Your search keyword '"autoantibodies and disease"' showing total 3 results

1. Response to comment on 'AIRE-deficient patients harbor unique high-affinity disease-ameliorating autoantibodies'

Author

Christina Hertel, Dmytro Fishman, Anna Lorenc, Annamari Ranki, Kai Krohn, Pärt Peterson, Kai Kisand, and Adrian Hayday

Subjects

APS1/APECED, human B cell biology, autoantibodies and disease, type 1 diabetes, Medicine, Science, Biology (General), QH301-705.5

Abstract

In 2016, we reported four substantial observations of APECED/APS1 patients, who are deficient in AIRE, a major regulator of central T cell tolerance (Meyer et al., 2016). Two of those observations have been challenged. Specifically, ‘private’ autoantibody reactivities shared by only a few patients but collectively targeting >1000 autoantigens have been attributed to false positives (Landegren, 2019). While acknowledging this risk, our study-design included follow-up validation, permitting us to adopt statistical approaches to also limit false negatives. Importantly, many such private specificities have now been validated by multiple, independent means including the autoantibodies’ molecular cloning and expression. Second, a significant correlation of antibody-mediated IFNα neutralization with an absence of disease in patients highly disposed to Type I diabetes has been challenged because of a claimed failure to replicate our findings (Landegren, 2019). However, flaws in design and implementation invalidate this challenge. Thus, our results present robust, insightful, independently validated depictions of APECED/APS1, that have spawned productive follow-up studies.

Published

2019

2. Comment on 'AIRE-deficient patients harbor unique high-affinity disease-ameliorating autoantibodies'

Author

Elise M. N. Ferré, Michail S. Lionakis, Michael Snyder, Tove Fall, Gustav Smith, Eva Freyhult, Donald Sharon, Daniel Eriksson, Nils Landegren, Petter Brodin, Olle Kämpe, Lindsey B. Rosen, and Mark S. Anderson

Subjects

0301 basic medicine, immune tolerance, medicine, type 1 diabetes, Disease, Immune tolerance, immunology, human B cell biology, 0302 clinical medicine, Immunology and Inflammation, 2.1 Biological and endogenous factors, Aetiology, Biology (General), Polyendocrinopathies, Autoimmune, General Neuroscience, human biology, General Medicine, autoantigen, autoantibodies and disease, Interferon Type I, Medicine, medicine.symptom, Scientific Correspondence, Type 1, Human, QH301-705.5, Science, Inflammation, Autoimmune Disease, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Clinical Research, Diabetes Mellitus, Humans, In patient, APS1/APECED, human, Human Biology and Medicine, Gene, Metabolic and endocrine, Autoantibodies, Type 1 diabetes, General Immunology and Microbiology, business.industry, Autoantibody, Immunology in the medical area, medicine.disease, 030104 developmental biology, Diabetes Mellitus, Type 1, Polyendocrinopathies, inflammation, Immunologi inom det medicinska området, Immunology, Biochemistry and Cell Biology, business, 030217 neurology & neurosurgery, autoantibody, Autoimmune, Transcription Factors

Abstract

In 2016, we reported four substantial observations of APECED/APS1 patients, who are deficient in AIRE, a major regulator of central T cell tolerance (Meyer et al., 2016). Two of those observations have been challenged. Specifically, ‘private’ autoantibody reactivities shared by only a few patients but collectively targeting >1000 autoantigens have been attributed to false positives (Landegren, 2019). While acknowledging this risk, our study-design included follow-up validation, permitting us to adopt statistical approaches to also limit false negatives. Importantly, many such private specificities have now been validated by multiple, independent means including the autoantibodies’ molecular cloning and expression. Second, a significant correlation of antibody-mediated IFNα neutralization with an absence of disease in patients highly disposed to Type I diabetes has been challenged because of a claimed failure to replicate our findings (Landegren, 2019). However, flaws in design and implementation invalidate this challenge. Thus, our results present robust, insightful, independently validated depictions of APECED/APS1, that have spawned productive follow-up studies.

Published

2019

3. Response to comment on 'AIRE-deficient patients harbor unique high-affinity disease-ameliorating autoantibodies'.

Author

Hertel C, Fishman D, Lorenc A, Ranki A, Krohn K, Peterson P, Kisand K, and Hayday A

Subjects

Autoantigens, Humans, T-Lymphocytes, Transcription Factors, Autoantibodies, Polyendocrinopathies, Autoimmune

Abstract

In 2016, we reported four substantial observations of APECED/APS1 patients, who are deficient in AIRE, a major regulator of central T cell tolerance (Meyer et al., 2016). Two of those observations have been challenged. Specifically, 'private' autoantibody reactivities shared by only a few patients but collectively targeting >1000 autoantigens have been attributed to false positives (Landegren, 2019). While acknowledging this risk, our study-design included follow-up validation, permitting us to adopt statistical approaches to also limit false negatives. Importantly, many such private specificities have now been validated by multiple, independent means including the autoantibodies' molecular cloning and expression. Second, a significant correlation of antibody-mediated IFNα neutralization with an absence of disease in patients highly disposed to Type I diabetes has been challenged because of a claimed failure to replicate our findings (Landegren, 2019). However, flaws in design and implementation invalidate this challenge. Thus, our results present robust, insightful, independently validated depictions of APECED/APS1, that have spawned productive follow-up studies., Competing Interests: CH CH is an employee in ImmunoQure AG, which contributed research funding to the study by Meyer et al., 2016. DF, AL No competing interests declared, AR AR is an equity holder in ImmunoQure AG. KK KKr is an equity holder in ImmunoQure AG. PP PP is an equity holder in ImmunoQure AG. KK KKi is an equity holder in ImmunoQure AG. AH AH is an equity holder in ImmunoQure AG., (© 2019, Hertel et al.)

Published

2019