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Drug Tolerant Anti-...
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Kharlamova, N.Karolinska Institutet
(author)
Drug Tolerant Anti-drug Antibody Assay for Infliximab Treatment in Clinical Practice Identifies Positive Cases Earlier
- Article/chapterEnglish2020
Publisher, publication year, extent ...
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2020-07-21
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Frontiers Media SA,2020
Numbers
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LIBRIS-ID:oai:gup.ub.gu.se/296304
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https://gup.ub.gu.se/publication/296304URI
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https://doi.org/10.3389/fimmu.2020.01365DOI
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http://kipublications.ki.se/Default.aspx?queryparsed=id:144398895URI
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Subject category:ref swepub-contenttype
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Subject category:art swepub-publicationtype
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A subgroup of patients treated with infliximab lose response to the treatment and one reason for this is the development of anti-drug antibodies (ADA). If used optimally, measuring drug and ADA level could lead to a more personalized and efficient treatment regime, and enable identification of ADA-positive patients before the underlying disease flares or allergic reactions occur. With the use of a drug-tolerant ADA assay which can detect ADA irrespective of drug levels in the sample, we determined the impact of ADA on treatment failure to infliximab. The aims of this study were to estimate the real-life optimal serum infliximab (sIFX) level and set a clinical threshold value for a drug-tolerant ADA assay. Trough levels of sIFX were measured with ELISA. Free ADA was measured with two drug-sensitive methods (ELISA and a bioassay) and one drug-tolerant method (PandA). Two real-life cohorts treated with infliximab were included; a cross-sectional cohort including patients with inflammatory rheumatic diseases (n= 270) and a prospective cohort of rheumatoid arthritis (RA) patients (n= 73) followed for 1 year. Normal range of sIFX was estimated from the prospective cohort and an arbitrary optimal drug level was set to be between 1 and 6 mu g/mL. Using this range, optimal sIFX was found in only 60% (163/270) of the patients in the cross-sectional cohort. These patients had significantly better treatment response than those with a drug level under 1 mu g/mL, who had an ADA frequency of 34% (19/56) using the drug-tolerant method. In the prospective cohort, the drug-tolerant assay could identify 34% (53/155 samples) as ADA positive in samples with sIFX level >0.2 mu g/mL. ADA were seldom detected in patients with >1 mu g/mL sIFX, with three interesting exceptions. A clinically relevant ADA threshold was determined to be >3 RECL as measured with the drug-tolerant assay. In a real-life setting, there was a substantial number of patients with suboptimal drug levels and a proportion of these had ADA. Both too low and too high drug levels correlated with worse disease, but for different reasons. Adding a drug-tolerant assay enabled detection of ADA earlier and regardless of drug level at time of sampling.
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Hermanrud, C.
(author)
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Dunn, N.Karolinska Institutet
(author)
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Ryner, M.
(author)
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Hambardzumyan, K.
(author)
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Pomiano, N. V.
(author)
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Marits, P.
(author)
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Gjertsson, Inger,1962Gothenburg University,Göteborgs universitet,Institutionen för medicin, avdelningen för reumatologi och inflammationsforskning,Institute of Medicine, Department of Rheumatology and Inflammation Research(Swepub:gu)xgjein
(author)
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Saevarsdottir, S.Karolinska Institutet
(author)
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Pullerits, Rille,1969Gothenburg University,Göteborgs universitet,Institutionen för medicin, avdelningen för reumatologi och inflammationsforskning,Institute of Medicine, Department of Rheumatology and Inflammation Research(Swepub:gu)xpulri
(author)
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Fogdell-Hahn, A.Karolinska Institutet
(author)
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Karolinska InstitutetInstitutionen för medicin, avdelningen för reumatologi och inflammationsforskning
(creator_code:org_t)
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In:Frontiers in Immunology: Frontiers Media SA111664-3224
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Kharlamova, N.
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Hermanrud, C.
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Dunn, N.
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Ryner, M.
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Pomiano, N. V.
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Marits, P.
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University of Gothenburg
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