immune cells that recognize and eliminate altered and non-self cells from the circulation. To study the interaction between NK cells and target cells, we set up an experimental system consisting of rat Interleukin-2 activated Natural Killer cells (A-NK cells) and rat hepatocytes with a masked Major Histocompatibility Complex (MHC). The masking of the MHC induces recognition of the hepatocytes by the NK cells as non-self. We showed that in vitro apoptosis is rapidly induced in the hepatocytes [Blom et al., 1999] after co-incubation with A-NK cells. Now we describe the morphological changes that occur during and after interaction of A-NK cells with hepatocytes. Confocal laser scanning microscopy showed that the actin cytoskeleton of the NK cells was remodeled during attack of hepatocytes. Some NK cells were in close contact with the hepatocytes while others had formed actin-containing dendrites of varying length that made contact with the hepatocytes. However, dendrite formation is not obligatory for induction of apoptosis because cells that were unable to form these did induce FAS-dependent apoptosis in hepatocytes. Apparently both direct as well as distant contact resulted in apoptosis. Formation of the dendrites was calcium-dependent as EGTA largely prevented it. Importantly, chelation of the calcium also suppressed killing of the hepatocytes. Within 1 h after addition of the A-NK cells, morphological changes in hepatocytes that are characteristic of apoptosis, such as the formation of apoptotic bodies and fragmented nuclei, became apparent. Specifically, the actin cytoskeleton of the hepatocytes was remodeled resulting in the formation of the apoptotic bodies. Inhibition of caspase activity by z-Val-Ala-DL-Asp-fluoromethylketone (100 μM) partly protected against the rearrangement of the actin filaments in the hepatocytes. Cell Motil. Cytoskeleton 49:78–92, 2001. © 2001 Wiley-Liss, Inc.

Published
2001
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36. Prevention of cycloheximide-induced apoptosis in hepatocytes by adenosine and by caspase inhibitors

Author

W. Marty Blom, Hans de Bont, Irma Meijerman, J. Fred Nagelkerke, and Gerard J. Mulder

Subjects
Male, Adenosine, Liver cytology, Apoptosis, Mitochondria, Liver, In Vitro Techniques, Cycloheximide, Mitochondrion, Protective Agents, Adenosine receptor antagonist, Biochemistry, Membrane Potentials, chemistry.chemical_compound, medicine, Animals, Drug Interactions, Enzyme Inhibitors, Rats, Wistar, Fragmentation (cell biology), Caspase, Protein Synthesis Inhibitors, Pharmacology, biology, Caspase Inhibitors, Molecular biology, Rats, Liver, chemistry, biology.protein, medicine.drug
Abstract

The mechanism by which cycloheximide induces apoptosis in isolated rat hepatocytes was studied. Cycloheximide (1-300 microM) induced apoptosis within 3-4 hr in the hepatocytes. Specific apoptotic characteristics such as blebbing, phosphatidyl serine (PS) exposure, chromatin condensation, and nuclear fragmentation were induced. Cycloheximide (CHX) dose dependently activated the caspase-3-like proteases, but not the caspase-1-like proteases. Pretreatment of the hepatocytes with 100 microM of the caspase inhibitors z-Val-Ala-DL-Asp-fluoromethylketone or Ac-Asp-Glu-Val-Asp-aldehyde completely abrogated the caspase activation and the apoptosis. Addition of adenosine (100 microM) reduced phosphatidyl serine exposure and other morphological characteristics of apoptosis by 50%; however, it did not prevent the activation of the caspases, suggesting that adenosine inhibited downstream of caspase activation. The adenosine receptor antagonist 8-[4-[[[[(2-aminoethyl)amino]-carbonyl]methyl]oxy]phenyl]-1,3-dipropylxa nthine abolished the capacity of adenosine to prevent apoptosis, indicating that prevention was receptor-mediated. During apoptosis, the mitochondrial membrane potential in apoptotic cells (cells with PS exposition) was decreased to 50-60% of the control value; in the population viable cells, however, the mitochondrial membrane potential remained stable. Prevention of apoptosis by the caspase inhibitor z-Val-Ala-DL-Asp-fluoromethylketone or adenosine prevented the decrease in mitochondrial membrane potential. In conclusion, CHX rapidly induces apoptosis in isolated rat hepatocytes, which is inhibited by adenosine at a relatively late step.

Published
1999
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37. Interleukin-2-activated natural killer cells can induce both apoptosis and necrosis in rat hepatocytes

Author

Gerard J. Mulder, Peter J. K. Kuppen, W. Marty Blom, Irma Meijerman, J. Fred Nagelkerke, and Hans de Bont

Subjects
Male, Programmed cell death, Necrosis, Apoptosis, Mitochondria, Liver, Biology, Membrane Potentials, Natural killer cell, medicine, Animals, Cytotoxic T cell, Rats, Wistar, Fragmentation (cell biology), Cells, Cultured, Hepatology, Intracellular Membranes, Natural killer T cell, Rats, Cell biology, Killer Cells, Natural, medicine.anatomical_structure, Liver, Biochemistry, Caspases, Interleukin 12, Interleukin-2, medicine.symptom
Abstract

Natural killer (NK) cells play a crucial role in the elimination of virus-infected or transformed cells in the liver. In this article, we describe the mechanism by which liver cells are killed by NK cells. Interleukin-2-activated natural killer (A-NK) cells from the rat induced apoptotic cell death in 30% of freshly isolated rat hepatocytes within 60 minutes. Recognition by the A-NK cells of the hepatocytes as nonself was established by masking the major histocompatibility complex (MHC) class I molecules on the hepatocytes with the OX18 antibody. During the killing process, a decrease of the mitochondrial membrane potential (MMP), formation of blebs, phosphatidyl serine (PS) externalization, chromatin condensation, and nuclear fragmentation were observed. The hepatocytes became apoptotic before permeabilization of the plasma membrane occurred, suggesting that the observed cytolysis was caused by secondary necrosis. The apoptotic process was completely abolished by the caspase inhibitors, Z-Val-Ala-DL-Asp fluormethylketone (zVAD-fmk) and Ac-Asp-Glu-Val-aldehyde (DEVD-cho). However, under these conditions, A-NK cells killed a smaller fraction of the hepatocytes by (primary) necrosis. These results indicate that apoptosis is the major cytotoxic process induced by A-NK cells in hepatocytes. If apoptosis is prevented, a more limited necrotic effect is induced. Therefore, this study shows that NK cells are fully equipped to induce both apoptosis and necrosis in hepatocytes, but appear to prefer the apoptotic route.

Published
1999
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38. New Developments in Food Safety Assessment: Innovations in Food Allergy and Toxicological Safety Assessment

Author

Geert F. Houben, Lisette Krul, W. Marty Blom, and J. van Bilsen

Subjects
business.industry, digestive, oral, and skin physiology, Novel food, Food safety, medicine.disease, Biotechnology, Risk analysis (engineering), Food allergy, Medicine, White Spots, Food risk, Genetically modify, business, Risk assessment, Risk management
Abstract

Food preferably has to be tasteful, healthy, attractive, and affordable, but should above all be safe. The safety of our daily food nowadays is at a reasonable level, but is far from obvious. During the past half century, food risk assessment and risk management approaches have developed. Yet, several white spots or areas of inefficiency still exist. In this chapter, recent and ongoing innovations in two areas are addressed: innovations in food allergy safety assessment and innovations in toxicological safety assessment of food. Regarding food allergy safety assessment, the development of risk assessment-based guidance on precautionary labeling is addressed as well as strategies for assessment of the allergenicity of novel food proteins, either from genetically modified (GM) or non-GM origin. Regarding the toxicological safety assessment of food, an innovative new toxicological safety assessment approach for complex food matrices based on the Threshold of Toxicological Concern concept is presented and discussed.

Published
2014
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39. Food allergy population thresholds: an evaluation of the number of oral food challenges and dosing schemes on the accuracy of threshold dose distribution modeling

Author

Carina M. Rubingh, Joseph L. Baumert, Rinke Klein Entink, Geert F. Houben, Astrid G. Kruizinga, W. Marty Blom, Benjamin C. Remington, and Steve L. Taylor

Subjects
Arachis, Population, Dose-Response Relationship, Immunologic, Limited availability, Toxicology, Models, Biological, Risk Assessment, Food allergy, Statistics, Medicine, Distribution (pharmacology), Humans, Dosing, education, education.field_of_study, No-Observed-Adverse-Effect Level, business.industry, Statistical model, General Medicine, Allergens, medicine.disease, Threshold dose, Sample size determination, business, Algorithms, Food Hypersensitivity, Food Science
Abstract

For most allergenic foods, limited availability of threshold dose information within the population restricts the advice on action levels of unintended allergenic foods which should trigger advisory labeling on packaged foods.The objective of this paper is to provide guidance for selecting an optimal sample size for threshold dosing studies for major allergenic foods and to identify factors influencing the accuracy of estimation. A simulation study was performed to evaluate the effects of sample size and dosing schemes on the accuracy of the threshold distribution curve. The relationships between sample size, dosing scheme and the employed statistical distribution on the one hand and accuracy of estimation on the other hand were obtained. It showed that the largest relative gains in accuracy are obtained when sample size increases from N= 20 to N= 60. Moreover, it showed that the EuroPrevall dosing scheme is a useful start, but that it may need revision for a specific allergen as more data become available, because a proper allocation of the dosing steps is important.The results may guide risk assessors in minimum sample sizes for new studies and in the allocation of proper dosing schemes for allergens in provocation studies. © 2014 Elsevier Ltd.

Published
2013

40. Double-blind placebo-controlled food challenges in children with alleged cow’s milk allergy: prevention of unnecessary elimination diets and determination of eliciting doses

Author

Geert F. Houben, W. Marty Blom, Esther de Vries, Wendy M Dambacher, and Ellen H M de Kort

Subjects
Male, Pediatrics, medicine.medical_specialty, Provocation test, Medicine (miscellaneous), Milk allergy, Clinical nutrition, Placebo, medicine.disease_cause, law.invention, Allergen, Double-Blind Method, Randomized controlled trial, law, Cow's milk allergy, medicine, Animals, Humans, Feeding disorder, Prospective Studies, Child, Nutrition and Dietetics, business.industry, Research, Infant, Allergens, medicine.disease, Diet, Milk, Cow’s milk allergy, Child, Preschool, Cow’s milk protein, Immunology, Minimum eliciting dose, Female, Milk Hypersensitivity, business, Double-blind placebo-controlled provocation
Abstract

Background Children with cow’s milk allergy (CMA) need a cow’s milk protein (CMP) free diet to prevent allergic reactions. For this, reliable allergy-information on the label of food products is essential to avoid products containing the allergen. On the other hand, both overzealous labeling and misdiagnosis that result in unnecessary elimination diets, can lead to potentially hazardous health situations. Our objective was to evaluate if excluding CMA by double-blind placebo-controlled food challenge (DBPCFC) prevents unnecessary elimination diets in the long term. Secondly, to determine the minimum eliciting dose (MED) for an acute allergic reaction to CMP in DBPCFC positive children. Methods All children with suspected CMA under our care (Oct’05 - Jun’09) were prospectively enrolled in a DBPCFC. Placebo and verum feedings were administered on two randomly assigned separate days. The MED was determined by noting the ‘lowest observed adverse effect level’ (LOAEL) in DBPCFC-positive children. Based on the outcomes of the DBPCFC a dietary advice was given. Parents were contacted by phone several months later about the diet of their child. Results 116 children were available for analysis. In 76 children CMA was rejected. In 60 of them CMP was successfully reintroduced, in 2 the parents refused introduction, in another 3 the parents stopped reintroduction. In 9 children CMA symptoms reappeared. In 40 children CMA was confirmed. Infants aged ≤ 12 months in our study group have a higher cumulative distribution of MED than older children. Conclusions Excluding CMA by DBPCFC successfully stopped unnecessary elimination diets in the long term in most children. The MEDs form potential useful information for offering dietary advice to patients and their caretakers.

Published
2013
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41. Threshold dose distributions for 5 major allergenic foods in children

Author

Astrid G. Kruizinga, W. Marty Blom, Sicco van der Heide, Berber Vlieg-Boerstra, Geert F. Houben, Anthony E.J. Dubois, and Groningen Research Institute for Asthma and COPD (GRIAC)

Subjects
Male, Allergy, CLINICAL REACTIVITY, No-observed-adverse-effect level, Adolescent, Arachis, Eggs, Immunology, Population, threshold dose distributions, medicine.disease_cause, PEANUT, Toxicology, DOUBLE-BLIND, Allergen, Corylus, children, Food allergy, CASHEW NUT ALLERGY, COWS MILK ALLERGY, medicine, eliciting dose, Immunology and Allergy, Animals, Humans, Nuts, ANAPHYLACTIC REACTIONS, Food science, education, Child, Asthma, Retrospective Studies, education.field_of_study, CHALLENGES, business.industry, NATURAL-HISTORY, Allergens, medicine.disease, Confidence interval, Soy allergy, Milk, Food, Child, Preschool, Female, RISK-ASSESSMENT, business, Food Hypersensitivity, Allergenic foods, SOY ALLERGY
Abstract

Background: For most allergenic foods, insufficient threshold dose information within the population restricts the advice on levels of unintended allergenic foods which should trigger precautionary labeling on prepackaged foods.Objective: We wanted to derive threshold dose distributions for major allergenic foods and to elaborate the protein doses at which a proportion of the allergic population is likely to respond.Methods: For 7 allergenic foods double-blind, placebo-controlled food challenges (DBPCFCs) with a positive outcome for allergic reactions were selected from the clinical database of children routinely tested to diagnose food allergy at the University Medical Center Groningen. For each allergen 2 population threshold distributions were determined with the individual minimal eliciting dose and the preceding dose of each DBPCFC for objective symptoms and any symptom (either subjective or objective).Results: Individual positive DBPCFCs were available for peanut (n = 135), cow's milk (n = 93), hen's egg (n = 53), hazelnut (n = 28), and cashew nut (n = 31). Fewer children were challenged with soy (n = 10) or walnut (n = 13). Threshold dose distributions showed a good statistical and visual fit. The protein dose at which 5% of the allergic population is likely to respond with objective reactions was 1.6 mg for peanut, 1.1 mg for cow's milk, 1.5 mg for hen's egg, 7.4 mg for cashew nut, and 0.29 mg for hazelnut. Thresholds for any symptom were on average 2 to 6 times lower than for objective symptoms. The 95% upper and lower confidence intervals of the threshold distributions were overlapping. The peanut threshold distribution on objective symptoms was similar to the distribution of another European center.Conclusions: Threshold distribution curves and eliciting doses are a powerful tool to compare different allergenic foods and for informing policy on precautionary labeling. (J Allergy Clin Immunol 2013;131:172-9.)

Published
2013

42. Summer ammonia measurements in a densely populated Mediterranean city

Author

Andrés Alastuey, René Otjes, Fulvio Amato, Marco Pandolfi, W. Marty Blom, Cristina Reche, and Xavier Querol

Subjects
Mediterranean climate, Atmospheric Science, Meteorology, Earth & Environment, CAS - Climate, Air and Sustainability, Environment Climate, Particulates, Atmospheric sciences, lcsh:QC1-999, lcsh:Chemistry, Ammonia, chemistry.chemical_compound, Urban Development, chemistry, Nitrate, lcsh:QD1-999, Urban background, Environmental science, Ammonium, Built Environment, EELS - Earth, Environmental and Life Sciences, Sulfate, Road traffic, lcsh:Physics
Abstract

Real-time measurements of ambient concentrations of gas-phase ammonia (NH3) were performed in Barcelona (NE Spain) in summer between May and September 2011. Two measurement sites were selected: one in an urban background traffic-influenced area (UB) and the other in the historical city centre (CC). Levels of NH3 were higher at CC (5.6 ± 2.1 μg m−3 or 7.5 ± 2.8 ppbv) compared with UB (2.2 ± 1.0 μg m−3 or 2.9 ± 1.3 ppbv). This difference is attributed to the contribution from non-traffic sources such as waste containers, sewage systems, humans and open markets more dense in the densely populated historical city centre. Under high temperatures in summer these sources had the potential to increase the ambient levels of NH3 well above the urban-background-traffic-influenced UB measurement station. Measurements were used to assess major local emissions, sinks and diurnal evolution of NH3. The measured levels of NH3, especially high in the old city, may contribute to the high mean annual concentrations of secondary sulfate and nitrate measured in Barcelona compared with other cities in Spain affected by high traffic intensity. Ancillary measurements, including PM10, PM2.5, PM1 levels (Particulate Matter with aerodynamic diameter smaller than 10 μm, 2.5 μm, and 1 μm), gases and black carbon concentrations and meteorological data, were performed during the measurement campaign. The analysis of specific periods (3 special cases) during the campaign revealed that road traffic was a significant source of NH3. However, its effect was more evident at UB compared with CC where it was masked given the high levels of NH3 from non-traffic sources measured in the old city. The relationship between SO42− daily concentrations and gas-fraction ammonia (NH3/(NH3 + NH4+)) revealed that the gas-to-particle phase partitioning (volatilization or ammonium salts formation) also played an important role in the evolution of NH3 concentration in summer in Barcelona.

Published
2012
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43. A cell-based screening assay for Natural Killer cell activity

Author

W. Marty Blom, Ruud Albers, Wim G.L. van Nielen, and Els. M. de Groene

Subjects
Cell type, Immunology, Cell, Drug Evaluation, Preclinical, Biology, Peripheral blood mononuclear cell, Natural killer cell, chemistry.chemical_compound, Cell Line, Tumor, medicine, Immunology and Allergy, Humans, Immunologic Factors, Propidium iodide, Pharmacology, Lymphokine-activated killer cell, Biological activity, Flow Cytometry, Molecular biology, Killer Cells, Natural, medicine.anatomical_structure, chemistry, Cell culture, Biological Assay, K562 Cells
Abstract

Natural Killer (NK) cells are important in the first response against viruses and tumours. Compounds that modulate human NK cell activity offer interesting prophylactic and therapeutic options, however, a systematic screening tool is lacking. Development of suitable NK cell lines or receptor-based assays is hindered by the highly complicated regulation of the different NK cell subsets by multiple receptors. Here, we describe a cell-based flowcytometric activity assay adapted to identify NK cell modulating compounds. Fresh human peripheral blood mononuclear cells (PBMC) were incubated with NK-sensitive K562 target cells labelled with 5-(6)-carboxyfluorescein succinimidyl ester, followed by DNA-labelling with propidium iodide to identify dead cells. The assay demonstrated a good performance with an average Z'-factor of 0.6 and over 95% of the assays fulfilled the quality criteria, suggesting that it is possible to use a complex system with two different cell types to screen compounds. A large number of (natural) compounds and extracts were tested and normalized to the positive control, Interleukin-2. Promising and less promising compounds were distinguished. Effectiveness of compounds was based on the augmentation of NK cell activity as well as the number of responding subjects. To conclude the assay is robust, reliable and can be used for functional screening of natural compounds modulating NK cell activity.

Published
2008

44. Food allergy population thresholds: DBPCFC data for rice, kiwi, apple, peach, carrot, maize, tomato, and other less common allergenic foods

Author

Joost Westerhout, Ben Remington, Geert F. Houben, Joseph L. Baumert, Astrid G. Kruizinga, Steve L. Taylor, and W. Marty Blom

Subjects
Pulmonary and Respiratory Medicine, Allergy, education.field_of_study, Food industry, biology, business.industry, Immunology, Population, food and beverages, medicine.disease, medicine.disease_cause, biology.organism_classification, Biotechnology, Allergen, Food allergy, Kiwi, Immunology and Allergy, Medicine, Oral Presentation, Food allergens, Risk assessment, business, education
Abstract

The "Big 8" food allergens consists of cow's milk, eggs, wheat, peanuts, tree nuts, soybeans, fish, and crustacean shellfish and account for ~90% of the allergic reactions to foods. During the scientific review of the VITAL® (Voluntary Incidental Trace Allergen Labelling) program, individual challenge data were gathered for the Big 8 food allergens (plus mustard, sesame and celery) and, where possible, population threshold distributions were calculated. The VITAL® review process yielded over 1800 individual minimal eliciting doses (MED) for these allergens. However, ~80% of the previously gathered threshold data was generated by only 4 allergens: peanut (~40%), milk (~20%), egg (~10%) and hazelnut (~10%). Furthermore, over 150 foods have been reported to cause allergic reactions and clear data gaps still exist. For example, data gathered on celery and fish were not sufficient to generate a population distribution, threshold data for cashew were only available in children. Minimal eliciting doses for less commonly allergenic foods provides valuable information to all food allergy stakeholders. This study examines the current publically available MED data for rice, kiwi, apple, peach, carrot, maize, tomato, and other less common allergenic foods. This study will also try to minimize the datagaps of the "Big 8" food allergens. Where possible, population based threshold distributions and ED-values are calculated. Potency data from the less common allergens are compared to previously gathered data on the Big 8 food allergens. Additionally, all data collected during this study regarding the potency of less common allergens will be incorporated into the continued development of a validated, predictive and accepted allergen risk assessment strategy for existing and new protein sources and new or modified protein (containing) products. The results from this study should enable government and food industry risk managers to make more informed decisions regarding less commonly allergic foods.

Published
2015

45. The role of calpains in apoptotic changes in isolated hepatocytes after attack by Natural Killer cells

Author

W. Marty Blom, J. Fred Nagelkerke, Hans de Bont, and Gerard J. Mulder

Subjects
Pharmacology, Membrane potential, biology, Health, Toxicology and Mutagenesis, Calpain, General Medicine, Toxicology, Molecular biology, In vitro, Cell biology, medicine.anatomical_structure, Apoptosis, biology.protein, medicine, Cytoskeleton, Incubation, Nucleus, Caspase
Abstract

Previously, we showed that interleukin-2 activated Natural Killer cells (A-NK cells) in vitro rapidly induced apoptosis in freshly isolated rat hepatocytes (Blom et al., 1999. Hepatology 29 (3): 785-792) which was caused by a rapid decrease in the mitochondrial membrane potential and activation of caspases. In the present study we investigated the involvement of calpains in A-NK cell-induced apoptosis in isolated hepatocytes. When NK cells and hepatocytes were incubated in the presence of a calpain inhibitor the number of apoptotic cells decreased from 46 to 36%. However, more hepatocytes became necrotic (48 vs. 30%) as compared to the uninhibited situation. Inhibition of the calpains alone could not prevent the induction of the nuclear and cytoskeletal disruptions occurring in the hepatocytes. Inhibition of both calpains and caspases increased the number of necrotic cells as compared to incubation with a single inhibitor. However, the damage to the cytoskeleton of the surviving cells was completely inhibited. We conclude that calpains play a role in induction of apoptosis by NK cells. However, their role is limited as compared to caspases.

Published
2001

46. Changes of G-actin localisation in the mitotic spindle region or nucleus during mitosis and after heat shock: a histochemical study of G-actin in various cell lines with fluorescent labelled vitamin D-binding protein

Author

Hans de Bont, W. Marty Blom, J. Fred Nagelkerke, Irma Meijerman, and Gerard J. Mulder

Subjects
Hot Temperature, Swine, Mitosis, macromolecular substances, Spindle Apparatus, Biology, Nucleus, Phragmosome, Cell Line, Cytosol, Antineoplastic Combined Chemotherapy Protocols, medicine, Tumor Cells, Cultured, Animals, Humans, Nuclear protein, Molecular Biology, Cyclophosphamide, Cytoskeleton, Fluorescent Dyes, Cell Nucleus, Microscopy, Confocal, Histocytochemistry, Quinolinium Compounds, Vitamin D-Binding Protein, Cell Biology, DNA, Haplorhini, Molecular biology, Actins, Cell biology, Spindle apparatus, Cell nucleus, Thiazoles, medicine.anatomical_structure, Heat shock, G-actin, Cytoplasm, Doxorubicin, Vincristine, Interphase
Abstract

The presence and localisation of G-actin in various cell lines was studied using the highly G-actin specific, fluorescence-labelled vitamin D-binding protein. In various cell-types, pig kidney-derived cells (LLC-PK1), Chinese hamster ovary (CHO) cells, SV-40 transformed African green monkey kidney (COS) cells and human hepatoma (HepG2) cells, G-actin was only visible in the cytoplasm of interphase cells. However, in mitotic cells, depending on the mitotic phase, intense G-actin staining was found associated with the mitotic spindle (early mitosis) or overlapping the DNA-staining pattern (late mitosis). Also after heat shock (60-180 min at 43 degrees C), an intense nuclear staining of G-actin was observed. In LLC-PK1 cells, the increase of nuclear G-actin staining disappeared again after 24 h at 37 degrees C, but in COS, CHO and HepG2 cells, it was still present in the nucleus after 24 h at 37 degrees C, indicating that the process was not rapidly reversible in these cells; the increased nuclear G-actin was not associated with cell division. Comparison of the amount of G-actin present in the nucleus and in the cytosol before and after heat shock using Western blotting demonstrated that the total amount of G-actin in both nucleus and cytosol was unchanged after heat shock. This indicates that the increased G-actin staining is not a result of import of G-actin into the nucleus. These observations suggest a rearrangement of G-actin in the nucleus during both mitosis and heat shock, which may be due to changes in interaction of G-actin with chromosomes.

Published
1999

47. Understanding food allergen thresholds requires careful analysis of the available clinical data

Author

Geert F. Houben, Benjamin C. Remington, W. Marty Blom, René W.R. Crevel, Joseph L. Baumert, André C. Knulst, Simon Brooke-Taylor, Katrina J. Allen, Anthony E.J. Dubois, Steve L. Taylor, Astrid G. Kruizinga, and Groningen Research Institute for Asthma and COPD (GRIAC)

Subjects
Male, medicine.medical_specialty, Allergic reaction, Arachis, Immunology, CHILDREN, Food allergy, medicine, Humans, Immunology and Allergy, Peanut Hypersensitivity, Food allergens, Intensive care medicine, Glycoproteins, Plant Proteins, business.industry, Allergens, Antigens, Plant, medicine.disease, Hazelnut allergy, Geographic origin, Food processing, Female, business, 2S Albumins, Plant
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48. Food allergy population thresholds: an evaluation of the dosing scheme and number of oral food challenges on the accuracy of threshold dose studies

Author

W. Marty Blom, Joseph L. Baumert, Steve L. Taylor, Ben Remington, Carina M. Rubingh, Astrid G. Kruizinga, Rinke Klein Entink, and Geert F. Houben

Subjects
Pulmonary and Respiratory Medicine, Protocol (science), education.field_of_study, business.industry, Immunology, Provocation test, Population, medicine.disease, Threshold dose, Food allergy, Sample size determination, Statistics, medicine, Oral Presentation, Immunology and Allergy, Dosing, education, business, Risk management
Abstract

The availability of clinically established DBPCFC minimal eliciting doses determined in food-allergic individuals is increasing and previous work has shown these data can be used to determine population based reference doses for allergen risk management. Despite the large amount of data for peanut, milk, egg and hazelnut, EU and US public health authorities have not established population thresholds for any of the allergenic foods. In the absence of regulatory guidance regarding thresholds, food producers have attempted to manage risk through the widespread application of precautionary "may contain" labelling. In turn, food-allergic consumer quality-of-life has decreased and some food-allergic individuals are ignoring these advisory statements. This study aimed to assess the effects of the number of individual threshold doses and the dosing scheme intervals on the accuracy of estimates of population thresholds for allergenic foods. A simulation study was performed to evaluate the effects of sample size (N=20-750) and dosing scheme (derivatives of the EuroPrevall protocol) on the accuracy of the resulting threshold distribution curve. The simulations were based on clinical data on individual subject thresholds from peanut, egg and soy flour allergic individuals. The relationships between sample size, dosing scheme and the employed statistical distribution on the one hand and the accuracy of estimation of population based eliciting doses on the other hand were obtained. The largest relative gains in accuracy were seen when sample size increases from N=20 to N=60. Additionally, proper allocation of the dosing steps is important. So, while the EuroPrevall dosing scheme is a good start, the scheme may need revision for a specific allergen as more data become available. These results may guide risk assessors in determining minimum sample sizes for new studies and in the allocation of proper dosing schemes for allergens in provocation studies. In turn, these results will help determine dataset requirements when establishing population thresholds and reference doses leading to improved allergen risk management of food products.

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