Your search keyword '"Lamb, Janine"' showing total 32 results

1. Panel of serum biomarkers for differential diagnosis of idiopathic interstitial lung disease and interstitial lung disease-secondary to systemic autoimmune rheumatic disease.

Author

d'Alessandro, Miriana, Cameli, Paolo, Cotton, Caroline V., Lamb, Janine A., Bergantini, Laura, Gangi, Sara, Sugden, Sarah, Spencer, Lisa G., Frediani, Bruno, New, Robert P., Chinoy, Hector, Bargagli, Elena, and Conticini, Edoardo

Subjects

INTERSTITIAL lung diseases, PULMONARY fibrosis, CHEMILUMINESCENCE assay, IDIOPATHIC diseases, RHEUMATISM, LUNGS, FERRITIN

Abstract

Background: Interstitial lung disease (ILD) may complicate the course of systemic autoimmune rheumatic disease (SARD) and diagnostic biomarkers are needed. Krebs von den Lungen-6 (KL-6), ferritin (FER) and interleukin 6 (IL-6) have been involved in the ILD development. Our study aimed to compare KL-6, FER, IL-6 and soluble mesothelin-related peptide (SMRP) concentrations in a cohort of idiopathic and SARD-ILD. Methods: 3169 patients were enrolled in the "UK Biomarkers in Interstitial Lung Disease (UK-BILD) Study". We selected patients affected by SARD-ILD and idiopathic ILD (usual interstitial pneumonia-idiopathic pulmonary fibrosis and fibrotic non-specific interstitial pneumonia). Serum marker concentrations were measured through chemiluminescent assays (Fujirebio Europe, Ghent, Belgium). Results: 1013 patients were selected for the study: 520 (51.3%) had idiopathic ILD and 493 (48.7%) SARD-ILD. Idiopathic ILD patients displayed higher KL-6 values than SARD-ILD (p = 0.0002). FER and SMRP, though within normal ranges, were significantly higher in idiopathic ILD (p<0.0001). Logistic regression showed good sensitivity (69.4%) and specificity (80.4%) selecting the variables FER and KL-6 concentrations, age and gender-male correlated with a diagnosis of idiopathic ILD. Conclusion: Our study showed the excellent diagnostic value of KL-6 for detecting ILD, which irrespective of the final diagnosis and extent of disease, is always elevated and is a reliable biomarker of lung fibrosis in various diseases, ranging from idiopathic to autoimmune forms. Our study proposed an ILD differentiation model including clinical background. In this context, combination of serum markers and clinical data, as seen in our cohort, may lead to a further improvement in diagnostic accuracy for ILD. [ABSTRACT FROM AUTHOR]

Published

2024

2. Comparison of clinical features between patients with anti-synthetase syndrome and dermatomyositis: results from the MYONET registry.

Author

Hum, Ryan Malcolm, Lilleker, James B, Lamb, Janine A, Oldroyd, Alexander G S, Wang, Guochun, Wedderburn, Lucy R, Diederichsen, Louise P, Schmidt, Jens, Danieli, Maria Giovanna, Oakley, Paula, Griger, Zoltan, Phuong, Thuy Nguyen Thi, Kodishala, Chanakya, Mercado, Monica Vazquez-Del, Andersson, Helena, Paepe, Boel De, Bleecker, Jan L De, Maurer, Britta, McCann, Liza, and Pipitone, Nicolo

Subjects

DERMATOMYOSITIS, DIFFERENTIAL diagnosis, RESEARCH funding, RAYNAUD'S disease, SKIN diseases, MYOSITIS, EXFOLIATIVE dermatitis, AUTOANTIBODIES, EXANTHEMA, INTERSTITIAL lung diseases, ANTISYNTHETASE syndrome, ARTHRITIS, COMPARATIVE studies, TUMORS, DISEASE complications, SYMPTOMS, ADULTS

Abstract

Objectives To compare clinical characteristics, including the frequency of cutaneous, extramuscular manifestations and malignancy, between adults with anti-synthetase syndrome (ASyS) and DM. Methods Using data regarding adults from the MYONET registry, a cohort of DM patients with anti-Mi2/-TIF1γ/-NXP2/-SAE/-MDA5 autoantibodies, and a cohort of ASyS patients with anti-tRNA synthetase autoantibodies (anti-Jo1/-PL7/-PL12/-OJ/-EJ/-Zo/-KS) were identified. Patients with DM sine dermatitis or with discordant dual autoantibody specificities were excluded. Sub-cohorts of patients with ASyS with or without skin involvement were defined based on presence of DM-type rashes (heliotrope rash, Gottron's papules/sign, violaceous rash, shawl sign, V-sign, erythroderma, and/or periorbital rash). Results In total 1054 patients were included (DM, n  = 405; ASyS, n  = 649). In the ASyS cohort, 31% (n  = 203) had DM-type skin involvement (ASyS-DMskin). A higher frequency of extramuscular manifestations, including Mechanic's hands, Raynaud's phenomenon, arthritis, interstitial lung disease and cardiac involvement differentiated ASyS-DMskin from DM (all P  < 0.001), whereas higher frequency of any of four DM-type rashes—heliotrope rash (n  = 248, 61% vs n  = 90, 44%), violaceous rash (n  = 166, 41% vs n  = 57, 9%), V-sign (n  = 124, 31% vs n  = 28, 4%), and shawl sign (n  = 133, 33% vs n  = 18, 3%)—differentiated DM from ASyS-DMskin (all P  < 0.005). Cancer-associated myositis (CAM) was more frequent in DM (n  = 67, 17%) compared with ASyS (n  = 21, 3%) and ASyS-DMskin (n  = 7, 3%) cohorts (both P  < 0.001). Conclusion DM-type rashes are frequent in patients with ASyS; however, distinct clinical manifestations differentiate these patients from classical DM. Skin involvement in ASyS does not necessitate increased malignancy surveillance. These findings will inform future ASyS classification criteria and patient management. [ABSTRACT FROM AUTHOR]

Published

2024

3. Anti-transcription intermediary factor 1-gamma IgG2 isotype is associated with cancer in adult dermatomyositis: an ENMC multinational study.

Author

Cordel, Nadège, Dechelotte, Benoît, Jouen, Fabienne, Lamb, Janine A, Chinoy, Hector, New, Paul, Vencovsky, Jiri, Mann, Herman, Galindo-Feria, Angeles S, Dani, Lara, Selva-O'Callaghan, Albert, Werth, Victoria P, Ravishankar, Adarsh, Landon-Cardinal, Océane, Tressières, Benoit, and Boyer, Olivier

Subjects

TUMOR risk factors, AUTOANTIBODIES, DERMATOMYOSITIS, RETROSPECTIVE studies, GAMMA globulins, RISK assessment, IMMUNOASSAY, CANCER patients, ENZYME-linked immunosorbent assay, DESCRIPTIVE statistics, TRANSCRIPTION factors, TUMOR markers, CRYOPRESERVATION of organs, tissues, etc., CHEMICAL inhibitors, ADULTS

Abstract

Objective To assess the role of the anti-TIF1γ auto-antibody (aAb) IgG2 isotype as a biomarker of cancer in anti-TIF1γ aAb-positive adult DM. Methods International multicentre retrospective study with the following inclusion criteria: (i) diagnosis of DM according to ENMC criteria; (ii) presence of anti-TIF1γ IgG aAb determined using an in-house addressable laser bead immunoassay (ALBIA) from cryopreserved serums sampled at time of DM diagnosis and (iii) available baseline characteristics and follow-up data until the occurrence of cancer and/or a minimum follow-up of 1 year for patients without known cancer at diagnosis. Detection and quantification of anti-TIF1γ IgG2 aAb was done using the in-house ALBIA. In addition, a recent ELISA commercial kit was used for anti-TIF1γ IgG aAb quantification. Results A total of 132 patients (mean age 55±15 years) of whom 72 (54.5%) had an associated cancer were analysed. The association between the presence of cancer and the presence of anti-TIF1γ IgG2 aAb was statistically significant (P  = 0.026), with an OR of 2.26 (95% CI: 1.10, 4.76). Patients with cancer displayed significantly higher anti-TIF1γ IgG2 aAb ALBIA values with a median value of 1.15 AU/ml (IQR: 0.14–9.76) compared with 0.50 AU/ml (IQR: 0.14–1.46) for patients without cancer (P  = 0.042). In addition, patients with cancer displayed significantly higher anti-TIF1γ IgG aAb ELISA values with a median value of 127.5 AU/ml (IQR: 81.5–139.6) compared with 93.0 AU/ml (IQR: 54.0–132.9) for patients without cancer (P  = 0.004). Conclusion These results suggest considering anti-TIF1γ IgG2 ALBIA and IgG ELISA values as biomarkers of cancer in anti-TIF1 γ aAb-positive adult DM. [ABSTRACT FROM AUTHOR]

Published

2023

4. The Genetics of Autoimmune Myositis.

Author

Lamb, Janine A.

Subjects

GENETICS, INCLUSION body myositis, MYOSITIS, GENETIC variation, SOMATIC mutation, AMINO acid residues

Abstract

The idiopathic inflammatory myopathies (IIM) are rare, heterogeneous systemic autoimmune disorders, characterized by inflammation of skeletal muscle and multi-organ involvement. Studies to identify genetic risk factors and dysregulated gene expression in IIM aim to increase our understanding of disease pathogenesis. Genome-wide association studies have confirmed the HLA region as the most strongly associated region in IIM, with different associations between clinically-defined subgroups. Associated genes are involved in both the innate and adaptive immune response, while identification of variants reported in other autoimmune disorders suggests shared biological pathways. Targeted imputation analysis has identified key associated amino acid residues within HLA molecules that may influence antigen recognition. These amino acids increase risk for specific clinical phenotypes and autoantibody subgroups, and suggest that serology-defined subgroups may be more homogeneous. Recent data support the contribution of rare genetic variation to disease susceptibility in IIM, including mitochondrial DNA variation in sporadic inclusion body myositis and somatic mutations and loss of heterozygosity in cancer-associated myositis. Gene expression studies in skeletal muscle, blood and skin from individuals with IIM has confirmed the role of interferon signalling and other dysregulated pathways, and identified cell-type specific signatures. These dysregulated genes differentiate IIM subgroups and identify potential biomarkers. Here, we review recent genetic studies in IIM, and how these inform our understanding of disease pathogenesis and provide mechanistic insights into biological pathways. [ABSTRACT FROM AUTHOR]

Published

2022

5. Analysis of human total antibody repertoires in TIF1γ autoantibody positive dermatomyositis.

Author

Megremis, Spyridon, Walker, Thomas D. J., He, Xiaotong, O'Sullivan, James, Ollier, William E. R., Chinoy, Hector, Pendleton, Neil, Payton, Antony, Hampson, Lynne, Hampson, Ian, and Lamb, Janine A.

Subjects

AUTOANTIBODIES, DERMATOMYOSITIS, EPITOPES, POXVIRUSES, PROTEOMICS

Abstract

We investigate the accumulated microbial and autoantigen antibody repertoire in adult-onset dermatomyositis patients sero-positive for TIF1γ (TRIM33) autoantibodies. We use an untargeted high-throughput approach which combines immunoglobulin disease-specific epitope-enrichment and identification of microbial and human antigens. We observe antibodies recognizing a wider repertoire of microbial antigens in dermatomyositis. Antibodies recognizing viruses and Poxviridae family species are significantly enriched. The identified autoantibodies recognise a large portion of the human proteome, including interferon regulated proteins; these proteins cluster in specific biological processes. In addition to TRIM33, we identify autoantibodies against eleven further TRIM proteins, including TRIM21. Some of these TRIM proteins share epitope homology with specific viral species including poxviruses. Our data suggest antibody accumulation in dermatomyositis against an expanded diversity of microbial and human proteins and evidence of non-random targeting of specific signalling pathways. Our findings indicate that molecular mimicry and epitope spreading events may play a role in dermatomyositis pathogenesis. Megremis, Walker at al. identify immunogenic epitopes in dermatomyositis patients. They identify antibodies recognizing a wider diversity of microbial antigens including poxviruses, and autoantibodies recognizing a large portion of the human proteome. Shared epitope homology between viral and human proteins suggests that molecular mimicry and epitope spreading events may play a role in dermatomyositis pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

6. Antibodies against immunogenic epitopes with high sequence identity to SARS-CoV-2 in patients with autoimmune dermatomyositis.

Author

Megremis, Spyridon, Walker, Thomas D. J., Xiaotong He, Ollier, William E. R., Chinoy, Hector, Hampson, Lynne, Hampson, Ian, Lamb, Janine A., and He, Xiaotong

Published

2020

7. MicroRNA and mRNA profiling in the idiopathic inflammatory myopathies.

Author

Parkes, Joanna E., Thoma, Anastasia, Lightfoot, Adam P., Day, Philip J., Chinoy, Hector, and Lamb, Janine A.

Published

2020

8. Genetics of idiopathic inflammatory myopathies: insights into disease pathogenesis.

Author

Rothwell, Simon, Chinoy, Hector, and Lamb, Janine A.

Published

2019

9. Focused HLA analysis in Caucasians with myositis identifies significant associations with autoantibody subgroups.

Author

Rothwell, Simon, Chinoy, Hector, Lamb, Janine A., Miller, Frederick W., Rider, Lisa G., Wedderburn, Lucy R., McHugh, Neil J., Mammen, Andrew L., Betteridge, Zoe E., Tansley, Sarah L., Bowes, John, Vencovskk, Jiii, Deakin, Claire T., Dankk, Katalin, Vidya, Limaye, Selva-OOCallaghan, Albert, Pachman, Lauren M., Reed, Ann M., Molberg, -yvind, and Benveniste, Olivier

Abstract

Objectives: Idiopathic inflammatory myopathies (IIM) are a spectrum of rare autoimmune diseases characterised clinically by muscle weakness and heterogeneous systemic organ involvement. The strongest genetic risk is within the major histocompatibility complex (MHC). Since autoantibody presence defines specific clinical subgroups of IIM, we aimed to correlate serotype and genotype, to identify novel risk variants in the MHC region that co-occur with IIM autoantibodies.Methods: We collected available autoantibody data in our cohort of 2582 Caucasian patients with IIM. High resolution human leucocyte antigen (HLA) alleles and corresponding amino acid sequences were imputed using SNP2HLA from existing genotyping data and tested for association with 12 autoantibody subgroups.Results: We report associations with eight autoantibodies reaching our study-wide significance level of p<2.9×10-5. Associations with the 8.1 ancestral haplotype were found with anti-Jo-1 (HLA-B*08:01, p=2.28×10-53 and HLA-DRB1*03:01, p=3.25×10-9), anti-PM/Scl (HLA-DQB1*02:01, p=1.47×10-26) and anti-cN1A autoantibodies (HLA-DRB1*03:01, p=1.40×10-11). Associations independent of this haplotype were found with anti-Mi-2 (HLA-DRB1*07:01, p=4.92×10-13) and anti-HMGCR autoantibodies (HLA-DRB1*11, p=5.09×10-6). Amino acid positions may be more strongly associated than classical HLA associations; for example with anti-Jo-1 autoantibodies and position 74 of HLA-DRB1 (p=3.47×10-64) and position 9 of HLA-B (p=7.03×10-11). We report novel genetic associations with HLA-DQB1 anti-TIF1 autoantibodies and identify haplotypes that may differ between adult-onset and juvenile-onset patients with these autoantibodies.Conclusions: These findings provide new insights regarding the functional consequences of genetic polymorphisms within the MHC. As autoantibodies in IIM correlate with specific clinical features of disease, understanding genetic risk underlying development of autoantibody profiles has implications for future research. [ABSTRACT FROM AUTHOR]

Published

2019

10. The temporal relationship between cancer and adult onset anti-transcriptional intermediary factor 1 antibody–positive dermatomyositis.

Author

Oldroyd, Alexander, Sergeant, Jamie C, New, Paul, McHugh, Neil J, Betteridge, Zoe, Lamb, Janine A, Ollier, William E, Cooper, Robert G, and Chinoy, Hector

Subjects

TUMOR risk factors, AGE distribution, AGE factors in disease, AUTOANTIBODIES, CONFIDENCE intervals, DERMATOMYOSITIS, OVARIAN tumors, DISEASE incidence, PROPORTIONAL hazards models, KAPLAN-Meier estimator, ODDS ratio, DISEASE complications, DIAGNOSIS

Abstract

Objectives To characterize the 10 year relationship between anti-transcriptional intermediary factor 1 antibody (anti-TIF1-Ab) positivity and cancer onset in a large UK-based adult DM cohort. Methods Data from anti-TIF1-Ab-positive/-negative adults with verified diagnoses of DM from the UK Myositis Network register were analysed. Each patient was followed up until they developed cancer. Kaplan–Meier methods and Cox proportional hazard modelling were employed to estimate the cumulative cancer incidence. Results Data from 263 DM cases were analysed, with a total of 3252 person-years and a median 11 years of follow-up; 55 (21%) DM cases were anti-TIF1-Ab positive. After 10 years of follow-up, a higher proportion of anti-TIF1-Ab-positive cases developed cancer compared with anti-TIF1-Ab-negative cases: 38% vs 15% [hazard ratio 3.4 (95% CI 2.2, 5.4)]. All the detected malignancy cases in the anti-TIF1-Ab-positive cohort occurred between 3 years prior to and 2.5 years after DM onset. No cancer cases were detected within the following 7.5 years in this group, whereas cancers were detected during this period in the anti-TIF1-Ab-negative cases. Ovarian cancer was more common in the anti-TIF1-Ab-positive vs -negative cohort: 19% vs 2%, respectively (P < 0.05). No anti-TIF1-Ab-positive case <39 years of age developed cancer, compared with 21 (53%) of those ≥39 years of age. Conclusion Anti-TIF1-Ab-positive-associated malignancy occurs exclusively within the 3 year period on either side of DM onset, the risk being highest in those ≥39 years of age. Cancer types differ according to anti-TIF1-Ab status, and this may warrant specific cancer screening approaches. [ABSTRACT FROM AUTHOR]

Published

2019

11. Splicing variant of augments MDA5 signalling and the risk of clinically amyopathic dermatomyositis.

Author

Yuta Kochi, Yoichiro Kamatani, Yuya Kondo, Akari Suzuki, Eiryo Kawakami, Ryosuke Hiwa, Yukihide Momozawa, Manabu Fujimoto, Masatoshi Jinnin, Yoshiya Tanaka, Takashi Kanda, Cooper, Robert G., Chinoy, Hector, Rothwell, Simon, Lamb, Janine A., Vencovsky, Jiří, Mann, Heřman, Koichiro Ohmura, Keiko Myouzen, and Kazuyoshi Ishigaki

Subjects

ALLELES, APOPTOSIS, ASIANS, AUTOANTIBODIES, CELLULAR signal transduction, COMPARATIVE studies, DERMATOMYOSITIS, GENES, GENETIC polymorphisms, GENETIC techniques, RESEARCH methodology, MEDICAL cooperation, POLYMYOSITIS, PROTEINS, RESEARCH, RNA, DNA-binding proteins, EVALUATION research, CASE-control method, SIGNAL peptides, SEQUENCE analysis, GENOTYPES

Abstract

Objectives: Idiopathic inflammatory myopathies (IIMs) are a heterogeneous group of rare autoimmune diseases in which both genetic and environmental factors play important roles. To identify genetic factors of IIM including polymyositis, dermatomyositis (DM) and clinically amyopathic DM (CADM), we performed the first genome-wide association study for IIM in an Asian population.Methods: We genotyped and tested 496 819 single nucleotide polymorphism for association using 576 patients with IIM and 6270 control subjects. We also examined the causal mechanism of disease-associated variants by in silico analyses using publicly available data sets as well as by in in vitro analyses using reporter assays and apoptosis assays.Results: We identified a variant in WDFY4 that was significantly associated with CADM (rs7919656; OR=3.87; P=1.5×10-8). This variant had a cis-splicing quantitative trait locus (QTL) effect for a truncated WDFY4isoform (tr-WDFY4), with higher expression in the risk allele. Transexpression QTL analysis of this variant showed a positive correlation with the expression of NF-κB associated genes. Furthermore, we demonstrated that both WDFY4 and tr-WDFY4 interacted with pattern recognition receptors such as TLR3, TLR4, TLR9 and MDA5 and augmented the NF-κB activation by these receptors. WDFY4 isoforms also enhanced MDA5-induced apoptosis to a greater extent in the tr-WDFY4-transfected cells.Conclusions: As CADM is characterised by the appearance of anti-MDA5 autoantibodies and severe lung inflammation, the WDFY4 variant may play a critical role in the pathogenesis of CADM. [ABSTRACT FROM AUTHOR]

Published

2018

12. Genetics in inclusion body myositis.

Author

Rothwell, Simon, Lilleker, James B., and Lamb, Janine A.

Published

2017

13. New developments in genetics of myositis.

Author

Rothwell, Simon, Lamb, Janine A., and Chinoy, Hector

Published

2016

14. Molecular findings from 537 individuals with inherited retinal disease.

Author

Ellingford, Jamie M., Barton, Stephanie, Bhaskar, Sanjeev, O'Sullivan, James, Williams, Simon G., Lamb, Janine A., Panda, Binay, Sergouniotis, Panagiotis I., Gillespie, Rachel L., Daiger, Stephen P., Hall, Georgina, Gale, Theodora, Lloyd, I. Christopher, Bishop, Paul N., Ramsden, Simon C., and Black, Graeme C. M.

Abstract

Background Inherited retinal diseases (IRDs) are a clinically and genetically heterogeneous set of disorders, for which diagnostic second-generation sequencing (next-generation sequencing, NGS) services have been developed worldwide. Methods We present the molecular findings of 537 individuals referred to a 105-gene diagnostic NGS test for IRDs. We assess the diagnostic yield, the spectrum of clinical referrals, the variant analysis burden and the genetic heterogeneity of IRD. We retrospectively analyse disease-causing variants, including an assessment of variant frequency in Exome Aggregation Consortium (ExAC). Results Individuals were referred from 10 clinically distinct classifications of IRD. Of the 4542 variants clinically analysed, we have reported 402 mutations as a cause or a potential cause of disease in 62 of the 105 genes surveyed. These variants account or likely account for the clinical diagnosis of IRD in 51% of the 537 referred individuals. 144 potentially disease-causing mutations were identified as novel at the time of clinical analysis, and we further demonstrate the segregation of known disease-causing variants among individuals with IRD. We show that clinically analysed variants indicated as rare in dbSNP and the Exome Variant Server remain rare in ExAC, and that genes discovered as a cause of IRD in the post-NGS era are rare causes of IRD in a population of clinically surveyed individuals. Conclusions Our findings illustrate the continued powerful utility of custom-gene panel diagnostic NGS tests for IRD in the clinic, but suggest clear future avenues for increasing diagnostic yields. [ABSTRACT FROM AUTHOR]

Published

2016

15. Systematic protein-protein interaction and pathway analyses in the idiopathic inflammatory myopathies.

Author

Parkes, Joanna E., Rothwell, Simon, Day, Philip J., McHugh, Neil J., Betteridge, Zoë E., Cooper, Robert G., Ollier, William E., Chinoy, Hector, and Lamb, Janine A.

Published

2016

16. Disease specificity of autoantibodies to cytosolic 5'-nucleotidase 1A in sporadic inclusion body myositis versus known autoimmune diseases.

Author

Herbert, Megan K., Stammen-Vogelzangs, Judith, Verbeek, Marcel M., Rietveld, Anke, Lundberg, Ingrid E., Chinoy, Hector, Lamb, Janine A., Cooper, Robert G., Roberts, Mark, Badrising, Umesh A., De Bleecker, Jan L., Machado, Pedro M., Hanna, Michael G., Plestilova, Lenka, Vencovsky, Jiri, van Engelen, Baziel G., and Pruijn, Ger J. M.

Abstract

Objectives: The diagnosis of inclusion body myositis (IBM) can be challenging as it can be difficult to clinically distinguish from other forms of myositis, particularly polymyositis (PM). Recent studies have shown frequent presence of autoantibodies directed against cytosolic 5'-nucleotidase 1A (cN-1A) in patients with IBM. We therefore, examined the autoantigenicity and disease specificity of major epitopes of cN-1A in patients with sporadic IBM compared with healthy and disease controls.Methods: Serum samples obtained from patients with IBM (n=238), PM and dermatomyositis (DM) (n=185), other autoimmune diseases (n=246), other neuromuscular diseases (n=93) and healthy controls (n=35) were analysed for the presence of autoantibodies using immunodominant cN-1A peptide ELISAs.Results: Autoantibodies directed against major epitopes of cN-1A were frequent in patients with IBM (37%) but not in PM, DM or non-autoimmune neuromuscular diseases (<5%). Anti-cN-1A reactivity was also observed in some other autoimmune diseases, particularly Sjögren's syndrome (SjS; 36%) and systemic lupus erythematosus (SLE; 20%).Conclusions: In summary, we found frequent anti-cN-1A autoantibodies in sera from patients with IBM. Heterogeneity in reactivity with the three immunodominant epitopes indicates that serological assays should not be limited to a distinct epitope region. The similar reactivities observed for SjS and SLE demonstrate the need to further investigate whether distinct IBM-specific epitopes exist. [ABSTRACT FROM AUTHOR]

Published

2016

17. Response to: 'Similarities and differences between severe COVID-19 pneumonia and anti-MDA-5 positive dermatomyositis associated rapidly progressive interstitial lung diseases: a challenge for the future' by Wang et al.

Author

Lamb, Janine A., Megremis, Spyridon, and Chinoy, Hector

Published

2022

18. The role of microRNAs in the idiopathic inflammatory myopathies.

Author

Parkes, Joanna E., Day, Philip J., Chinoy, Hector, and Lamb, Janine A.

Published

2015

19. Bias in microRNA functional enrichment analysis.

Author

Bleazard, Thomas, Lamb, Janine A., and Griffiths-Jones, Sam

Subjects

MICRORNA, GENE expression, GENE targeting, HYPERGEOMETRIC distribution, GENETIC regulation

Abstract

Motivation: Many studies have investigated the differential expression of microRNAs (miRNAs) in disease states and between different treatments, tissues and developmental stages. Given a list of perturbed miRNAs, it is common to predict the shared pathways on which they act. The standard test for functional enrichment typically yields dozens of significantly enriched functional categories, many of which appear frequently in the analysis of apparently unrelated diseases and conditions. Results: We show that the most commonly used functional enrichment test is inappropriate for the analysis of sets of genes targeted by miRNAs. The hypergeometric distribution used by the standard method consistently results in significant P-values for functional enrichment for targets of randomly selected miRNAs, reflecting an underlying bias in the predicted gene targets of miRNAs as a whole. We developed an algorithm to measure enrichment using an empirical sampling approach, and applied this in a reanalysis of the gene ontology classes of targets of miRNA lists from 44 published studies. The vast majority of the miRNA target sets were not significantly enriched in any functional category after correction for bias. We therefore argue against continued use of the standard functional enrichment method for miRNA targets. [ABSTRACT FROM AUTHOR]

Published

2015

20. Strategies for Evaluating Idiopathic Inflammatory Myopathy Disease Susceptibility Genes.

Author

Rothwell, Simon, Cooper, Robert, Lamb, Janine, and Chinoy, Hector

Abstract

This review outlines the progress that has been made in understanding the genetics of the idiopathic inflammatory myopathies in the previous 2 years, with a particular focus on dermatomyositis and polymyositis. A recent genome-wide association study in dermatomyositis has confirmed the importance of the major histocompatibility region in this disease, and has suggested a shared genetic etiology with other autoimmune disorders. This has led to an ongoing study of additional immune-related loci using the Immunochip array. Candidate gene studies have identified novel risk associations in non-Europeans, such as STAT4 and HLA-DRB1 in the Japanese population. Evidence for gene-environment interactions has come from two recent studies implicating smoking status and statin use with HLA alleles. This review also touches on future approaches to genetic research in myositis, including bioinformatics tools to identify causal variants, HLA imputation from existing genetic data and statistical methods to investigate shared effects between subgroups of myositis. [ABSTRACT FROM AUTHOR]

Published

2014

21. Genome-Wide Association Study of Dermatomyositis Reveals Genetic Overlap With Other Autoimmune Disorders.

Author

Miller, Frederick W., Cooper, Robert G., Vencovský, Jiří, Rider, Lisa G., Danko, Katalin, Wedderburn, Lucy R., Lundberg, Ingrid E., Pachman, Lauren M., Reed, Ann M., Ytterberg, Steven R., Padyukov, Leonid, Selva‐O'Callaghan, Albert, Radstake, Timothy R. D. J., Isenberg, David A., Chinoy, Hector, Ollier, William E. R., O'Hanlon, Terrance P., Peng, Bo, Lee, Annette, and Lamb, Janine A.

Subjects

GENETICS of autoimmune diseases, DERMATOMYOSITIS, CONFIDENCE intervals, EPIDEMIOLOGY, GENES, GENETIC polymorphisms, MEDICAL cooperation, RESEARCH, RESEARCH funding, LOGISTIC regression analysis, GENOMICS, DATA analysis, CASE-control method, GENETICS

Abstract

Objective To identify new genetic associations with juvenile and adult dermatomyositis (DM). Methods We performed a genome-wide association study (GWAS) of adult and juvenile DM patients of European ancestry (n = 1,178) and controls (n = 4,724). To assess genetic overlap with other autoimmune disorders, we examined whether 141 single-nucleotide polymorphisms (SNPs) outside the major histocompatibility complex (MHC) locus, and previously associated with autoimmune diseases, predispose to DM. Results Compared to controls, patients with DM had a strong signal in the MHC region consisting of GWAS-level significance ( P < 5 × 10-8) at 80 genotyped SNPs. An analysis of 141 non-MHC SNPs previously associated with autoimmune diseases showed that 3 SNPs linked with 3 genes were associated with DM, with a false discovery rate (FDR) of <0.05. These genes were phospholipase C-like 1 ( PLCL1; rs6738825, FDR = 0.00089), B lymphoid tyrosine kinase ( BLK; rs2736340, FDR = 0.0031), and chemokine (C-C motif) ligand 21 ( CCL21; rs951005, FDR = 0.0076). None of these genes was previously reported to be associated with DM. Conclusion Our findings confirm the MHC as the major genetic region associated with DM and indicate that DM shares non-MHC genetic features with other autoimmune diseases, suggesting the presence of additional novel risk loci. This first identification of autoimmune disease genetic predispositions shared with DM may lead to enhanced understanding of pathogenesis and novel diagnostic and therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2013

22. Entering a new phase of immunogenetics in the idiopathic inflammatory myopathies.

Author

Rothwell, Simon, Cooper, Robert G, Lamb, Janine A, and Chinoy, Hector

Published

2013

23. Risk for myasthenia gravis maps to a 151Pro→Ala change in TNIP1 and to human leukocyte antigen-B*08.

Author

Gregersen, Peter K., Kosoy, Roman, Lee, Annette T., Lamb, Janine, Sussman, Jon, McKee, David, Simpfendorfer, Kim R., Pirskanen-Matell, Ritva, Piehl, Frederik, Pan-Hammarstrom, Qiang, Verschuuren, Jan J. G. M., Titulaer, Maarten J., Niks, Erik H., Marx, Alexander, Ströbel, Philipp, Tackenberg, Björn, Pütz, Michael, Maniaol, Angelina, Elsais, Ahmed, and Tallaksen, Chantal

Abstract

Objective: The objective of this study is to comprehensively define the genetic basis of early onset myasthenia gravis (EOMG). Methods: We have carried out a 2-stage genome-wide association study on a total of 649 North European EOMG patients. Cases were matched 1:4 with controls of European ancestry. We performed imputation and conditional analyses across the major histocompatibility complex, as well as in the top regions of association outside the human leukocyte antigen (HLA) region. Results: We observed the strongest association in the HLA class I region at rs7750641 ( p = 1.2 × 10−92; odds ratio [OR], 6.25). By imputation and conditional analyses, HLA-B*08 proves to be the major associated allele ( p = 2.87 × 10−113; OR, 6.41). In addition to the expected association with PTPN22 (rs2476601; OR, 1.71; p = 8.2 × 10−10), an imputed coding variant (rs2233290) at position 151 (Pro→Ala) in the TNFAIP3-interacting protein 1, TNIP1, confers even stronger risk than PTPN22 (OR, 1.91; p = 3.2 × 10−10). Interpretation: The association at TNIP1 in EOMG implies disease mechanisms involving ubiquitin-dependent dysregulation of NF-κB signaling. The localization of the major HLA signal to the HLA-B*08 allele suggests that CD8+ T cells may play a key role in disease initiation or pathogenesis. ANN NEUROL 2012; [ABSTRACT FROM AUTHOR]

Published

2012

24. Recent advances in the immunogenetics of idiopathic inflammatory myopathy.

Author

Chinoy, Hector, Lamb, Janine A., Ollier, William E. R., and Cooper, Robert G.

Published

2011

25. MET and autism susceptibility: family and case–control studies.

Author

Sousa, Inês, Clark, Taane G., Toma, Claudio, Kobayashi, Kazuhiro, Choma, Maja, Holt, Richard, Sykes, Nuala H., Lamb, Janine A., Bailey, Anthony J., Battaglia, Agatino, Maestrini, Elena, and Monaco, Anthony P.

Subjects

AUTISM, GENETIC polymorphisms, CHROMOSOMES, LINKAGE (Genetics), HUMAN genetics

Abstract

Autism is a common, severe and highly heritable neurodevelopmental disorder. The International Molecular Genetic Study of Autism Consortium (IMGSAC) genome screen for linkage in affected sib-pair families identified a chromosome 7q susceptibility locus (AUTS1), that has subsequently shown evidence of increased sharing in several independent multiplex samples and in two meta-analyses. Taking into account the location of the MET gene under this linkage peak, and the fact that it has recently been reported to be associated with autism, the gene was further analyzed as a promising autism candidate. The gene encodes a transmembrane receptor tyrosine kinase of the hepatocyte growth factor/scatter factor (HGF/SF). MET is best known as an oncogene, but its signalling also participates in immune function, peripheral organ development and repair, and the development of the cerebral cortex and cerebellum (all of which have been observed earlier as being disregulated in individuals with autism). Here we present a family-based association analysis covering the entire MET locus. Significant results were obtained in both single locus and haplotype approaches with a single nucleotide polymorphism in intron 1 (rs38845, P<0.004) and with one intronic haplotype (AAGTG, P<0.009) in 325 multiplex IMGSAC families and 10 IMGSAC trios. Although these results failed to replicate in an independent sample of 82 Italian trios, the association itself was confirmed by a case–control analysis performed using the Italian cohort (P<0.02). The previously reported positive association of rs1858830 failed to replicate in this study. Overall, our findings provide further evidence that MET may play a role in autism susceptibility.European Journal of Human Genetics (2009) 17, 749–758; doi:10.1038/ejhg.2008.215; published online 12 November 2008 [ABSTRACT FROM AUTHOR]

Published

2009

26. Genetic susceptibility to Keloid scarring: SMAD gene SNP frequencies in Afro-Caribbeans.

Author

Brown, Jason J., Ollier, William, Arscott, Guyan, Xiayi Ke, Lamb, Janine, Day, Philip, and Bayat, Ardeshir

Subjects

EXPERIMENTAL dermatology, GENES, DIAGNOSIS, BIOMARKERS, GENETIC markers

Abstract

Keloid disease (KD) is a fibroproliferative dermal tumour of unknown aetiology. The increased familial clustering in KD, its increased prevalence in certain races and increased concordance in identical twins suggest a strong genetic predisposition to keloid formation. The highest incidence of keloids is found in the black population, where it has been estimated around 4–6% and up to 16% in random samples of black Africans. SMAD genes 3, 6 and 7 were investigated as candidate genes in Jamaican patients with keloid scars ( n = 183) and a matched control population ( n = 121) because of their previously reported involvement in fibrotic disorders and to determine if they were associated with keloid disease susceptibility. Thirty Five SNPs across these genes were genotyped using Time-of-Flight Mass Spectrometry (MALDI-TOF MS) and iPLEX assay. Linkage disequilibrium (LD) was established between several of the SNPs investigated. In the Jamaican population, the SMAD SNPs investigated for this study were not strongly associated with increased risk of developing KD. Identification of genetic markers in candidate genes such as the SMAD family may be of significant importance in diagnosis, prognosis and development of new therapies in the management of keloid scarring. [ABSTRACT FROM AUTHOR]

Published

2008

27. Mutation screening and association analysis of six candidate genes for autism on chromosome 7q.

Author

Bonora, Elena, Lamb, Janine A., Barnby, Gabrielle, Sykes, Nuala, Moberly, Thomas, Beyer, Kim S., Klauck, Sabine M., Poustka, Firtz, Bacchelli, Elena, Blasi, Francesca, Maestrini, Elena, Battaglia, Agatino, Haracopos, Demetrios, Pedersen, Lennart, Isager, Torben, Eriksen, Gunna, Viskum, Birgitte, Sorensen, Ester-Ulsted, Brondum-Nielsen, Karen, and Cotterill, Rodney

Subjects

GENETIC polymorphisms, DEVELOPMENTAL disabilities, AUTISM, HUMAN biology, SIBLINGS, CELL nuclei

Abstract

Genetic studies have provided evidence for an autism susceptibility locus (AUTS1) on chromosome 7q. Screening for mutations in six genes mapping to 7q, CUTL1, SRPK2, SYPL, LAMB1, NRCAM and PTPRZ1 in 48 unrelated individuals with autism led to the identification of several new coding variants in the genes CUTL1, LAMB1 and PTPRZ1. Analysis of genetic variants provided evidence for association with autism for one of the new missense changes identified in LAMB1; this effect was stronger in a subgroup of affected male sibling pair families, implying a possible specific sex-related effect for this variant. Association was also detected for several polymorphisms in the promoter and untranslated region of NRCAM, suggesting that alterations in expression of this gene may be linked to autism susceptibility.European Journal of Human Genetics (2005) 13, 198-207. doi:10.1038/sj.ejhg.5201315 Published online 3 November 2004 [ABSTRACT FROM AUTHOR]

Published

2005

28. Autism.

Author

Lamb, Janine, Parr, Jeremy, Bailey, Anthony, and Monaco, Anthony

Abstract

Autism is a neurodevelopmental disorder of unknown etiology. There is convincing data for the involvement of genetic factors in the development of autism, and the absence of any consistent evidence for an environmental, neuroanatomical, or biochemical cause has led to an increasing number of genetic studies to determine the basis of this complex disorder. The results of recent genetic linkage and candidate gene studies are reviewed in relation to the challenge of clinical and genetic heterogeneity, and prospects for the future of genetic research in autism are considered. [ABSTRACT FROM AUTHOR]

Published

2002

29. Comment on: The temporal relationship between cancer and adult onset anti-transcriptional intermediary factor 1 antibody–positive dermatomyositis: Reply.

Author

Oldroyd, Alexander, Sergeant, Jamie C, New, R Paul, McHugh, Neil J, Betteridge, Zoe, Lamb, Janine A, Ollier, William E, Cooper, Robert G, and Chinoy, Hector

Subjects

BREAST tumor diagnosis, TUMOR risk factors, AGE factors in disease, AUTOANTIBODIES, BREAST tumors, COMPUTED tomography, DERMATOMYOSITIS, MYOSITIS, OVARIAN tumors, POSITRON emission tomography, DISEASE incidence, DISEASE duration, EARLY detection of cancer, DISEASE complications

Abstract

The authors convey their response to a feedback about their report on cancer risk in anti-transcriptional intermediary factor 1 antibody (anti-TIF1-Ab)-positive dermatomyositis (DM). Topics mentioned include the need for focused cancer screening in anti-TIF1-Ab-positive patients, how cancer screening should be carried out, and the significance of vigilance of cancer-related symptoms and repeated cancer screening within the three years after DM onset.

Published

2019

30. Investigation of myositis and scleroderma specific autoantibodies in patients with lung cancer.

Author

Betteridge, Zoe E., Priest, Lynsey, Cooper, Robert G., McHugh, Neil J., Blackhall, Fiona, and Lamb, Janine A.

Published

2018

31. Genetic background may contribute to the latitude-dependent prevalence of dermatomyositis and anti-TIF1-γ autoantibodies in adult patients with myositis.

Author

Parkes, Joanna E., Rothwell, Simon, Oldroyd, Alexander, Chinoy, Hector, Lamb, Janine A., and The Myositis Genetics Consortium (MYOGEN)

Published

2018

32. Autism: recent molecular genetic advances.

Author

Lamb, Janine A.

Abstract

Focuses on molecular investigations to identify susceptibility loci implicated in autistic disorder. Cytogenetic studies and chromosomal abnormalities in autism; Candidate gene studies in autism; Genetic linkage studies of autism.

Published

2000