Identification of drug-specific public TCR driving severe cutaneous adverse reactions

Pan, Ren‐You; Chu, Mu-Tzu; Wang, Chuang‐Wei; Lee, Yun‐Shien; Lemonnier, François; Michels, Aaron; Schutte, Ryan J.; Ostrov, David A.; Chen, Chun‐Bing; Phillips, Elizabeth; Mallal, S.; Mockenhaupt, Maja; Bellón, Teresa; Tassaneeyakul, Wichittra; White, Katie D.; Roujeau, Jean‐Claude; Chung, Wen‐Hung; Hung, Shuen‐Iu

doi:10.1038/s41467-019-11396-2

Cited by 98 publications

(121 citation statements)

References 71 publications

(89 reference statements)

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“…Furthermore, carbamazepine‐specific cytotoxic T cells could be primed from PBMC of healthy human donors that were carriers of both HLA‐B*15:02 and VB‐11‐IsGSY. More recently, the same group working on the same patient cohort reported the detection of a public T‐cell receptor composed of paired TCRα CDR3 “VFDNTDKLI” and TCRβ CDR3 “ASSLAGELF” clonotypes and that similar receptor clusters are found in the blister fluid cells and peripheral blood . These data suggest that the correct combination of HLA, drug‐peptide complex and T‐cell receptor may be important drivers for carbamazepine‐induced Stevens‐Johnson syndrome.…”

Section: Does Expression Of Specific T‐cell Receptors Impact On Suscementioning

confidence: 92%

Immune dysregulation increases the incidence of delayed‐type drug hypersensitivity reactions

Naisbitt

Olsson‐Brown

Gibson

et al. 2019

Allergy

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Delayed-type, T cell-mediated, drug hypersensitivity reactions are a serious unwanted manifestation of drug exposure that develops in a small percentage of the human population. Drugs and drug metabolites are known to interact directly and indirectly (through irreversible protein binding and processing to the derived adducts) with HLA proteins that present the drug-peptide complex to T cells. Multiple forms of drug hypersensitivity are strongly linked to expression of a single HLA allele, and there is increasing evidence that drugs and peptides interact selectively with the protein encoded by the HLA allele. Despite this, many individuals expressing HLA risk alleles do not develop hypersensitivity when exposed to culprit drugs suggesting a nonlinear, multifactorial relationship in which HLA risk alleles are one factor. This has prompted a search for additional susceptibility factors. Herein, we argue that immune regulatory pathways are one key determinant of susceptibility. As expression and activity of these pathways are influenced by disease, environmental and patient factors, it is currently impossible to predict whether drug exposure will result in a health benefit, hypersensitivity or both. Thus, a concerted effort is required to investigate how immune dysregulation influences susceptibility towards drug hypersensitivity. K E Y W O R D Sdrug hypersensitivity, HLA, immune checkpoint inhibitors, regulation, T cells

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Section: Does Expression Of Specific T‐cell Receptors Impact On Suscementioning

confidence: 92%

Immune dysregulation increases the incidence of delayed‐type drug hypersensitivity reactions

Naisbitt

Olsson‐Brown

Gibson

et al. 2019

Allergy

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“…Multiple predictive genomic markers (Table 2) are subsequently determined to prevent drugspecific SJS/TEN and serum biomarkers such as IL-15 and granulysin [34,35] may have roles in predicting the prognosis of acute stage SJS/TEN. Single-cell (sc) T-cell receptor (TCR) sequencing and repertoire analysis are novel approaches to investigate drug-specific T cell populations and can be paired with sc-RNAseq and Cite-seq to examine expression of the related transcriptome and proteome of total cell populations on interest [48][49]. Dominant TCRαβ clonotypes have been identified in single cells sorted from blister samples of patients with HLA-B*58:01 restricted allopurinol-SJS/TEN and HLA-B*15:02 restricted carbamazepine-SJS/TEN which in the case of the latter represent a public TCRαβ clonotype that is shared amongst unrelated HLA-B*15:02 positive patients with carbamazepine SJS/TEN [48][49].…”

Section: Models and Mechanismmentioning

confidence: 99%

SJS/TEN 2019: From science to translation

Chang

Abe

Anderson

et al. 2020

Journal of Dermatological Science

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Stevens-Johnson syndrome and toxic epidermal necrolysis (SJS/TEN) are potentially lifethreatening, immune-mediated adverse reactions characterized by widespread erythema, epidermal necrosis, and detachment of skin and mucosa. Efforts to grow and develop functional international collaborations and a multidisciplinary interactive network focusing on SJS/TEN as an uncommon but high burden disease will be necessary to improve efforts in prevention, early diagnosis and improved acute and long-term management. SJS/TEN 2019: From Science to Translation was a 1.5-day scientific program held April 26-27, 2019, in Vancouver, Canada. The meeting successfully engaged clinicians, researchers, and patients and conducted many productive discussions on research and patient care needs.

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“…Intracellular processing was not required for cytotoxicity 112 . Computational modelling confirmed binding of carbamazepine in the HLA binding groove and interaction with the TCR to establish the TCR‐HLA complex 112–114 . Carbamazepine did not alter the peptide repertoire of HLA‐B*15:2, excluding the altered peptide model of EN pathogenesis 115 …”

Section: Genetic Susceptibilitymentioning

confidence: 90%

“…Apart from the HLA molecules, a specific TCR and peptide presented are required to establish the TCR‐HLA interaction 119–121 . Recently, a preferential TCR clonotype was identified, binding to carbamazepine which can subsequently constitute the interaction between this TCR and HLA‐B*15:2 114 . Regarding the sequence and quantity of the peptide presented by the HLA, variants in genes related to proteasomal function or peptide generation can contribute to the risk for EN 120,122,123 .…”

Section: Genetic Susceptibilitymentioning

confidence: 99%

Clinical and pathogenic aspects of the severe cutaneous adverse reaction epidermal necrolysis (EN)

Kuijper

French

Tensen

et al. 2020

Acad Dermatol Venereol

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The severe cutaneous adverse reaction epidermal necrolysis (EN) which includes toxic epidermal necrolysis and the milder Stevens‐Johnson syndrome is characterized by epidermal loss due to massive keratinocyte apoptosis and/or necroptosis. EN is often caused by a drug mediating a specific TCR‐HLA interaction via the (pro)hapten, pharmacological interaction or altered peptide loading mechanism involving a self‐peptide presented by keratinocytes. (Memory) CD8 + T cells are activated and exhibit cytotoxicity against keratinocytes via the perforin/granzyme B and granulysin pathway and Fas/FasL interaction. Alternatively drug‐induced annexin release by CD14 + monocytes can induce formyl peptide receptor 1 death of keratinocytes by necroptosis. Subsequent keratinocyte death stimulates local inflammation, activating other immune cells producing pro‐inflammatory molecules and downregulating regulatory T cells. Widespread epidermal necrolysis and inflammation can induce life‐threatening systemic effects, leading to high mortality rates. Research into genetic susceptibility aims to identify risk factors for eventual prevention of EN. Specific HLA class I alleles show the strongest association with EN, but risk variants have also been identified in genes involved in drug metabolism, cellular drug uptake, peptide presentation and function of CD8 + T cells and other immune cells involved in cytotoxic responses. After the acute phase of EN, long‐term symptoms can remain or arise mainly affecting the skin and eyes. Mucosal sequelae are characterized by occlusions and strictures due to adherence of denuded surfaces and fibrosis following mucosal inflammation. In addition, systemic pathology can cause acute and chronic hepatic and renal symptoms. EN has a large psychological impact and strongly affects health‐related quality of life among EN survivors.

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Identification of drug-specific public TCR driving severe cutaneous adverse reactions

Cited by 98 publications

References 71 publications

Immune dysregulation increases the incidence of delayed‐type drug hypersensitivity reactions

Immune dysregulation increases the incidence of delayed‐type drug hypersensitivity reactions

SJS/TEN 2019: From science to translation

Clinical and pathogenic aspects of the severe cutaneous adverse reaction epidermal necrolysis (EN)

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