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159 results on '"Bilò, M B"'

3. Allergen immunotherapy for insect venom allergy: a systematic review and meta‐analysis

Author

Dhami, S., Zaman, H., Varga, E.‐M., Sturm, G. J., Muraro, A., Akdis, C. A., Antolín‐Amérigo, D., Bilò, M. B., Bokanovic, D., Calderon, M. A., Cichocka‐Jarosz, E., Oude Elberink, J. N. G., Gawlik, R., Jakob, T., Kosnik, M., Lange, J., Mingomataj, E., Mitsias, D. I., Mosbech, H., Ollert, M., Pfaar, O., Pitsios, C., Pravettoni, V., Roberts, G., Ruëff, F., Sin, B. A., Asaria, M., Netuveli, G., and Sheikh, A.

Published
2017
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7. Anaphylaxis: guidelines from the European Academy of Allergy and Clinical Immunology

Author

Muraro, A., Roberts, G., Worm, M., Bilò, M. B., Brockow, K., Rivas, Fernández M., Santos, A. F., Zolkipli, Z. Q., Bellou, A., Beyer, K., Bindslev-Jensen, C., Cardona, V., Clark, A. T., Demoly, P., Dubois, A. E. J., DunnGalvin, A., Eigenmann, P., Halken, S., Harada, L., Lack, G., Jutel, M., Niggemann, B., Ruëff, F., Timmermans, F., Vlieg–Boerstra, B. J., Werfel, T., Dhami, S., Panesar, S., Akdis, C. A., and Sheikh, A.

Published
2014
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8. Management of anaphylaxis: a systematic review

Author

Dhami, S., Panesar, S. S., Roberts, G., Muraro, A., Worm, M., Bilò, M. B., Cardona, V., Dubois, A. E. J., DunnGalvin, A., Eigenmann, P., Fernandez-Rivas, M., Halken, S., Lack, G., Niggemann, B., Rueff, F., Santos, A. F., Vlieg-Boerstra, B., Zolkipli, Z. Q., and Sheikh, A.

Published
2014
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9. Detection of Gibberellin-Regulated Protein (Peamaclein) Sensitization among Italian Cypress Pollen-Sensitized Patients

Author

Asero, R, Abbadessa, S, Aruanno, A, Barilaro, G, Barzaghi, C, Bignardi, D, Bilò, M B, Borro, M, Bresciani, M, Busa, M, Buzzulini, F, Cavaliere, C, Cecchi, L, Ciccarelli, A, Cortellini, G, Cucinelli, F, Deleonardi, G, Emiliani, F, Farsi, A, Ferrarini, E, Franchini, M, Ingrassia, A, Lippolis, D, Losappio, L, Marra, A M, Martini, M, Masieri, S, Mauro, M, Mazzolini, M, Muratore, L, Murzilli, F, Nucera, E, Pastorello, E A, Pinter, E, Polillo, B R, Pravettoni, V, Quercia, O, Rizzi, A, Russello, M, Sacerdoti, C, Scala, E, Scala, G, Scarpa, A, Schroeder, J, Uasuf, G G, Villalta, D, Yang, B, Mistrello, G, Amato, S, Lidholm, J, Nucera, E (ORCID:0000-0002-0565-7680), Rizzi, A (ORCID:0000-0002-6795-746X), Asero, R, Abbadessa, S, Aruanno, A, Barilaro, G, Barzaghi, C, Bignardi, D, Bilò, M B, Borro, M, Bresciani, M, Busa, M, Buzzulini, F, Cavaliere, C, Cecchi, L, Ciccarelli, A, Cortellini, G, Cucinelli, F, Deleonardi, G, Emiliani, F, Farsi, A, Ferrarini, E, Franchini, M, Ingrassia, A, Lippolis, D, Losappio, L, Marra, A M, Martini, M, Masieri, S, Mauro, M, Mazzolini, M, Muratore, L, Murzilli, F, Nucera, E, Pastorello, E A, Pinter, E, Polillo, B R, Pravettoni, V, Quercia, O, Rizzi, A, Russello, M, Sacerdoti, C, Scala, E, Scala, G, Scarpa, A, Schroeder, J, Uasuf, G G, Villalta, D, Yang, B, Mistrello, G, Amato, S, Lidholm, J, Nucera, E (ORCID:0000-0002-0565-7680), and Rizzi, A (ORCID:0000-0002-6795-746X)

Abstract

Background: Peach gibberellin-regulated protein (peamaclein) has recently emerged as a relevant food allergen in cypress pollen-hypersensitive patients. Objective: We looked for mono-sensitization to peamaclein among Italian cypress-pollen allergic patients. Material and methods: 835 cypress pollen hypersensitive patients from 28 Italian allergy centers under went thorough interview for food-allergic reactions, and SPT with a commercial peach extracts containing peamaclein. In peach reactors, IgE to rPru p 3 was measured, and those scoring negative were enrolled as potentially mono-sensitized to peamaclein. IgE reactivity to rPru p 7 was evaluated by immunoblot and by an experimental ImmunoCAP with rPru p 7. Results: Peach SPT scored positive in 163 (19.5%) patients but 127 (77,9%) were excluded because Pru p 3 reactors. Twenty-four (14,7%, corresponding to 2.8% of the entire study population) were considered as potentially mono-sensitized to peamaclein. Their distribution did not show any geographic preference. Seventeen/24 (70,8%) had a history of food allergy, in most cases (n=15) to peach. Other offending foods included other Rosaceae, citrus fruits, fig, melon, tree nuts, and kiwi. On peach immunoblot, only 3/18 putative peamaclein allergic subjects reacted to a band at about 7kDa; 4 other patients reacted at about 50-60 kDa. Ten/18 (56%) scored positive for Pru p 7 on ImmunoCAP. Conclusion: Peamaclein allergy and sensitization prevalence seem rare in Italy. Most patients react to peach, albeit other Rosaceae fruits and several citrus fruits may also act as offending foods. Peach and cypress pollen probably share also cross-reacting allergens other than peamaclein.

Published
2020

10. The epidemiology of anaphylaxis in Europe: a systematic review

Author

Panesar, S. S., Javad, S., de Silva, D., Nwaru, B. I., Hickstein, L., Muraro, A., Roberts, G., Worm, M., Bilò, M. B., Cardona, V., Dubois, A. E. J., Galvin, Dunn A., Eigenmann, P., Fernandez-Rivas, M., Halken, S., Lack, G., Niggemann, B., Santos, A. F., Vlieg-Boerstra, B. J., Zolkipli, Z. Q., and Sheikh, A.

Published
2013
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15. European Polistes venom allergy

Author

Severino, M. G., Campi, P., Macchia, D., Manfredi, M., Turillazzi, S., Spadolini, I., Bilò, M. B., and Bonifazi, F.

Published
2006

16. EAACI guidelines on allergen immunotherapy: Hymenoptera venom allergy

Author

Sturm, G J, Varga, E-M, Roberts, G, Mosbech, H, Bilò, M B, Akdis, C A, Antolín-Amérigo, D, Cichocka-Jarosz, E, Gawlik, R, Jakob, T, Kosnik, M, Lange, J, Mingomataj, E, Mitsias, D I, Ollert, M, Oude Elberink, J N G, Pfaar, O, Pitsios, C, Pravettoni, V, Ruëff, F, Sin, B A, Agache, I, Angier, E, Arasi, S, Calderón, M A, Fernandez-Rivas, M, Halken, S, Jutel, M, Lau, S, Pajno, G B, et al, and University of Zurich

Subjects
2403 Immunology, 10183 Swiss Institute of Allergy and Asthma Research, Immunology, 2723 Immunology and Allergy, Immunology and Allergy, 610 Medicine & health
Published
2018

22. The urgent need for a harmonized severity scoring system for acute allergic reactions

Author

Muraro, A., primary, Fernandez-Rivas, M., additional, Beyer, K., additional, Cardona, V., additional, Clark, A., additional, Eller, E., additional, Hourihane, J. O'B., additional, Jutel, M., additional, Sheikh, A., additional, Agache, I., additional, Allen, K. J., additional, Angier, E., additional, Ballmer-Weber, B., additional, Bilò, M. B., additional, Bindslev-Jensen, C., additional, Camargo, C. A., additional, Cianferoni, A., additional, DunnGalvin, A., additional, Eigenmann, P. A., additional, Halken, S., additional, Hoffmann-Sommergruber, K., additional, Lau, S., additional, Nilsson, C., additional, Poulsen, L. K., additional, Rueff, F., additional, Spergel, J., additional, Sturm, G., additional, Timmermans, F., additional, Torres, M. J., additional, Turner, P., additional, van Ree, R., additional, Wickman, M., additional, Worm, M., additional, Mills, E. N. C., additional, and Roberts, G., additional

Published
2018
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23. Cover Image

Author

Blank, S., primary, Bilò, M. B., additional, and Ollert, M., additional

Published
2018
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25. Allergy in urban elderly population living in Campania region (Southern Italy). A multicenter study

Author

Liccardi, G., Baldi, G., Berra, A., Ciccarelli, A., Cutajar, M., D Amato, M., D Angelo, R., Gargano, D., Giannattasio, D., Leone, G., Lo Schiavo, M., Madonna, F., Montera, C., Monti, R., Parente, R., Pedicini, A., Pio, A., Russo, M., Salzillo, A., Stanziola, A., Alessandro Vatrella, Manzi, F., and Bilò, M. B.

Subjects
Adult, allergic rhinitis, Urban Health, allergic sensitization, Intradermal Tests, Middle Aged, allergy, elderly, Campania region, bronchial asthma, hypersensitivity, Age Distribution, Age of Onset, Aged, Cross-Sectional Studies, Humans, Italy, Prevalence, Respiratory Hypersensitivity, Risk Factors
Abstract

Given the increasing life expectancy observed in Western countries, there is a marked interest to know more about how aging could influence respiratory health. The aim of our study was to assess the prevalence, clinical characteristics and age of onset of allergic sensitization and clinical symptoms in a sample of atopic elders living in Campania region area (Southern Italy). Fourteen Allergy units or Centres examined a total of 462 patients. In this context 215 (46.53%) had positive skin prick tests (SPTs) to at least one allergen and were diagnosed with respiratory allergy. Parietaria represents the most common sensitizing agent in elders living in Campania region, followed by dust mites, grass pollen and Olea europaea. A relatively high percentage of atopic subjects suffered from respiratory symptoms at a fairly advanced age, namely 8.3% at 60-64 years, 10.2% at 65-70 and 5.7% at70 years. In conclusion, the prevalence and clinical significance of airway allergic sensitization in the elderly living in Campania region is more significant than expected in latter stages of life. Physicians should not neglect the role of atopy as a risk factor for the onset of allergic respiratory symptoms even in elderly patients.

Published
2016

26. EAACI guidelines on allergen immunotherapy: Hymenoptera venom allergy

Author

Sturm, G. J., primary, Varga, E.‐M., additional, Roberts, G., additional, Mosbech, H., additional, Bilò, M. B., additional, Akdis, C. A., additional, Antolín‐Amérigo, D., additional, Cichocka‐Jarosz, E., additional, Gawlik, R., additional, Jakob, T., additional, Kosnik, M., additional, Lange, J., additional, Mingomataj, E., additional, Mitsias, D. I., additional, Ollert, M., additional, Oude Elberink, J. N. G., additional, Pfaar, O., additional, Pitsios, C., additional, Pravettoni, V., additional, Ruëff, F., additional, Sin, B. A., additional, Agache, I., additional, Angier, E., additional, Arasi, S., additional, Calderón, M. A., additional, Fernandez‐Rivas, M., additional, Halken, S., additional, Jutel, M., additional, Lau, S., additional, Pajno, G. B., additional, van Ree, R., additional, Ryan, D., additional, Spranger, O., additional, van Wijk, R. G., additional, Dhami, S., additional, Zaman, H., additional, Sheikh, A., additional, and Muraro, A., additional

Published
2017
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27. EAACI Molecular Allergology User's Guide

Author

Matricardi, P. M., Kleine-Tebbe, J., Hoffmann, H. J., Valenta, R., Hilger, C., Hofmaier, S., Aalberse, R. C., Agache, I., Asero, R., Ballmer-Weber, B., Barber, D., Beyer, K., Biedermann, T., Bilò, M. B., Blank, S., Bohle, B., Bosshard, P. P., Breiteneder, H., Brough, H. A., Caraballo, L., Caubet, J. C., Crameri, R., Davies, J. M., Douladiris, N., Ebisawa, M., EIgenmann, P. A., Fernandez-Rivas, M., Ferreira, F., Gadermaier, G., Glatz, M., Hamilton, R. G., Hawranek, T., Hellings, P., Hoffmann-Sommergruber, K., Jakob, T., Jappe, U., Jutel, M., Kamath, S. D., Knol, E. F., Korosec, P., Kuehn, A., Lack, G., Lopata, A. L., Mäkelä, M., Morisset, M., Niederberger, V., Nowak-Węgrzyn, A. H., Papadopoulos, N. G., Pastorello, E. A., Pauli, G., Platts-Mills, T., Posa, D., Poulsen, L. K., Raulf, M., Sastre, J., Scala, E., Schmid, J. M., Schmid-Grendelmeier, P., van Hage, M., van Ree, R., Vieths, S., Weber, R., Wickman, M., Muraro, A., Ollert, M., Matricardi, P. M., Kleine-Tebbe, J., Hoffmann, H. J., Valenta, R., Hilger, C., Hofmaier, S., Aalberse, R. C., Agache, I., Asero, R., Ballmer-Weber, B., Barber, D., Beyer, K., Biedermann, T., Bilò, M. B., Blank, S., Bohle, B., Bosshard, P. P., Breiteneder, H., Brough, H. A., Caraballo, L., Caubet, J. C., Crameri, R., Davies, J. M., Douladiris, N., Ebisawa, M., EIgenmann, P. A., Fernandez-Rivas, M., Ferreira, F., Gadermaier, G., Glatz, M., Hamilton, R. G., Hawranek, T., Hellings, P., Hoffmann-Sommergruber, K., Jakob, T., Jappe, U., Jutel, M., Kamath, S. D., Knol, E. F., Korosec, P., Kuehn, A., Lack, G., Lopata, A. L., Mäkelä, M., Morisset, M., Niederberger, V., Nowak-Węgrzyn, A. H., Papadopoulos, N. G., Pastorello, E. A., Pauli, G., Platts-Mills, T., Posa, D., Poulsen, L. K., Raulf, M., Sastre, J., Scala, E., Schmid, J. M., Schmid-Grendelmeier, P., van Hage, M., van Ree, R., Vieths, S., Weber, R., Wickman, M., Muraro, A., and Ollert, M.

Published
2016

28. EAACI Molecular Allergology User's Guide

Author

MS Dermatologie/Allergologie, CDL Celdiagnostiek, Infection & Immunity, Matricardi, P. M., Kleine-Tebbe, J., Hoffmann, H. J., Valenta, R., Hilger, C., Hofmaier, S., Aalberse, R. C., Agache, I., Asero, R., Ballmer-Weber, B., Barber, D., Beyer, K., Biedermann, T., Bilò, M. B., Blank, S., Bohle, B., Bosshard, P. P., Breiteneder, H., Brough, H. A., Caraballo, L., Caubet, J. C., Crameri, R., Davies, J. M., Douladiris, N., Ebisawa, M., EIgenmann, P. A., Fernandez-Rivas, M., Ferreira, F., Gadermaier, G., Glatz, M., Hamilton, R. G., Hawranek, T., Hellings, P., Hoffmann-Sommergruber, K., Jakob, T., Jappe, U., Jutel, M., Kamath, S. D., Knol, E. F., Korosec, P., Kuehn, A., Lack, G., Lopata, A. L., Mäkelä, M., Morisset, M., Niederberger, V., Nowak-Węgrzyn, A. H., Papadopoulos, N. G., Pastorello, E. A., Pauli, G., Platts-Mills, T., Posa, D., Poulsen, L. K., Raulf, M., Sastre, J., Scala, E., Schmid, J. M., Schmid-Grendelmeier, P., van Hage, M., van Ree, R., Vieths, S., Weber, R., Wickman, M., Muraro, A., Ollert, M., MS Dermatologie/Allergologie, CDL Celdiagnostiek, Infection & Immunity, Matricardi, P. M., Kleine-Tebbe, J., Hoffmann, H. J., Valenta, R., Hilger, C., Hofmaier, S., Aalberse, R. C., Agache, I., Asero, R., Ballmer-Weber, B., Barber, D., Beyer, K., Biedermann, T., Bilò, M. B., Blank, S., Bohle, B., Bosshard, P. P., Breiteneder, H., Brough, H. A., Caraballo, L., Caubet, J. C., Crameri, R., Davies, J. M., Douladiris, N., Ebisawa, M., EIgenmann, P. A., Fernandez-Rivas, M., Ferreira, F., Gadermaier, G., Glatz, M., Hamilton, R. G., Hawranek, T., Hellings, P., Hoffmann-Sommergruber, K., Jakob, T., Jappe, U., Jutel, M., Kamath, S. D., Knol, E. F., Korosec, P., Kuehn, A., Lack, G., Lopata, A. L., Mäkelä, M., Morisset, M., Niederberger, V., Nowak-Węgrzyn, A. H., Papadopoulos, N. G., Pastorello, E. A., Pauli, G., Platts-Mills, T., Posa, D., Poulsen, L. K., Raulf, M., Sastre, J., Scala, E., Schmid, J. M., Schmid-Grendelmeier, P., van Hage, M., van Ree, R., Vieths, S., Weber, R., Wickman, M., Muraro, A., and Ollert, M.

Published
2016

29. EAACI molecular allergology user's guide

Author

Matricardi, P M, Kleine-Tebbe, J, Hoffmann, H.J., Valenta, R, Hilger, C, Hofmaier, S, Aalberse, R C, Agache, I, Asero, R, Ballmer-Weber, B, Barber, D, Beyer, K, Biedermann, T, Bilò, M B, Blank, S, Bohle, B, Bosshard, P P, Breiteneder, H, Brough, H A, Caraballo, L, Caubet, J C, Crameri, R, Davies, J M, Douladiris, N, Ebisawa, M, EIgenmann, P A, Fernandez-Rivas, M, Ferreira, F, Gadermaier, G, Glatz, M, Hamilton, R G, Hawranek, T, Hellings, P, Hoffmann-Sommergruber, K, Jakob, T, Jappe, U, Jutel, M, Kamath, S D, Knol, E F, Korosec, P, Kuehn, A, Lack, G, Lopata, A L, Mäkelä, M, Morisset, M, Niederberger, V, Nowak-Węgrzyn, A H, Papadopoulos, N G, Pastorello, E A, Pauli, G, Platts-Mills, T, Posa, D, Poulsen, L. K., Raulf, M, Sastre, J, Scala, E, Schmid, J M, Schmid-Grendelmeier, P, van Hage, M, van Ree, R, Vieths, S, Weber, R, Wickman, M, Muraro, A, Ollert, M., Matricardi, P M, Kleine-Tebbe, J, Hoffmann, H.J., Valenta, R, Hilger, C, Hofmaier, S, Aalberse, R C, Agache, I, Asero, R, Ballmer-Weber, B, Barber, D, Beyer, K, Biedermann, T, Bilò, M B, Blank, S, Bohle, B, Bosshard, P P, Breiteneder, H, Brough, H A, Caraballo, L, Caubet, J C, Crameri, R, Davies, J M, Douladiris, N, Ebisawa, M, EIgenmann, P A, Fernandez-Rivas, M, Ferreira, F, Gadermaier, G, Glatz, M, Hamilton, R G, Hawranek, T, Hellings, P, Hoffmann-Sommergruber, K, Jakob, T, Jappe, U, Jutel, M, Kamath, S D, Knol, E F, Korosec, P, Kuehn, A, Lack, G, Lopata, A L, Mäkelä, M, Morisset, M, Niederberger, V, Nowak-Węgrzyn, A H, Papadopoulos, N G, Pastorello, E A, Pauli, G, Platts-Mills, T, Posa, D, Poulsen, L. K., Raulf, M, Sastre, J, Scala, E, Schmid, J M, Schmid-Grendelmeier, P, van Hage, M, van Ree, R, Vieths, S, Weber, R, Wickman, M, Muraro, A, and Ollert, M.

Abstract

The availability of allergen molecules ('components') from several protein families has advanced our understanding of immunoglobulin E (IgE)-mediated responses and enabled 'component-resolved diagnosis' (CRD). The European Academy of Allergy and Clinical Immunology (EAACI) Molecular Allergology User's Guide (MAUG) provides comprehensive information on important allergens and describes the diagnostic options using CRD. Part A of the EAACI MAUG introduces allergen molecules, families, composition of extracts, databases, and diagnostic IgE, skin, and basophil tests. Singleplex and multiplex IgE assays with components improve both sensitivity for low-abundance allergens and analytical specificity; IgE to individual allergens can yield information on clinical risks and distinguish cross-reactivity from true primary sensitization. Part B discusses the clinical and molecular aspects of IgE-mediated allergies to foods (including nuts, seeds, legumes, fruits, vegetables, cereal grains, milk, egg, meat, fish, and shellfish), inhalants (pollen, mold spores, mites, and animal dander), and Hymenoptera venom. Diagnostic algorithms and short case histories provide useful information for the clinical workup of allergic individuals targeted for CRD. Part C covers protein families containing ubiquitous, highly cross-reactive panallergens from plant (lipid transfer proteins, polcalcins, PR-10, profilins) and animal sources (lipocalins, parvalbumins, serum albumins, tropomyosins) and explains their diagnostic and clinical utility. Part D lists 100 important allergen molecules. In conclusion, IgE-mediated reactions and allergic diseases, including allergic rhinoconjunctivitis, asthma, food reactions, and insect sting reactions, are discussed from a novel molecular perspective. The EAACI MAUG documents the rapid progression of molecular allergology from basic research to its integration into clinical practice, a quantum leap in the management of allergic patients.

Published
2016

30. EAACI Molecular Allergology User's Guide

Author

Matricardi, P. M., primary, Kleine‐Tebbe, J., additional, Hoffmann, H. J., additional, Valenta, R., additional, Hilger, C., additional, Hofmaier, S., additional, Aalberse, R. C., additional, Agache, I., additional, Asero, R., additional, Ballmer‐Weber, B., additional, Barber, D., additional, Beyer, K., additional, Biedermann, T., additional, Bilò, M. B., additional, Blank, S., additional, Bohle, B., additional, Bosshard, P. P., additional, Breiteneder, H., additional, Brough, H. A., additional, Caraballo, L., additional, Caubet, J. C., additional, Crameri, R., additional, Davies, J. M., additional, Douladiris, N., additional, Ebisawa, M., additional, EIgenmann, P. A., additional, Fernandez‐Rivas, M., additional, Ferreira, F., additional, Gadermaier, G., additional, Glatz, M., additional, Hamilton, R. G., additional, Hawranek, T., additional, Hellings, P., additional, Hoffmann‐Sommergruber, K., additional, Jakob, T., additional, Jappe, U., additional, Jutel, M., additional, Kamath, S. D., additional, Knol, E. F., additional, Korosec, P., additional, Kuehn, A., additional, Lack, G., additional, Lopata, A. L., additional, Mäkelä, M., additional, Morisset, M., additional, Niederberger, V., additional, Nowak‐Węgrzyn, A. H., additional, Papadopoulos, N. G., additional, Pastorello, E. A., additional, Pauli, G., additional, Platts‐Mills, T., additional, Posa, D., additional, Poulsen, L. K., additional, Raulf, M., additional, Sastre, J., additional, Scala, E., additional, Schmid, J. M., additional, Schmid‐Grendelmeier, P., additional, van Hage, M., additional, van Ree, R., additional, Vieths, S., additional, Weber, R., additional, Wickman, M., additional, Muraro, A., additional, and Ollert, M., additional

Published
2016
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31. Self-medication of anaphylactic reactions due to Hymenoptera stings-an EAACI Task Force Consensus Statement

Author

Bilò, M. B., primary, Cichocka-Jarosz, E., additional, Pumphrey, R., additional, Oude-Elberink, J. N., additional, Lange, J., additional, Jakob, T., additional, Bonadonna, P., additional, Fernandez, J., additional, Kosnik, M., additional, Helbling, A., additional, Mosbech, H., additional, Gawlik, R., additional, Niedoszytko, M., additional, Patella, V., additional, Pravettoni, V., additional, Rodrigues-Alves, R., additional, Sturm, G. J., additional, and Rueff, F., additional

Published
2016
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32. EAACI guidelines on allergen immunotherapy: Hymenoptera venom allergy.

Author

Sturm, G. J., Varga, E.‐M., Roberts, G., Mosbech, H., Bilò, M. B., Akdis, C. A., Antolín‐Amérigo, D., Cichocka‐Jarosz, E., Gawlik, R., Jakob, T., Kosnik, M., Lange, J., Mingomataj, E., Mitsias, D. I., Ollert, M., Oude Elberink, J. N. G., Pfaar, O., Pitsios, C., Pravettoni, V., and Ruëff, F.

Subjects
ALLERGENS, IMMUNOTHERAPY, CLINICAL immunology, ALLERGY treatment, ANTIHISTAMINES, VENOM hypersensitivity
Abstract

Abstract: Hymenoptera venom allergy is a potentially life‐threatening allergic reaction following a honeybee, vespid, or ant sting. Systemic‐allergic sting reactions have been reported in up to 7.5% of adults and up to 3.4% of children. They can be mild and restricted to the skin or moderate to severe with a risk of life‐threatening anaphylaxis. Patients should carry an emergency kit containing an adrenaline autoinjector, H1‐antihistamines, and corticosteroids depending on the severity of their previous sting reaction(s). The only treatment to prevent further systemic sting reactions is venom immunotherapy. This guideline has been prepared by the European Academy of Allergy and Clinical Immunology's (EAACI) Taskforce on Venom Immunotherapy as part of the EAACI Guidelines on Allergen Immunotherapy initiative. The guideline aims to provide evidence‐based recommendations for the use of venom immunotherapy, has been informed by a formal systematic review and meta‐analysis and produced using the Appraisal of Guidelines for Research and Evaluation (AGREE II) approach. The process included representation from a range of stakeholders. Venom immunotherapy is indicated in venom‐allergic children and adults to prevent further moderate‐to‐severe systemic sting reactions. Venom immunotherapy is also recommended in adults with only generalized skin reactions as it results in significant improvements in quality of life compared to carrying an adrenaline autoinjector. This guideline aims to give practical advice on performing venom immunotherapy. Key sections cover general considerations before initiating venom immunotherapy, evidence‐based clinical recommendations, risk factors for adverse events and for relapse of systemic sting reaction, and a summary of gaps in the evidence. [ABSTRACT FROM AUTHOR]

Published
2018
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33. Management of anaphylaxis:a systematic review

Author

Dhami, S, Panesar, S S, Roberts, G, Muraro, A, Worm, M, Bilò, M B, Cardona, V, Dubois, A E J, DunnGalvin, A, Eigenmann, P, Fernandez-Rivas, M, Halken, S, Lack, G, Niggemann, B, Rueff, F, Santos, A F, Vlieg-Boerstra, B, Zolkipli, Z Q, Sheikh, A, Poulsen, Lars K., Dhami, S, Panesar, S S, Roberts, G, Muraro, A, Worm, M, Bilò, M B, Cardona, V, Dubois, A E J, DunnGalvin, A, Eigenmann, P, Fernandez-Rivas, M, Halken, S, Lack, G, Niggemann, B, Rueff, F, Santos, A F, Vlieg-Boerstra, B, Zolkipli, Z Q, Sheikh, A, and Poulsen, Lars K.

Abstract

To establish the effectiveness of interventions for the acute and long-term management of anaphylaxis, seven databases were searched for systematic reviews, randomized controlled trials, quasi-randomized controlled trials, controlled clinical trials, controlled before-after studies and interrupted time series and - only in relation to adrenaline - case series investigating the effectiveness of interventions in managing anaphylaxis. Fifty-five studies satisfied the inclusion criteria. We found no robust studies investigating the effectiveness of adrenaline (epinephrine), H1-antihistamines, systemic glucocorticosteroids or methylxanthines to manage anaphylaxis. There was evidence regarding the optimum route, site and dose of administration of adrenaline from trials studying people with a history of anaphylaxis. This suggested that administration of intramuscular adrenaline into the middle of vastus lateralis muscle is the optimum treatment. Furthermore, fatality register studies have suggested that a failure or delay in administration of adrenaline may increase the risk of death. The main long-term management interventions studied were anaphylaxis management plans and allergen-specific immunotherapy. Management plans may reduce the risk of further reactions, but these studies were at high risk of bias. Venom immunotherapy may reduce the incidence of systemic reactions in those with a history of venom-triggered anaphylaxis.

Published
2014

34. The epidemiology of anaphylaxis in Europe:a systematic review

Author

Panesar, S S, Javad, S, de Silva, D, Nwaru, B I, Hickstein, L, Muraro, A, Roberts, G, Worm, M, Bilò, M B, Cardona, V, Dubois, A E J, Dunn Galvin, A, Eigenmann, P, Fernandez-Rivas, M, Halken, S, Lack, G, Niggemann, B, Santos, A F, Vlieg-Boerstra, B J, Zolkipli, Z Q, Sheikh, A, Poulsen, Lars K., Panesar, S S, Javad, S, de Silva, D, Nwaru, B I, Hickstein, L, Muraro, A, Roberts, G, Worm, M, Bilò, M B, Cardona, V, Dubois, A E J, Dunn Galvin, A, Eigenmann, P, Fernandez-Rivas, M, Halken, S, Lack, G, Niggemann, B, Santos, A F, Vlieg-Boerstra, B J, Zolkipli, Z Q, Sheikh, A, and Poulsen, Lars K.

Abstract

BACKGROUND: Anaphylaxis is an acute, potentially fatal, multi-organ system, allergic reaction caused by the release of chemical mediators from mast cells and basophils. Uncertainty exists around epidemiological measures of incidence and prevalence, risk factors, risk of recurrence, and death due to anaphylaxis. This systematic review aimed to (1) understand and describe the epidemiology of anaphylaxis and (2) describe how these characteristics vary by person, place, and time.METHODS: Using a highly sensitive search strategy, we identified systematic reviews of epidemiological studies, descriptive and analytical epidemiological investigations, and studies involving analysis of routine data.RESULTS: Our searches identified a total of 5,843 potentially eligible studies, of which 49 satisfied our inclusion criteria. Of these, three were suitable for pooled estimates of prevalence. The incidence rates for all-cause anaphylaxis ranged from 1.5 to 7.9 per 100,000 person-years. These data indicated that an estimated 0.3% (95% CI 0.1-0.5) of the population experience anaphylaxis at some point in their lives. Food, drugs, stinging insects, and latex were the most commonly identified triggers.CONCLUSIONS: Anaphylaxis is a common problem, affecting an estimated 1 in 300 of the European population at some time in their lives. Future research needs to focus on better understanding of the trends across Europe and identifying those most likely to experience fatal reactions.

Published
2013

36. Drug hypersensitivity in clonal mast cell disorders: ENDA/ EAACI position paper.

Author

Bonadonna, P., Pagani, M., Aberer, W., Bilò, M. B., Brockow, K., Oude Elberink, H., Garvey, L., Mosbech, H., Romano, A., Zanotti, R., and Torres, M. J.

Subjects
MAST cell disease, DRUG allergy, SKIN physiology, BONE marrow physiology, ANTI-inflammatory agents
Abstract

Mastocytosis is a clonal disorder characterized by the proliferation and accumulation of mast cells ( MC) in different tissues, with a preferential localization in skin and bone marrow ( BM). The excess of MC in mastocytosis as well as the increased releasability of MC may lead to a higher frequency and severity of immediate hypersensitivity reactions. Mastocytosis in adults is associated with a history of anaphylaxis in 22-49%. Fatal anaphylaxis has been described particularly following hymenoptera stings, but also occasionally after the intake of drugs such as nonsteroidal anti-inflammatory drugs, opioids and drugs in the perioperative setting. However, data on the frequency of drug hypersensitivity in mastocytosis and vice versa are scarce and evidence for an association appears to be limited. Nevertheless, clonal MC disorders should be ruled out in cases of severe anaphylaxis: basal serum tryptase determination, physical examination for cutaneous mastocytosis lesions, and clinical characteristics of anaphylactic reaction might be useful for differential diagnosis. In this position paper, the ENDA group performed a literature search on immediate drug hypersensitivity reactions in clonal MC disorders using MEDLINE, EMBASE, and Cochrane Library, reviewed and evaluated the literature in five languages using the GRADE system for quality of evidence and strength of recommendation. [ABSTRACT FROM AUTHOR]

Published
2015
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39. Efficacy of an air-cleaning device equipped with a high efficiency particulate air filter in house dust mite respiratory allergy.

Author

Antonicelli, L., Bilò, M. B., Pucci, S., Schou, C., and Bonifazi, F.

Subjects
RESPIRATORY allergy, DERMATOPHAGOIDES, ASTHMA, PATIENTS, OBSTRUCTIVE lung diseases, RESPIRATORY diseases
Abstract

The efficacy of an air-cleaning device equipped with a high efficiency particulate air (HEPA) filter (without further avoidance measures) was studied in patients allergic to house dust mite. The effects of the air-cleaner on indoor Dermatophagoides sp. levels, symptom score and bronchial hyperresponsiveness in nine mite-allergic patients were assessed using a cross-over controlled study. No significant effect was demonstrated on indoor Dermatophagoides sp. levels when comparing the period of air-cleaner activity (2 months) with the control period (2 months). The Dermatophagoides sp. levels in the houses studied were lower than the risk level for asthmatic attacks, making it difficult to assess any effect on asthma; however, neither bronchial hyperresponsiveness nor rhinitis symptom score were changed by air-cleaner activity. During the trial period, however the mean level of Dermatophagoides sp. allergen in the houses changed spontaneously from 4.4 μg/g ( mean level in the first 2 trial months) to 1.75 μg/g of dust (second 2 months) (P < 0.05). Owing to this change, the mean rhinitis symptom score also decreased (P < 0.05), even if no significant correlation was demonstrated (r = 0.4 P = 0.089). HEPA filter air-cleaners appear insufficient as substitutes for standard avoidance measures in mite allergic patients. [ABSTRACT FROM AUTHOR]

Published
1991
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42. Near fatal asthma: Treatment and prevention

Author

D Amato, G., Vitale, C., Lanza, M., Sanduzzi, A., Molino, A., Mormile, M., Vatrella, A., Bilo, M. B., Antonicelli, L., Bresciani, M., CLAUDIO MICHELETTO, Vaghi, A., D Amato, M., D'Amato, G, Vitale, C, Lanza, M, SANDUZZI ZAMPARELLI, Alessandro, Molino, Antonio, Mormile, Mauro, Vatrella, A, Bilò, M. B, Antonicelli, L, Bresciani, M, Micheletto, C, Vaghi, A, and D'Amato, M.

Subjects
Emergency Medical Services, Severe asthma, Near fatal asthma, Asthma attack, Combined Modality Therapy, Respiration, Artificial, Severity of Illness Index, Asthma, Acute asthma, Asthma exacerbations, Asthma-related deaths, Immunology and Allergy, asthma exacerbation, Phenotype, Treatment Outcome, Predictive Value of Tests, Risk Factors, Acute Disease, asthma-related death, Humans, Anti-Asthmatic Agents
Abstract

Near-fatal asthma (NFA) is described as acute asthma associated with a respiratory arrest or arterial carbon dioxide tension greater than 50 mmHg, with or without altered consciousness, requiring mechanical ventilation. Risk factors for near fatal asthma have not been fully elucidated. In 80-85% of all fatal events, a phenotype, characterized by eosinophilic inflammation associated with gradual deterioration occurring in patients with severe and poorly controlled asthma, has been identified. Regarding to the management, acute severe asthma remains a significant clinical problem, which needs to be identified to facilitate early and appropriate therapeutic interventions. The assessment relies on clinical signs, but additional information might be obtained from chest radiography or blood gas analysis. No investigation should delay the initiation of appropriate therapy. The goals of therapy are the maintenance of oxygenation, relief of airflow obstruction, reduction of airways edema and mucus plugging (with Increased use of medications such as beta-agonists via metered dose inhalers and nebulizers, oral and/or intravenous (other than by inhalation) corticosteroids and oral or intravenous theophylline) whereas supporting ventilation as clinically indicated. Of course, the emergency physician needs to consider the wide range of potential complications, as attention to these problems when managing severe acute asthma might significantly improve outcome. An understanding of the available agents and potential pitfalls in the management of NFA is mandatory for the emergency physician.

43. The added value of targeting airway hyperresponsiveness by blocking TSLP in the management of severe asthma.

Author

Vaghi A, Bilò MB, Bini F, Cecchi L, Micheletto C, and Musarra A

Abstract

Summary: Airways hyperresponsiveness (AHR) is a pathognomonic event of asthma in which the airways are reactive to various bronchoconstrictor stimuli at 'doses' that normally have no bronchoconstrictor effect in non-asthmatics. AHR is an objective measure of clinical efficacy, and the introduction of biologics revived interest as a marker of disease and its pathophysiologic mechanism. This article aims to discuss the mechanisms of AHR, focusing on the role of epithelial damage and TSLP production, and promote its correct assessment for the evaluation of patients with severe asthma, to predict the risk of exacerbations and outcomes, and the eligibility for treatment with an anti-TSLP agent. AHR is a complex trait of asthma, induced by the concurrence of many pathophysiological factors and related to different clinical manifestations. Recent evidence demonstrates the important role of airway epithelial damage and TSLP production in many of these events. A therapeutic response based on AHR control could be considered as a condition of disease remission and seems a promising new goal for the management of patients with severe asthma.

Published
2024
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44. A narrative review on allergy and exposure to domestic and non-domestic animals: favorable and unfavorable effects.

Author

Liccardi G, Martini M, Bilò MB, Cecchi L, Milanese M, Musarra A, Puxeddu E, and Rogliani P

Abstract

Summary: The aim of this contribution was to highlight the "favorable" and "unfavorable" roles of domestic and non-domestic animals on airway sensitization processes and on the type/severity of the clinical symptoms induced by their exposure. We performed a literature research in MEDLINE for allergic manifestations and animals. Pets can be "allergy friends" through mechanisms related to hygiene hypothesis and translational aspects, the dual role of IgG4 antibodies for pets, and their promising role as healthcare service animals (dogs). On the contrary, animals can be "allergy enemies" when inducing allergic sensitization and  respiratory symptoms (sometimes leading to severe reactions), and also due to cross reactivity with other pets allergens, indirect exposure and ubiquity of their allergens, cross reactivity between Can f 5 and human prostate-specific antigen (PSA). Moreover, in some cases they can trigger anaphylaxis, induce occupational asthma, and act as pests. Finally, we must outline the modest efficacy of allergen immunotherapy (AIT) for their allergens. From a strictly allergological perspective, it is evident that the "negative" aspects resulting from exposure to domestic / non-domestic animals outweigh the "positive" aspects. As a consequence, it is up to humans to seek new ways to balance the pros and cons by exploring research areas that can allow the best possible coexistence with subjects at risk of allergy with domestic and non-domestic animals.

Published
2024
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45. Eosinophil-associated diseases: the Allergist's and Clinical Immunologist's perspective.

Author

Marra AM, Rossi CM, Piga MA, Moroncini G, and Bilò MB

Subjects
Humans, Hypereosinophilic Syndrome diagnosis, Hypereosinophilic Syndrome immunology, Hypereosinophilic Syndrome drug therapy, Allergy and Immunology, Sinusitis immunology, Sinusitis diagnosis, Eosinophils immunology, Eosinophilia immunology, Eosinophilia diagnosis, Allergists
Abstract

Summary: Eosinophil-associated diseases (EADs) refer to heterogeneous conditions in which eosinophils are believed to play critical pathological roles. They encompass common respiratory conditions, such as asthma, chronic rhinosinusitis with nasal polyps (CRSwNP), less common primary eosinophilic disorders of gastrointestinal tract, and rare conditions including eosinophilic granulomatosis with polyangiitis (EGPA) and hypereosinophilic syndrome (HES). A literature search was carried out in January 2024 in the MEDLINE and Scopus databases using the PubMed search engine (PubMed, National Library of Medicine, Bethesda, MD). We focused on blood eosinophilia and hypereosinophilia. A diagnostic workup is proposed. From allergist's point of view, we focused the review on 4 groups of eosinophilic disorders of specific interest. Our increased understanding of type 2 inflammation and biology has recently led to development of highly effective precision targeted therapies that are now approved for a growing number of eosinophilic disorders. Novel targeted biologics have a major impact on treatment strategies and have resulted in major advances in our understanding of the pathogenesis of these disorders. In the context of EADs, according to the heterogeneity of eosinophilic disorders a multidisciplinary approach should be adopted. Allergists and Clinical Immunologists play an important role as they have a clear understanding of the eosinophilic inflammation and the role of cytokines and are trained to recognize and characterize type 2 (T2) inflammation and its associated pathologies.

Published
2024
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46. Why is pet (cat/dog) allergen immunotherapy (AIT) such a controversial topic? Current perspectives and future directions.

Author

Liccardi G, Martini M, Bilò MB, Cecchi L, Milanese M, Brussino L, Motta E, and Rogliani P

Subjects
Cats, Animals, Dogs, Humans, Desensitization, Immunologic methods, Desensitization, Immunologic trends, Allergens immunology, Hypersensitivity immunology, Hypersensitivity therapy, Hypersensitivity diagnosis, Pets immunology
Abstract

Summary: Dogs and cats are the most common pets worldwide. In Italy, the prevalence of allergic sensitization to cats and dogs is 16% and 9% respectively. The limited standardization of allergenic extracts, especially for dogs, emphasizes the importance of Component Resolved Diagnosis (CRD) for accurate diagnosis and subsequent prescription of allergen immunotherapy (AIT). However, this low standardization is the main factor contributing to the unsatisfactory clinical efficacy of traditional AIT, AIT with modified allergens, and intralymphatic allergen-specific immunotherapy (ILAIT). Emerging immunological approaches, particularly for controlling the primary cat allergen, show promise but are hindered by high costs (e.g., use of anti-Fel d 1 monoclonal antibodies in humans) or by exclusively targeting Fel d 1 produced by one's own animal (e.g., immunizing cats to induce neutralizing antibodies against Fel d 1 or including an egg product with anti Fel d 1 IgY antibodies in feline diet). Further studies are imperative for standardizing pet allergens, enhancing the efficacy of various AIT modalities, and exploring other immunological approaches, to optimize the relationship between pets and their owners and prevent distressing "forced removals".

Published
2024
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47. Chronic rhinosinusitis with nasal polyposis and biological agents: the ARIA-ITALY Survey.

Author

Lombardi C, Passalacqua G, Menzella F, Mauritz Canevari RF, Danesi G, Pusateri AM, Carone M, Vancheri C, Di Marco F, Micheletto C, Manzotti G, Di Gioacchino M, Bilò MB, Gelardi M, Senna G, and Canonica GW

Abstract

Summary: Background. Chronic rhinosinusitis (CRS) is an inflammatory disease that affects the nasal mucosa and the paranasal sinuses. CRS can be associated by nasal polyposis (CRSwNP phenotype) in up to 30% of patients and it is frequently associated with bronchial asthma. CRSwNP shows predominantly an underlying activation of type 2 inflammatory pathways with the involvement of eosinophils, IgE, interleukin (IL)-4, IL-5 and IL-13. Biological drugs that target these inflammatory cytokines are currently a therapeutic option recognized by guidelines for the treatment of uncontrolled form of the disease. Methods. As part of the activity of the "ARIA-Italy" working group, a panel of 255 Italian Ear, Nose and Throat (ENT) specialists, pneumologists and immuno-allergologists actively participated in this national survey and answered a series of questions geared toward understanding the main criteria for patient characterization and therapeutic decision, highlighting multidisciplinarity, and the implementation of the management of CRSwNP patients, as a part of the precision medicine concept and the appropriate use of the biologicals. Results. Two hundred and fifty-five experts and specialists participated in the survey. Conclusions. The results of this survey obtained from an extensive number of active specialists throughout Italy allow some important concluding remarks to be drawn. The main points of agreement were that multidisciplinary care teams provide many benefits but that, once the team is established, meetings and communication between members must be coordinated. Finally, the dissemination of national disease registries and the continuous updating of guidelines and position papers related to CRSwNP and comorbidities should be encouraged.

Published
2024
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50. Severe asthma: follow-up after one year from the Italian Registry on Severe Asthma (IRSA)

Author

Bilò MB, Martini M, Antonicelli L, Aliani M, Carone M, Cecchi L, de Michele F, Polese G, Vaghi A, Musarra A, and Micheletto C

Subjects
Humans, Child, Cost-Effectiveness Analysis, Portugal epidemiology, Standard of Care, Immunotherapy, Poaceae, Asthma drug therapy, Rhinitis, Allergic, Biological Products therapeutic use, Anti-Asthmatic Agents therapeutic use
Abstract

Summary: Background. Asthma affects millions of people worldwide, with a subgroup suffering from severe asthma (SA). Biologics have revolutionized SA treatment, but challenges remain in managing different patient traits. This study analyzed data from the Italian Registry on Severe Asthma (IRSA) to investigate changes in SA characteristics and effectiveness of treatments after one year of follow-up, and to identify factors associated with response to treatments in a real-world setting. Methods. Data on SA patients with one year of follow-up were extracted from IRSA. Asthma control, exacerbations, lung function, and treatments, were assessed at follow-up and analyzed against baseline characteristics. Results. After one year of follow-up, notable improvements were observed in all the outcomes of SA of the included patients (n = 570). The effectiveness of biologic therapies was particularly evident, as they contributed significantly to these positive outcomes. Additionally, certain factors were found to be associated with improvement, namely T2 phenotype, baseline eosinophil count (BEC), and area of residence. On the other hand, comorbidities (obesity, gastro-esophageal reflux disease) and poor lung function were risk factors. Notably, poor-responders to biologics exhibited lower level of education, BEC, and exacerbations, and higher frequency of atopy and ACT score ≥ 20. Conclusions. The findings demonstrate the effectiveness of biologics in asthma management, when implemented as part of a planned follow-up strategy aimed at optimizing and fine-tuning the therapy. Moreover, the study highlights the importance of considering key traits such as the T2 phenotype, BEC, education, and comorbidities when tailoring SA treatment. Overall, this study contributes to enhancing our understanding of SA management and guiding the development of personalized treatment approaches for patients with SA.

Published
2023
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