Your search keyword '"Isaacs, J.D."' showing total 6 results

1. Reply: Functional cognitive disorder: dementia's blind spot

Author

Ball, H.A., McWhirter, L., Ballard, C., Bhome, R., Blackburn, D.J., Edwards, M.J., Fox, N.C., Howard, R., Huntley, J., Isaacs, J.D., Larner, A.J., Nicholson, T.R., Pennington, C.M., Poole, N., Price, G., Price, J.P., Reuber, M., Ritchie, C., Rossor, M.N., Schott, J.M., Venneri, A., Stone, J., and Carson, A.J.

Published

2021

2. High frequency of antidrug antibodies and association of random drug levels with efficacy in certolizumab pegol-treated patients with rheumatoid arthritis: results from the BRAGGSS cohort

Author

Jani, M., Isaacs, J.D., Morgan, A.W., Wilson, A.G., Plant, D., Hyrich, K.L., Chinoy, H., and Barton, A.

Abstract

Objectives To evaluate (i) the association between\ud random certolizumab drug levels, antidrug antibodies\ud (ADAbs) and treatment response in patients with\ud rheumatoid arthritis (RA); (ii) longitudinal factors\ud associated with ADAbs and certolizumab drug levels.\ud Methods This prospective cohort included 115 patients\ud with RA treated with certolizumab. Serum samples were\ud collected at 3, 6 and 12 months following treatment\ud initiation. Drug levels and ADAbs were measured using\ud ELISA and radioimmunoassay, respectively, at 3, 6 and\ud 12 months. Disease Activity Score in 28 joints (DAS28)\ud were measured at each visit and 12 months European\ud League Against Rheumatism (EULAR) response was\ud calculated. Patient self-reported adherence was collected\ud longitudinally. Ordinal logistic regression and generalised\ud estimating equation were used to test the association: (i)\ud between drug levels, from serum sampled and treatment\ud response; (ii) between ADAbs and drug levels; (iii)\ud patient-centred factors and drug levels.\ud Results ADAbs were detected in 37% (42/112 patients\ud by 12 months). The presence of ADAbs were significantly\ud associated with lower drug levels over 12 months\ud (β=−0.037, 95% CI −0.055 to 0.018, p

Published

2016

3. Rheumatoid Arthritis Risk Allele PTPRC Is Also Associated With Response to Anti-Tumor Necrosis Factor alpha Therapy

Author

Cui, J., Saevarsdottir, S., Thomson, B., Padyukov, L., Helm-van Mil, A.H.M. van der, Nititham, J., Hughes, L.B., Vries, N. de, Raychaudhuri, S., Alfredsson, L., Askling, J., Wedren, S., Ding, B., Guiducci, C., Wolbink, G.J., Crusius, J.B.A., Horst-Bruinsma, I.E. van der, Herenius, M., Weinblatt, M.E., Shadick, N.A., Worthington, J., Batliwalla, F., Kern, M., Morgan, A.W., Wilson, A.G., Isaacs, J.D., Hyrich, K., Seldin, M.F., Moreland, L.W., Behrens, T.W., Allaart, C.F., Criswell, L.A., Huizinga, T.W.J., Tak, P.P., Bridges, S.L., Toes, R.E.M., Barton, A., Klareskog, L., Gregersen, P.K., Karlson, E.W., Plenge, R.M., and Biol Rheumatoid Arthrit Genet & Ge

Subjects

genome-wide association genetic-variants controlled-trial susceptibility methotrexate locus polymorphism etanercept efficacy phosphatase

Abstract

Objective. Anti-tumor necrosis factor alpha (anti-TNF) therapy is a mainstay of treatment in rheumatoid arthritis (RA). The aim of the present study was to test established RA genetic risk factors to determine whether the same alleles also influence the response to anti-TNF therapy. Methods. A total of 1,283 RA patients receiving etanercept, infliximab, or adalimumab therapy were studied from among an international collaborative consortium of 9 different RA cohorts. The primary end point compared RA patients with a good treatment response according to the European League Against Rheumatism (EULAR) response criteria (n = 505) with RA patients considered to be nonresponders (n = 316). The secondary end point was the change from baseline in the level of disease activity according to the Disease Activity Score in 28 joints (Delta DAS28). Clinical factors such as age, sex, and concomitant medications were tested as possible correlates of treatment response. Thirty-one single-nucleotide polymorphisms (SNPs) associated with the risk of RA were genotyped and tested for any association with treatment response, using univariate and multivariate logistic regression models. Results. Of the 31 RA-associated risk alleles, a SNP at the PTPRC (also known as CD45) gene locus (rs10919563) was associated with the primary end point, a EULAR good response versus no response (odds ratio [OR] 0.55, P = 0.0001 in the multivariate model). Similar results were obtained using the secondary end point, the Delta DAS28 (P = 0.0002). There was suggestive evidence of a stronger association in autoantibody-positive patients with RA (OR 0.55, 95% confidence interval [95% CI] 0.39-0.76) as compared with autoantibody-negative patients (OR 0.90, 95% CI 0.41-1.99). Conclusion. Statistically significant associations were observed between the response to anti-TNF therapy and an RA risk allele at the PTPRC gene locus. Additional studies will be required to replicate this finding in additional patient collections.

Published

2010

4. Analysis of Fcγ receptor haplotypes in rheumatoid arthritis: FCGR3A remains a major susceptibility gene at this locus, with an additional contribution from FCGR3B

Author

Morgan, A.W., Barrett, J.H., Griffiths, B., Subramanian, D., Robinson, J.I., Keyte, V.H., Ali, M., Jones, E.A., Old, R.W., Ponchel, F., Boylston, A.W., Situnayake, R.D., Markham, A.F., Emery, P., and Isaacs, J.D.

Abstract

The Fcγ receptors play important roles in the initiation and regulation of many immunological and inflammatory processes, and genetic variants (FCGR) have been associated with numerous autoimmune and infectious diseases. The data in rheumatoid arthritis (RA) are conflicting and we previously demonstrated an association between FCGR3A and RA. In view of the close molecular proximity with FCGR2A, FCGR2B and FCGR3B, additional polymorphisms within these genes and FCGR haplotypes were examined to refine the extent of association with RA. Biallelic polymorphisms in FCGR2A, FCGR2B and FCGR3B were examined for association with RA in two well characterized UK Caucasian and North Indian/ Pakistani cohorts, in which FCGR3A genotyping had previously been undertaken. Haplotype frequencies and linkage disequilibrium were estimated across the FCGR locus and a model-free analysis was performed to determine association with RA. This was followed by regression analysis, allowing for phase uncertainty, to identify the particular haplotype(s) that\ud influences disease risk. Our results reveal that FCGR2A,\ud FCGR2B and FCGR3B were not associated with RA. The\ud haplotype with the strongest association with RA susceptibility was the FCGR3A–FCGR3B 158V-NA2 haplotype (odds ratio 3.18, 95% confidence interval 1.13–8.92 [P = 0.03] for homozygotes compared with all genotypes). The association was stronger in the presence of nodules (odds ratio 5.03, 95% confidence interval 1.44–17.56; P = 0.01). This haplotype was also more common in North Indian/Pakistani RA patients than in control individuals, but not significantly so. Logistic regression\ud analyses suggested that FCGR3A remained the most significant gene at this locus. The increased association with an FCGR3A–FCGR3B haplotype suggests that other\ud polymorphic variants within FCGR3A or FCGR3B, or in linkage\ud disequilibrium with this haplotype, may additionally contribute to disease pathogenesis.\ud

Published

2005

5. Association of FCGR3A and FCGR3B haplotypes with rheumatoid arthritis and primary Sjögren's syndrome [POSTER PRESENTATION]\ud

Author

Mackie, S., Robinson, J.I., Barrett, J.H., Lawson, C.A., Martin, S., Haroon-Rashid, L., Cooper, D., Bowman, S.J., Pease, C.T., Conaghan, P.G., Green, M., Quinn, M., Isaacs, J.D., Emery, P., and Morgan, A.W.

Abstract

Background \ud \ud \ud Rheumatoid arthritis (RA) is an autoimmune disease that is thought to arise from a complex interaction between multiple genetic factors and environmental triggers. We have previously demonstrated an association between a Fc gamma receptor (FcγR) haplotype and RA in a cross-sectional cohort of RA patients. We have sought to confirm this association in an inception cohort of RA patients and matched controls. We also extended our study to investigate a second autoanti-body associated rheumatic disease, primary Sjögren's syndrome (PSS).\ud \ud Methods \ud \ud The FCGR3A-158F/V and FCGR3B-NA1/NA2 functional polymorphisms were examined for association in an inception cohort of RA patients (n = 448), and a well-characterised PSS cohort (n = 83) from the United Kingdom. Pairwise disequilibrium coefficients (D') were calculated in 267 Blood Service healthy controls. The EHPlus program was used to estimate haplotype frequencies for patients and controls and to determine whether significant linkage disequilibrium was present. A likelihood ratio test is performed to test for differences between the haplotype frequencies in cases and controls. A permutation procedure implemented in this program enabled 1000 permutations to be performed on all haplotype associations to assess significance.\ud \ud \ud Results \ud \ud There was significant linkage disequilibrium between FCGR3A and FCGR3B (D' = -0.445, P = 0.001). There was no significant difference in the FCGR3A or FCGR3B allele or genotype frequencies in the RA or PSS patients compared with controls. However, there was a significant difference in the FCGR3A-FCGR3B haplotype distributions with increased homozygosity for the FCGR3A-FCGR3B 158V-NA2 haplotype in both our inception RA cohort (odds ratio = 2.15, 95% confidence interval = 1.1–4.2 P = 0.027) and PSS (odds ratio = 2.83, 95% confidence interval = 1.0–8.2, P = 0.047) compared with controls. The reference group for these analyses comprised individuals who did not possess a copy of the FCGR3A-FCGR3B 158V-NA2 haplotype.\ud \ud \ud Conclusions \ud \ud We have confirmed our original findings of association between the FCGR3A-FCGR3B 158V-NA2 haplotype and RA in a new inception cohort of RA patients. This suggests that there may be an RA-susceptibility gene at this locus. The significant increased frequency of an identical haplotype in PSS suggests the FcγR genetic locus may contribute to the pathogenesis of diverse autoantibody-mediated rheumatic diseases.\ud \ud

Published

2005

6. Real-time PCR based on SYBR-Green I fluorescence: An alternative to the TaqMan assay for a relative quantification of gene rearrangements, gene amplifications and micro gene deletions

Author

Ponchel, F., Toomes, C., Bransfield, K., Leong, F.T., Douglas, S.H., Field, S.L., Bell, S.M., Combaret, V., Puisieux, A., Mighell, A.J., Robinson, P.A., Inglehearn, C.F., Isaacs, J.D., and Markham, A.F.

Abstract

BACKGROUND:\ud \ud Real-time PCR is increasingly being adopted for RNA quantification and genetic analysis. At present the most popular real-time PCR assay is based on the hybridisation of a dual-labelled probe to the PCR product, and the development of a signal by loss of fluorescence quenching as PCR degrades the probe. Though this so-called 'TaqMan' approach has proved easy to optimise in practice, the dual-labelled probes are relatively expensive.\ud \ud RESULTS:\ud \ud We have designed a new assay based on SYBR-Green I binding that is quick, reliable, easily optimised and compares well with the published assay. Here we demonstrate its general applicability by measuring copy number in three different genetic contexts; the quantification of a gene rearrangement (T-cell receptor excision circles (TREC) in peripheral blood mononuclear cells); the detection and quantification of GLI, MYC-C and MYC-N gene amplification in cell lines and cancer biopsies; and detection of deletions in the OPA1 gene in dominant optic atrophy.\ud \ud CONCLUSION:\ud \ud Our assay has important clinical applications, providing accurate diagnostic results in less time, from less biopsy material and at less cost than assays currently employed such as FISH or Southern blotting.\ud

Published

2003