Michael R. Ardern‐Jones scite author profile

Atopic dermatitis comorbidities extend well beyond the march to allergic conditions (food allergy, asthma, allergic rhinitis, allergic conjunctivitis, and eosinophilic esophagitis), suggesting both cutaneous and systemic immune activation. In reviewing atopic dermatitis comorbidities, Councilors of the International Eczema Council found a strong pattern of immune activation in peripheral blood and the propensity to both skin and systemic infections. Associations with cardiovascular, neuropsychiatric, and malignant diseases were increasingly reported, but confirmation of their link with atopic dermatitis requires longitudinal studies. Given the possibility of atopic dermatitis-related systemic immune activation, future investigations of new interventions should concurrently examine the impact on these comorbidities.

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UK guidelines for the management of Stevens–Johnson syndrome/toxic epidermal necrolysis in adults 2016

Creamer

Walsh

Dziewulski

et al. 2016

Journal of Plastic, Reconstructive & Aesthetic Surgery

128

238

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U.K. guidelines for the management of Stevens–Johnson syndrome/toxic epidermal necrolysis in adults 2016

et al. 2016

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When does atopic dermatitis warrant systemic therapy? Recommendations from an expert panel of the International Eczema Council

Simpson

Bruin‐Weller

Flohr

et al. 2017

Journal of the American Academy of Dermatology

175

186

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Conformation of the Human Immunoglobulin G2 Hinge Imparts Superagonistic Properties to Immunostimulatory Anticancer Antibodies

et al. 2015

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SummaryMonoclonal antibody (mAb) drugs that stimulate antitumor immunity are transforming cancer treatment but require optimization for maximum clinical impact. Here, we show that, unlike other immunoglobulin isotypes, human IgG2 (h2) imparts FcγR-independent agonistic activity to immune-stimulatory mAbs such as anti-CD40, -4-1BB, and -CD28. Activity is provided by a subfraction of h2, h2B, that is structurally constrained due its unique arrangement of hinge region disulfide bonds. Agonistic activity can be transferred from h2 to h1 by swapping their hinge and CH1 domains, and substitution of key hinge and CH1 cysteines generates homogenous h2 variants with distinct agonistic properties. This provides the exciting opportunity to engineer clinical reagents with defined therapeutic activity regardless of FcγR expression levels in the local microenvironment.

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EAACI position paper on how to classify cutaneous manifestations of drug hypersensitivity

Brockow

Ardern‐Jones

Mockenhaupt

et al. 2018

Allergy

164

172

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SJS/TEN 2017: Building Multidisciplinary Networks to Drive Science and Translation

White

Abe

Ardern‐Jones

et al. 2018

The Journal of Allergy and Clinical Immunology: In Practice

138

125

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Stevens-Johnson syndrome/toxic epidermal necrolysis (SJS/TEN) is a life-threatening, immunologically mediated, and usually drug-induced disease with a high burden to individuals, their families, and society with an annual incidence of 1 to 5 per 1,000,000. To effect significant reduction in short- and long-term morbidity and mortality, and advance clinical care and research, coordination of multiple medical, surgical, behavioral, and basic scientific disciplines is required. On March 2, 2017, an investigator-driven meeting was held immediately before the American Academy of Dermatology Annual meeting for the central purpose of assembling, for the first time in the United States, clinicians and scientists from multiple disciplines involved in SJS/TEN clinical care and basic science research. As a product of this meeting, this article summarizes the current state of knowledge and expert opinion related to SJS/TEN covering a broad spectrum of topics including epidemiology and pharmacogenomic networks; clinical management and complications; special populations such as pediatrics, the elderly, and pregnant women; regulatory issues and the electronic health record; new agents that cause SJS/TEN; pharmacogenomics and immunopathogenesis; and the patient perspective. Goals include the maintenance of a durable and productive multidisciplinary network that will significantly further scientific progress and translation into prevention, early diagnosis, and management of SJS/TEN.

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Persistent central memory phenotype of circulating Fel d 1 peptide/DRB1∗0101 tetramer-binding CD4+ T cells

Bateman

Ardern‐Jones

Ogg

2006

Journal of Allergy and Clinical Immunology

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