Your search keyword '"Mammen, Andrew"' showing total 48 results

1. Distinct Transcript‐Level Expression Profiles and Unique Alternative Splicing in Inflammatory Myopathies.

Author

Najjar, Rayan, Alessi, Hugh, Pinal‐Fernandez, Iago, Mammen, Andrew L., and Mustelin, Tomas

Subjects

RNA analysis, DERMATOMYOSITIS, BIOPSY, MYOSITIS, SKELETAL muscle, RESEARCH funding, INCLUSION body myositis, AUTOANTIBODIES, STATISTICAL sampling, DESCRIPTIVE statistics, GENE expression, CONFIDENCE intervals, SEQUENCE analysis

Abstract

Objective: The pathogenesis of inflammatory myopathies is poorly understood and there is a need to dissect the transcriptome in more granular ways beyond gene expression. Methods: We used a set of muscle RNA‐sequencing data from different myositis subtypes grouped by their specific autoantibodies (n = 152). We quantified annotated RNA transcripts for each myositis subtype and identified uniquely expressed RNA as well as transcriptional similarities among myositis types. In addition, we quantified event‐based alternative splicing with predicted protein changes. And finally, we searched for cryptic exons. Results: We saw considerable overlap in RNA expression among subtypes. In addition, MADCAM1 was previously shown to be uniquely expressed in Mi‐2 myositis; we discovered it was two noncanonical transcripts that predominantly contributed to the observed increased expression. At the transcriptional level, dermatomyositis subtypes were least similar to inclusion body myositis (IBM) or Jo1, followed by HMGCR, then SRP and other dermatomyositis subtype. Additionally, we discovered many alternative splicing events that were unique by myositis subgroup, including events in muscle dystrophy genes and one event in SRP72, which was seen uniquely in SRP myositis. Finally, we looked for previously reported cryptic exons in IBM and did not find them. Conclusion: The large degree of transcriptional overlap among myositis subtypes reinforces the need to use disease (in addition to healthy) controls to find unique features of autoimmune disease. Unique alterations in the transcriptome that are seen in one myositis subtype and not others advance our understanding of distinct disease pathology. [ABSTRACT FROM AUTHOR]

Published

2024

2. Myositis‐Associated Autoantibodies in Patients With Juvenile Myositis Are Associated With Refractory Disease and Mortality.

Author

Sherman, Matthew A., Noroozi Farhadi, Payam, Pak, Katherine, Trieu, Edward P., Sarkar, Kakali, Targoff, Ira N., Neely, Megan L., Mammen, Andrew L., Rider, Lisa G., Albert, Daniel A., Arabshahi, Bita, Ardalan, Kaveh, Baer, Alan N., Balboni, Imelda M., Ballinger, Susan H., Bayat, Nastaran, Becker, Mara L., April Bingham, C., Bohnsack, John F., and Cartwright, Victoria W.

Subjects

CROSS-sectional method, MORTALITY, DERMATOMYOSITIS, MYOSITIS, RAYNAUD'S disease, RESEARCH funding, AUTOANTIBODIES, MULTIPLE regression analysis, ENZYME-linked immunosorbent assay, SEVERITY of illness index, INTERSTITIAL lung diseases, LONGITUDINAL method, ODDS ratio, CHRONIC diseases, COMPARATIVE studies, CONFIDENCE intervals, PRECIPITIN tests, IMMUNOBLOTTING

Abstract

Objective: Myositis‐associated autoantibodies (MAAs) have been associated with overlap myositis, certain disease manifestations such as interstitial lung disease (ILD), and worse prognosis in the idiopathic inflammatory myopathies. MAAs overall remain largely uncharacterized in patients with juvenile‐onset myositis. Moreover, it is unknown whether the number of MAAs is associated with disease severity. Methods: Patients with juvenile myositis in cross‐sectional natural history studies who underwent testing for myositis autoantibodies were included. Demographics, myositis autoantibodies, clinical characteristics, medications received, and outcomes of those with and without MAAs were compared. Multivariable logistic regression was performed to determine whether the number of MAAs detected was associated with severe disease features. Results: Among 551 patients, 36% had an MAA and 13% had more than one MAA. Among those who were MAA positive, there was a higher frequency of overlap myositis (18% vs 5.9%, P < 0.001). MAA positivity was associated with certain clinical features, including Raynaud phenomenon (odds ratio [OR] 2.44, 95% confidence interval [CI] 1.41–4.28) and ILD (OR 3.43, 95% CI 1.75–6.96), as well as a chronic disease course (OR 1.72, 95% CI 1.10–2.72) and mortality (OR 3.76, 95% CI 1.72–8.43). The number of MAAs was also associated with mortality (OR 1.83, 95% CI 1.16–2.86). Conclusion: MAAs were prevalent in a large cohort of patients with juvenile myositis. ILD, refractory disease, and mortality were associated with MAA positivity. Prospective studies are needed to determine whether early detection of MAAs may lead to improved outcomes for patients with juvenile myositis. [ABSTRACT FROM AUTHOR]

Published

2024

3. Clinical Features and Immunogenetic Risk Factors Associated With Additional Autoantibodies in Anti‐Transcriptional Intermediary Factor 1γ Juvenile‐Onset Dermatomyositis.

Author

Sherman, Matthew A., Yang, Qingyuan, Gutierrez‐Alamillo, Laura, Pak, Katherine, Flegel, Willy A., Mammen, Andrew L., Rider, Lisa G., Casciola‐Rosen, Livia A., Arabshahi, Bita, Ballinger, Susan, April Bingham, C., Bohnsack, John F., Carrasco, Ruy, Anne Eberhardt, B., Edelheit, Barbara S., Farhadi, Payam Noroozi, Finkel, Terri H., Fuhlbrigge, Robert C., Goldmuntz, Ellen A., and Gottlieb, Beth S.

Subjects

TUMOR risk factors, DERMATOMYOSITIS, IMMUNOGENETICS, RISK assessment, CROSS-sectional method, AUTOANTIBODIES, LOGISTIC regression analysis, TRANSCRIPTION factors, DESCRIPTIVE statistics, CHI-squared test, MANN Whitney U Test, AGE factors in disease, LONGITUDINAL method, ODDS ratio, CONFIDENCE intervals, FACTOR analysis, HLA-B27 antigen, BIOMARKERS, GENOTYPES, ADULTS

Abstract

Objective: Novel autoantibody specificities including anti‐CCAR1 were recently discovered in adult patients with anti‐transcriptional intermediary factor (TIF1)–positive dermatomyositis (DM) and were associated with attenuated cancer emergence. The aims of the present study were to examine whether these autoantibodies occur in patients with juvenile‐onset DM (JDM) and to determine their associated features. Methods: Sera from 150 patients with anti‐TIF1γ autoantibody‐positive JDM in a cross‐sectional cohort and 90 juvenile healthy controls were assayed for anti‐CCAR1, anti‐C1Z1, anti‐IMMT, anti‐TBL1XR1, and anti‐Sp4 autoantibodies. Demographics, myositis autoantibodies, clinical features, medications, outcomes, and HLA‐DRB1 and HLA‐DQA1 alleles were compared between those with and without these autoantibodies. Results: Any one of the anti‐TIF1γ‐associated autoantibodies was present in 44 patients (29%) overall, including 25 (17%) with anti‐Sp4, 22 (15%) with anti‐TBL1XR1, 14 (9%) with anti‐CCAR1, 2 (1%) with anti‐C1Z1, and 2 (1%) with anti‐IMMT autoantibodies. These anti‐TIF1γ‐associated autoantibodies frequently co‐occurred. Patients with any of the anti‐TIF1γ‐associated autoantibodies had less frequent falling (34% [15] vs. 53% [56], P = 0.032) and lower peak muscle enzymes. None of the patients had cancer. Among White patients, HLA‐DRB1*03 was protective against an anti‐TIF1γ‐associated autoantibody (odds ratio 0.20, 95% confidence interval 0.07–0.52). Conclusion: Autoantibodies associated with anti‐TIF1γ were found in isolation and in combination among a subset of patients with JDM. Patients with these autoantibodies had less severe muscle disease and were not enriched for HLA‐DRB1*03. Additional autoantibodies among patients with positive anti‐TIF1γ with JDM likely contribute to the heterogeneity of the anti‐TIF1γ serologic subgroup. [ABSTRACT FROM AUTHOR]

Published

2024

4. Diagnostic Yield of Computed Tomography for Cancer Detection in a Tertiary Referral Population of Idiopathic Inflammatory Myositis Patients.

Author

Mecoli, Christopher A., Chee, Brant, Chen, Mengkun, Wang, XingYao, Albayda, Jemima, Paik, Julie J., Tiniakou, Eleni, Adler, Brittany, Kelly, Will, Mammen, Andrew L., Platz, Elizabeth A., Casciola‐Rosen, Livia, Christopher‐Stine, Lisa, and Shah, Ami A.

Subjects

EARLY detection of cancer, COMPUTED tomography, MYOSITIS, DERMATOMYOSITIS, CANCER diagnosis, PELVIS, AUTOANTIBODIES

Abstract

Objective: To inform guidance for cancer detection in patients with idiopathic inflammatory myopathy (IIM), we evaluated the diagnostic yield of computed tomography (CT) imaging for cancer screening/surveillance within distinct IIM subtypes and myositis‐specific autoantibody strata. Methods: We conducted a single‐center, retrospective cohort study in IIM patients. Overall diagnostic yield (number of cancers diagnosed/number of tests performed), percentage of false positives (number of biopsies performed not leading to cancer diagnosis/number of tests performed), and test characteristics were determined on CT of the chest and abdomen/pelvis. Results: Within the first 3 years since IIM symptom onset, a total of 9 of 1,011 (0.9%) chest CT scans and 12 of 657 (1.8%) abdomen/pelvis CT scans detected cancer. Diagnostic yields for both CT of the chest and CT of the abdomen/pelvis were highest in dermatomyositis, specifically anti–transcription intermediary factor 1γ (2.9% and 2.4% for CT of the chest and abdomen/pelvis, respectively). The highest percentage of false positives was in patients with antisynthetase syndrome (ASyS) (4.4%) and immune‐mediated necrotizing myopathy (4.4%) on CT of the chest, and ASyS (3.8%) on CT of the abdomen/pelvis. Patients ages <40 years old at IIM onset had both low diagnostic yields (0% and 0.5%) and high false‐positive rates (1.9% and 4.4%) for CT of the chest and abdomen/pelvis, respectively. Conclusion: In a tertiary referral cohort of IIM patients, CT imaging has a wide range of diagnostic yield and frequency of false positives for contemporaneous cancer. These findings suggest that cancer detection strategies targeted according to IIM subtype, autoantibody positivity, and age may maximize cancer detection while minimizing the harms and costs of over‐screening. [ABSTRACT FROM AUTHOR]

Published

2023

5. Autoantibodies Recognizing Specificity Protein 4 Co‐occur With Anti–Transcription Intermediary Factor 1 and Are Associated With Distinct Clinical Features and Immunogenetic Risk Factors in Juvenile Myositis.

Author

Sherman, Matthew A., Pak, Katherine, Pinal‐Fernandez, Iago, Flegel, Willy A., Targoff, Ira N., Miller, Frederick W., Rider, Lisa G., Mammen, Andrew L., Albert, Daniel A., Arabshahi, Bita, Balboni, Imelda M., Ballinger, Susan, Bayat, Nastaran, Bingham, C. April, Bohnsack, John F., Cartwright, Victoria W., Cron, Randy Q., Curiel, Rodolfo, de la Pena, Wendy, and de Guzman, Marietta M.

Subjects

AUTOANTIBODIES, PROTEINS, RISK assessment, DISEASE susceptibility, DESCRIPTIVE statistics, RESEARCH funding, MYOSITIS, TRANSCRIPTION factors, AMINOTRANSFERASES, PHENOTYPES, DISEASE risk factors, CHILDREN, ADOLESCENCE

Abstract

Objective: Autoantibodies recognizing specificity protein 4 (Sp4) were recently discovered in adults with idiopathic inflammatory myopathies (IIM). Anti‐Sp4 autoantibodies co‐occurred in patients with anti–transcription intermediary factor 1 (anti‐TIF1) autoantibody‐positive dermatomyositis (DM) and were associated with a reduced risk of cancer. In the present study, the prevalence and clinical features associated with anti‐Sp4 autoantibodies in juvenile‐onset IIM were investigated. Methods: Serum samples from 336 patients with juvenile myositis in a cross‐sectional cohort and 91 healthy controls were screened for anti‐Sp4 autoantibodies using enzyme‐linked immunosorbent assay. Clinical characteristics, outcomes, and HLA alleles of those with and those without anti‐Sp4 autoantibodies were compared. Results: Anti‐Sp4 autoantibodies were present in 23 patients (7%) with juvenile myositis and were not present in any of the controls. Anti‐Sp4 autoantibodies were found among each clinical myositis subgroup. The frequency of TIF1 autoantibody positivity was significantly higher among those with anti‐Sp4 autoantibodies (21 [91%] versus 92 [30%], P < 0.001). In the anti‐TIF1 autoantibody–positive subgroup, Raynaud's phenomenon (8 [38%] versus 2 [2%], P < 0.001) was more common and peak aspartate aminotransferase was significantly lower in those with anti‐Sp4 autoantibodies. None of the patients with anti‐Sp4 autoantibodies required a wheelchair. Among White patients, DQA1*04 and DRB1*08 were associated with anti‐Sp4 autoantibodies. Conclusion: Anti‐Sp4 autoantibodies were found in patients with juvenile‐onset IIM, predominantly those with coexisting anti‐TIF1 autoantibodies. Patients with anti‐Sp4 autoantibodies represent a phenotypic subset of anti‐TIF1 autoantibody–positive myositis characterized by frequent Raynaud's phenomenon and less pronounced muscle involvement, similar to adults with these autoantibodies. Novel immunogenetic risk factors for White patients with IIM were identified among juveniles with anti‐Sp4 autoantibodies. [ABSTRACT FROM AUTHOR]

Published

2023

6. Association of Anti‐CCAR1 Autoantibodies With Decreased Cancer Risk Relative to the General Population in Patients With Anti–Transcriptional Intermediary Factor 1γ–Positive Dermatomyositis.

Author

Fiorentino, David, Mecoli, Christopher A., Igusa, Tak, Albayda, Jemima, Paik, Julie J., Tiniakou, Eleni, Adler, Brittany, Mammen, Andrew L., Shah, Ami A., Rosen, Antony, Christopher‐Stine, Lisa, and Casciola‐Rosen, Livia

Subjects

BLOOD serum analysis, TUMOR risk factors, AUTOANTIBODIES, RESEARCH, DERMATOMYOSITIS, CONFIDENCE intervals, CELL cycle proteins, APOPTOSIS, DISEASE incidence, RISK assessment, CELL division, SYMPTOMS, ENZYME-linked immunosorbent assay, DESCRIPTIVE statistics, TRANSCRIPTION factors, STATISTICAL correlation, PHENOTYPES

Abstract

Objective: To describe the disease specificity, clinical phenotype, and risk of cancer in dermatomyositis (DM) patients with autoantibodies against cell division cycle and apoptosis regulator protein 1 (anti‐CCAR1). Methods: The frequency of anti‐CCAR1 autoantibodies was measured by enzyme‐linked immunosorbent assay in the serum of DM patients from 2 independent cohorts (Johns Hopkins and Stanford), with patients with several other rheumatic diseases and healthy controls used as comparators. Clinical features and the risk of cancer incidence relative to that in the general population were determined in anti‐CCAR1–positive DM patients. Results: Anti‐CCAR1 antibodies were significantly associated with anti–transcriptional intermediary factor 1γ (anti‐TIF1γ) antibodies present in the serum of patients with DM: 80 (32%) of 252 anti‐TIF1γ–positive DM patients versus 14 (8%) of 186 anti‐TIF1γ–negative DM patients were positive for anti‐CCAR1 antibodies (P < 0.001). Anti‐CCAR1 antibodies were not detected in any of the 32 serum samples from healthy controls, and were present at very low frequencies in the sera of patients with other rheumatic diseases: 1 (2.3%) of 44 patients with anti–hydroxymethylglutaryl‐coenzyme A reductase–positive necrotizing myopathy, 1 (2.3%) of 44 patients with inclusion body myositis, and 3 (6.5%) of 46 patients with systemic lupus erythematosus were positive for anti‐CCAR1 antibodies. Upon examining data on occurrence of cancer from the onset of DM onward, the observed number of cancers diagnosed in anti–TIF‐1γ–positive DM patients was significantly greater than expected in both cohorts, with a standardized incidence ratio (SIR) of 3.49 (95% confidence interval [95% CI] 2.39–4.92) in the Johns Hopkins cohort and a SIR of 4.54 (95% CI 3.04–6.52) in the Stanford cohort (each P < 0.001). DM patients who were both anti‐TIF1γ positive and anti‐CCAR1 positive had lower SIRs for cancer, with a SIR of 1.78 (95% CI 0.77–3.51) (P = 0.172) in the Johns Hopkins cohort and a SIR of 1.61 (95% CI 0.44–4.13) (P = 0.48) in the Stanford cohort. Conclusion: Anti‐CCAR1 autoantibodies are specific for anti‐TIF1γ–positive DM. Their presence in anti‐TIF1γ–positive patients attenuates the risk of cancer to a level comparable to that seen in the general population. [ABSTRACT FROM AUTHOR]

Published

2023

7. Subsets of Idiopathic Inflammatory Myositis Enriched for Contemporaneous Cancer Relative to the General Population.

Author

Mecoli, Christopher A., Igusa, Tak, Chen, Mengkun, Wang, XingYao, Albayda, Jemima, Paik, Julie J., Tiniakou, Eleni, Adler, Brittany, Richardson, Carrie, Kelly, Will, Danoff, Sonye, Mammen, Andrew L., Platz, Elizabeth A., Rosen, Antony, Christopher‐Stine, Lisa, Casciola‐Rosen, Livia, and Shah, Ami A.

Subjects

TUMOR risk factors, AUTOANTIBODIES, PUBLIC health surveillance, CONFIDENCE intervals, DERMATOMYOSITIS, RETROSPECTIVE studies, PRECIPITIN tests, RISK assessment, ENZYME-linked immunosorbent assay, MYOSITIS, TRANSCRIPTION factors, LONGITUDINAL method, DISEASE complications

Abstract

Objective: This study investigates cancer risk in idiopathic inflammatory myopathy (IIM) relative to the general population. Methods: We conducted a single‐center, retrospective cohort study of IIM patients and malignancy. Myositis‐specific and ‐associated autoantibodies were determined by Euroimmun line blot, enzyme‐linked immunosorbent assay, and immunoprecipitation. We calculated standardized prevalence ratios (SPRs) and adjusted for calendar year, age, sex, race, and ethnicity by comparing observed cancers in IIM patients versus expected cancers in the general population using the Surveillance, Epidemiology, and End Results registry. Results: Of 1,172 IIM patients, 203 (17%) patients with a cancer history were studied. Over a median follow‐up of 5.2 years, the observed number of IIM patients diagnosed with cancer was increased 1.43‐fold (SPR 1.43 [95% confidence interval (95% CI) 1.15–1.77]; P = 0.002). Within 3 years of IIM symptom onset, an increased SPR was observed for anti–transcription intermediary factor 1γ (anti‐TIF1γ)–positive patients for ovarian and breast cancer (ovarian SPR 18.39 [95% CI 5.01–47.08], P < 0.001; breast SPR 3.84 [95% CI 1.99–6.71], P < 0.001). As expected, anti‐TIF1γ positivity was associated with a significantly elevated SPR; however, only 55% (36 of 66) of all cancers within 3 years of dermatomyositis onset were observed in anti‐TIF1γ–positive patients. Other myositis‐specific autoantibodies, including anti–Mi‐2, anti–small ubiquitin‐like modifier activating enzyme (SAE), and anti‐nuclear matrix protein 2 (NXP‐2), accounted for 26% (17 of 66) of cancers diagnosed within 3 years of dermatomyositis onset. No cancer association, positive or negative, was observed for patients with antisynthetase, anti–melanoma differentiation–associated protein 5 (anti–MDA‐5), or anti–hydroxymethylglutaryl‐coenzyme A reductase (anti‐HMGCR) antibodies. Conclusion: In a tertiary referral center population, anti‐TIF1γ was most strongly associated with breast and ovarian cancer. Patients with antisynthetase, anti–MDA‐5, or anti‐HMGCR antibodies had the same cancer risk as the general population. [ABSTRACT FROM AUTHOR]

Published

2023

8. Muscle Transcriptomics Shows Overexpression of Cadherin 1 in Inclusion Body Myositis.

Author

Ikenaga, Chiseko, Date, Hidetoshi, Kanagawa, Motoi, Mitsui, Jun, Ishiura, Hiroyuki, Yoshimura, Jun, Pinal‐Fernandez, Iago, Mammen, Andrew L., Lloyd, Thomas E., Tsuji, Shoji, Shimizu, Jun, Toda, Tatsushi, and Goto, Jun

Subjects

INCLUSION body myositis, POLYMYOSITIS, CELL adhesion molecules, RNA sequencing, IMMUNOSTAINING, MAJOR histocompatibility complex, MYOBLASTS

Abstract

Objective: This study aimed to elucidate the molecular features of inclusion body myositis (IBM). Methods: We performed RNA sequencing analysis of muscle biopsy samples from 67 participants, consisting of 58 myositis patients with the pathological finding of CD8‐positive T cells invading non‐necrotic muscle fibers expressing major histocompatibility complex class I (43 IBM, 6 polymyositis, and 9 unclassifiable myositis), and 9 controls. Results: Cluster analysis, principal component analysis, and pathway analysis showed that differentially expressed genes and pathways identified in IBM and polymyositis were mostly comparable. However, pathways related to cell adhesion molecules were upregulated in IBM as compared with polymyositis and controls (p < 0.01). Notably, CDH1, which encodes the epidermal cell junction protein cadherin 1, was overexpressed in the muscles of IBM, which was validated by another RNA sequencing dataset from previous publications. Western blotting confirmed the presence of mature cadherin 1 protein in the muscles of IBM. Immunohistochemical staining confirmed the positivity for anti‐cadherin 1 antibody in the muscles of IBM, whereas there was no muscle fiber positive for anti‐cadherin 1 antibody in immune‐mediated necrotizing myopathy, antisynthetase syndrome, and controls. The fibers stained with anti‐cadherin 1 antibody did not have rimmed vacuoles or abnormal protein accumulation. Experimental skeletal muscle regeneration and differentiation systems showed that CDH1 is expressed during skeletal muscle regeneration and differentiation. Interpretation: CDH1 was detected as a differentially expressed gene, and immunohistochemistry showed that cadherin 1 exists in the muscles of IBM, whereas it was rarely seen in those of other idiopathic inflammatory myopathies. Cadherin 1 upregulation in muscle could provide a valuable clue to the pathological mechanisms of IBM. ANN NEUROL 2022;91:317–328 [ABSTRACT FROM AUTHOR]

Published

2022

9. Performance of the 2017 European Alliance of Associations for Rheumatology/American College of Rheumatology Classification Criteria for Idiopathic Inflammatory Myopathies in Patients With Myositis‐Specific Autoantibodies.

Author

Casal‐Dominguez, Maria, Pinal‐Fernandez, Iago, Pak, Katherine, Huang, Wilson, Selva‐O'Callaghan, Albert, Albayda, Jemima, Casciola‐Rosen, Livia, Paik, Julie J., Tiniakou, Eleni, Mecoli, Christopher A., Lloyd, Thomas E., Danoff, Sonye K., Christopher‐Stine, Lisa, and Mammen, Andrew L.

Subjects

AUTOANTIBODIES, STATISTICS, INCLUSION body myositis, MUSCLES, CLASSIFICATION, PATIENTS, REGRESSION analysis, FACTOR analysis, DESCRIPTIVE statistics, MYOSITIS, SENSITIVITY & specificity (Statistics), DATA analysis, OXIDOREDUCTASES, PHENOTYPES

Abstract

Objective: We undertook this study to 1) determine the sensitivity of the European Alliance of Associations for Rheumatology (EULAR)/American College of Rheumatology (ACR) classification criteria for idiopathic inflammatory myopathies (IIMs) to properly classify myositis‐specific autoantibody (MSA)–positive myositis patients, 2) describe the phenotype and muscle involvement over time in different MSA‐positive patients, and 3) compare MSA subgroups to EULAR/ACR criteria–defined myositis subgroups for their capacity to predict clinical phenotypes in patients with IIMs. Methods: The study included 524 MSA‐positive myositis patients from the Johns Hopkins Myositis Center. Each patient was classified using the EULAR/ACR classification criteria. Patient phenotypes were summarized using factor analysis of mixed data (FAMD). We compared the ability of MSAs to that of the EULAR/ACR classification subgroups to predict the phenotype of patients by applying the Akaike information criterion (AIC) and the Bayesian information criteria (BIC) to the linear regression models. Results: Overall, 91% of MSA‐positive patients met the EULAR/ACR criteria to be classified as having myositis. However, 20% of patients with anti–hydroxymethylglutaryl‐coenzyme A reductase (anti‐HMGCR) and 50% of patients with anti–PL‐7 were incorrectly classified as not having myositis. Furthermore, ~10% of patients with anti–signal recognition particle (anti‐SRP) and patients with anti‐HMGCR were misclassified as having inclusion body myositis. FAMD demonstrated that patients within each MSA‐defined subgroup had similar phenotypes. Application of both the AIC and BIC to the linear regression models revealed that MSAs were better predictors of myositis phenotypes than the subgroups defined by the EULAR/ACR criteria. Conclusion: Although the EULAR/ACR criteria successfully classified 91% of MSA‐positive myositis patients, certain MSA‐defined subgroups, including those with autoantibodies against HMGCR, SRP, and PL‐7, are frequently misclassified. In myositis patients with MSAs, autoantibodies outperform the EULAR/ACR‐defined myositis subgroups in predicting the clinical phenotypes of patients. These findings underscore the need to include MSAs in a revised myositis classification scheme. [ABSTRACT FROM AUTHOR]

Published

2022

10. Necrotizing myopathy with elevated anti‐HMGCR antibodies following exposure to the supplement Bacopa.

Author

Yaworski, Amanda M., Blyumin, Michael, Chang, Tiffany, Mammen, Andrew L., and Greene, Maxwell

Published

2023

11. Anti‐Cortactin Autoantibodies Are Associated With Key Clinical Features in Adult Myositis But Are Rarely Present in Juvenile Myositis.

Author

Pinal‐Fernandez, Iago, Pak, Katherine, Gil‐Vila, Albert, Baucells, Andres, Plotz, Benjamin, Casal‐Dominguez, Maria, Derfoul, Assia, Martinez‐Carretero, Maria Angeles, Selva‐O'Callaghan, Albert, Sabbagh, Sara, Casciola‐Rosen, Livia, Albayda, Jemima, Paik, Julie, Tiniakou, Eleni, Danoff, Sonye K., Lloyd, Thomas E., Miller, Frederick W., Rider, Lisa G., Christopher‐Stine, Lisa, and Mammen, Andrew L.

Subjects

AUTOANTIBODIES, DERMATOMYOSITIS, HEALTH outcome assessment, COMPARATIVE studies, DISEASE prevalence, ENZYME-linked immunosorbent assay, DESCRIPTIVE statistics, MYOSITIS, PHENOTYPES, LONGITUDINAL method

Abstract

Objective: To define the prevalence and clinical phenotype of anti‐cortactin autoantibodies in adult and juvenile myositis. Methods: In this longitudinal cohort study, anti‐cortactin autoantibody titers were assessed by enzyme‐linked immunosorbent assay in 670 adult myositis patients and 343 juvenile myositis patients as well as in 202 adult healthy controls and 90 juvenile healthy controls. The prevalence of anti‐cortactin autoantibodies was compared among groups. Clinical features of patients with and those without anti‐cortactin autoantibodies were also compared. Results: Anti‐cortactin autoantibodies were more common in adult dermatomyositis (DM) patients (15%; P = 0.005), particularly those with coexisting anti–Mi‐2 autoantibodies (24%; P = 0.03) or anti–NXP‐2 autoantibodies (23%; P = 0.04). In adult myositis, anti‐cortactin was associated with DM skin involvement (62% of patients with anti‐cortactin versus 38% of patients without anti‐cortactin; P = 0.03), dysphagia (36% versus 17%; P = 0.02) and coexisting anti–Ro 52 autoantibodies (47% versus 26%; P = 0.001) or anti‐NT5c1a autoantibodies (59% versus 33%; P = 0.001). Moreover, the titers of anti‐cortactin antibodies were higher in patients with interstitial lung disease (0.15 versus 0.12 arbitrary units; P = 0.03). The prevalence of anti‐cortactin autoantibodies was not different in juvenile myositis patients (2%) or in any juvenile myositis subgroup compared to juvenile healthy controls (4%). Nonetheless, juvenile myositis patients with these autoantibodies had a higher prevalence of "mechanic's hands" (25% versus 7%; P = 0.03), a higher number of hospitalizations (2.9 versus 1.3; P = 0.04), and lower peak creatine kinase values (368 versus 818 IU/liter; P = 0.02) than those without anti‐cortactin. Conclusion: The prevalence of anti‐cortactin autoantibodies is increased in adult DM patients with coexisting anti–Mi‐2 or anti–NXP‐2 autoantibodies. In adults, anti‐cortactin autoantibodies are associated with dysphagia and interstitial lung disease. [ABSTRACT FROM AUTHOR]

Published

2022

12. A North American Cohort of Anti‐SAE Dermatomyositis: Clinical Phenotype, Testing, and Review of Cases.

Author

Albayda, Jemima, Mecoli, Christopher, Casciola‐Rosen, Livia, Danoff, Sonye K., Lin, Cheng Ting, Hines, David, Gutierrez‐Alamillo, Laura, Paik, Julie J., Tiniakou, Eleni, Mammen, Andrew L., and Christopher‐Stine, Lisa

Subjects

IMMUNOGLOBULINS, UBIQUITIN, DERMATOMYOSITIS, IMMUNOPRECIPITATION, AUTOANTIBODIES

Abstract

Objective: Antibodies against the small ubiquitin‐like modifier (SUMO) activating enzyme (SAE) are one of the rarer specificities associated with dermatomyositis (DM). The purpose of this study is to describe the clinical characteristics of patients with anti‐SAE autoantibodies in a North American cohort and to ascertain cancer prevalence. We also describe the performance characteristics of the line blotting (Euroimmun) method for antibody detection compared with an immunoprecipitation‐based assay. Methods: Sera from 2127 patients suspected of having myositis were assayed for myositis‐specific autoantibodies using the Euroimmun platform. Those positive for SAE autoantibodies were assayed by a second method (immunoprecipitation) for confirmation. Only those cases positive by both methods were taken as definite cases of anti‐SAE–positive DM. Chart reviews of these patients were completed to obtain information on clinical characteristics, cancer history, and treatment. Results: Forty‐three of 2127 sera were anti‐SAE autoantibody positive by Euroimmun (≥15 units, +); of these, only 19 were confirmed positive by immunoprecipitation. All 19 cases had skin involvement and varying presentations of muscle, lung, and joint disease. Cancer occurred coincident with DM in two patients, and cancers were detected more than 5 years from symptom onset in three patients. In a population of suspected inflammatory myositis, a higher cutoff on line blot testing (≥36 units, ++) yielded better agreement with immunoprecipitation methods. Conclusion: SAE autoantibodies associate with a clinical phenotype of DM, which most commonly presents with a rash first, followed by muscle involvement and varying extramuscular involvement. As coincident cancer was seen in anti‐SAE–positive DM, judicious malignancy screening may be warranted. [ABSTRACT FROM AUTHOR]

Published

2021

13. Sequestosome‐1 (p62) expression reveals chaperone‐assisted selective autophagy in immune‐mediated necrotizing myopathies.

Author

Fischer, Norina, Preuße, Corinna, Radke, Josefine, Pehl, Debora, Allenbach, Yves, Schneider, Udo, Feist, Eugen, Casteleyn, Vincent, Hahn, Katrin, Ruck, Tobias, Meuth, Sven G., Goebel, Hans‐Hilmar, Graf, Rose, Mammen, Andrew, Benveniste, Olivier, and Stenzel, Werner

Subjects

MOLECULAR chaperones, MUSCLE proteins, SKELETAL muscle, ENDOPLASMIC reticulum, PROTEOLYSIS, MUSCLE diseases

Abstract

Diffuse myofiber necrosis in the context of inflammatory myopathy is the hallmark of immune‐mediated necrotizing myopathy (IMNM). We have previously shown that skeletal muscle fibers of IMNM patients may display nonrimmed vacuoles and sarcoplasmic irregularities. The dysfunctional chaperone activity has been linked to the defective assembly of skeletal muscle proteins and their degradation via lysosomes, autophagy and the proteasomal machinery. This study was undertaken to highlight a chaperone‐assisted selective autophagy (CASA) pathway, functionally involved in protein homeostasis, cell stress and the immune response in skeletal muscle of IMNM patients. Skeletal muscle biopsies from 54 IMNM patients were analyzed by immunostaining, as well as by qPCR. Eight biopsies of sIBM patients served as pathological controls, and eight biopsies of nondisease control subjects were included. Alteration of autophagy was detectable in all IMNM biopsy samples highlighted via a diffuse sarcoplasmic staining pattern by p62 and LC3 independent of vacuoles. This pattern was at variance with the coarse focal staining pattern mostly confined to rimmed vacuoles in sIBM. Colocalization of p62 with the chaperone proteins HSP70 and αB‐crystalline points to the specific targeting of misfolded proteins to the CASA machinery. Bcl2‐associated athanogene 3 (BAG3) positivity of these fibers emphasizes the selectivity of autophagy processes and these fibers also express MHC class I sarcolemma. Expression of genes involved in autophagy and endoplasmic reticulum (ER) stress pathways studied here is significantly upregulated in IMNM. We highlight that vacuoles without sarcolemmal features may arise in IMNM muscle biopsies, and they must not be confounded with sIBM‐specific vacuoles. Further, we show the activation of selective autophagy and emphasize the role of chaperones in this context. CASA occurs in IMNM muscle, and specific molecular pathways of autophagy differ from the ones in sIBM, with p62 as a unique identifier of this process. [ABSTRACT FROM AUTHOR]

Published

2020

14. Myositis‐Specific Autoantibodies as Relevant Adjusting Variables in Myositis Research: Comment on the Article by Hou et al.

Author

Pinal‐Fernandez, Iago and Mammen, Andrew L.

Subjects

*AUTOANTIBODIES, *BIOMARKERS, *GENE expression, *INTERFERONS, *MYOSITIS, *CARRIER proteins

Published

2021

15. Use of Proprotein Convertase Subtilisin/Kexin Type 9 Inhibitors in Statin‐Associated Immune‐Mediated Necrotizing Myopathy: A Case Series.

Author

Tiniakou, Eleni, Rivera, Erika, Mammen, Andrew L., and Christopher‐Stine, Lisa

Subjects

MUSCLE disease treatment, COENZYMES, CREATINE kinase, HYPERLIPIDEMIA, LIPIDS, MUSCLE strength, MYOSITIS, OXIDOREDUCTASES, PROTEOLYTIC enzymes, STATINS (Cardiovascular agents), DESCRIPTIVE statistics, CHEMICAL inhibitors

Abstract

Objective: To determine the safety of proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitors in patients with statin‐associated anti–3‐hydroxy‐3‐methlyglutaryl coenzyme A reductase (anti‐HMGCR)–positive immune‐mediated necrotizing myopathy (IMNM). Methods: Muscle strength was assessed in anti‐HMGCR–positive patients at each visit before and after initiation of PCSK9 inhibitors. The trends in creatine kinase (CK) levels and serum anti‐HMGCR antibody titers were monitored over time. Results: Among 122 anti‐HMGCR–positive patients, we identified 8 patients who were receiving PCSK9 inhibitors for hyperlipidemia. Patients were followed up for an average of 1.5 years (range 3–37 months), and none exhibited reduction in muscle strength. The mean ± SD CK level prior to the initiation of PCSK9 inhibitors was 956 ± 1,137 IU/liter, which was reduced to 419 ± 393 IU/liter at their last visit. Anti‐HMGCR antibody titers followed a similar trend. Notably, in 2 patients, the initiation of the lipid‐lowering medication was followed by unanticipated spontaneous clinical improvement and reduction in immunosuppression. Conclusion: PCSK9 inhibitors are safe for long‐term use as a cholesterol‐lowering agent in patients with statin‐associated IMNM. [ABSTRACT FROM AUTHOR]

Published

2019

16. Myositis Autoantigen Expression Correlates With Muscle Regeneration but Not Autoantibody Specificity.

Author

Pinal‐Fernandez, Iago, Amici, David R., Parks, Cassie A., Derfoul, Assia, Casal‐Dominguez, Maria, Pak, Katherine, Yeker, Richard, Plotz, Paul, Milisenda, Jose C., Grau‐Junyent, Josep M., Selva‐O'Callaghan, Albert, Paik, Julie J., Albayda, Jemima, Corse, Andrea M., Lloyd, Thomas E., Christopher‐Stine, Lisa, and Mammen, Andrew L.

Subjects

ANTIGEN analysis, AUTOANTIBODY analysis, RNA analysis, ANIMAL experimentation, BIOPSY, GENE expression, IMMUNITY, MICE, MYOSITIS, OXIDOREDUCTASES, REGENERATION (Biology), TRANSCRIPTION factors, TRANSFERASES, NUCLEAR proteins, SEQUENCE analysis

Abstract

Objective: Although more than a dozen myositis‐specific autoantibodies (MSAs) have been identified, most patients with myositis are positive for a single MSA. The specific overexpression of a given myositis autoantigen in myositis muscle has been proposed as initiating and/or propagating autoimmunity against that particular autoantigen. The present study was undertaken to test this hypothesis. Methods: In order to quantify autoantigen RNA expression, RNA sequencing was performed on muscle biopsy samples from control subjects, MSA‐positive patients with myositis, regenerating mouse muscles, and cultured human muscle cells. Results: Muscle biopsy samples were available from 20 control subjects and 106 patients with autoantibodies recognizing hydroxymethylglutaryl‐coenzyme A reductase (n = 40), signal recognition particles (n = 9), Jo‐1 (n = 18), nuclear matrix protein 2 (n = 12), Mi‐2 (n = 11), transcription intermediary factor 1γ (n = 11), or melanoma differentiation–associated protein 5 (n = 5). The increased expression of a given autoantigen in myositis muscle was not associated with autoantibodies recognizing that autoantigen (all q > 0.05). In biopsy specimens from both myositis muscle and regenerating mouse muscles, autoantigen expression correlated directly with the expression of muscle regeneration markers and correlated inversely with the expression of genes encoding mature muscle proteins. Myositis autoantigens were also expressed at high levels in cultured human muscle cells. Conclusion: Most myositis autoantigens are highly expressed during muscle regeneration, which may relate to the propagation of autoimmunity. However, factors other than overexpression of specific autoantigens are likely to govern the development of unique autoantibodies in individual patients with myositis. [ABSTRACT FROM AUTHOR]

Published

2019

17. Muscle endurance deficits in myositis patients despite normal manual muscle testing scores.

Author

Amici, David R., Pinal-Fernandez, Iago, Pagkatipunan, Ruben, Mears, Albert, de Lorenzo, Rebecca, Tiniakou, Eleni, Albayda, Jemima, Paik, Julie J., Lloyd, Thomas E., Christopher-STINE, Lisa, Mammen, Andrew L., and Chung, Tae

Subjects

COMPARATIVE studies, CREATINE kinase, DERMATOMYOSITIS, RESEARCH methodology, MEDICAL cooperation, MUSCLE strength, MYOSITIS, PHYSICAL fitness, POLYMYOSITIS, RESEARCH, RESEARCH funding, TIME, INCLUSION body myositis, EVALUATION research, RETROSPECTIVE studies, SEVERITY of illness index

Abstract

Introduction: It is unclear whether quantitating muscle endurance adds nonredundant information useful for the care of patients with muscular disease.Methods: Records were retrospectively reviewed for all Johns Hopkins Myositis Center patients with a muscle endurance assessment (n = 128, 226 patient-visits). Muscle endurance and strength were quantitated with the Myositis Functional Index-2 (FI2) and manual muscle testing (MMT), respectively.Results: Composite FI2 muscle endurance scores were comparable in inclusion body myositis (n = 58), dermatomyositis (n = 31), and polymyositis (n = 39). Overall, muscle endurance correlated with and evolved similarly to strength, inversely to serum creatine kinase. However, in patients with normal or near-normal strength (mean MMT > 9.75/10), muscle endurance was typically abnormal and highly variable (mean FI2, 5.6/10; interquartile range, 3.3-7.8/10).Discussion: Muscle endurance testing may identify muscle impairment inadequately described by MMT, particularly in patients with high MMT scores. Muscle Nerve 59:70-75, 2019. [ABSTRACT FROM AUTHOR]

Published

2019

18. Myositis Autoantibodies: A Comparison of Results From the Oklahoma Medical Research Foundation Myositis Panel to the Euroimmun Research Line Blot.

Author

Mecoli, Christopher A., Albayda, Jemima, Tiniakou, Eleni, Paik, Julie J., Zahid, Umar, Danoff, Sonye K., Casciola‐Rosen, Livia, Casal‐Dominguez, Maria, Pak, Katherine, Pinal‐Fernandez, Iago, Mammen, Andrew L., and Christopher‐Stine, Lisa

Subjects

AUTOANTIBODIES, BIOLOGICAL assay, COMPARATIVE studies, IMMUNOGLOBULINS, MYOSITIS, STATISTICS, PHENOTYPES, DISEASE duration, PRECIPITIN tests

Abstract

The article reports about how the ability to assay a broad range of well-defined autoantibody specificities in myositis patients is imperative for clinical phenotyping and patient care. Topics include systematic serotyping of patient cohorts, often performed using various research assays; and understanding the relationship between research testing and clinical testing paramount to advancing the field of myositis.

Published

2020

19. Anti-3-hydroxy-3-methylglutaryl-coenzyme a reductase necrotizing myopathy masquerading as a muscular dystrophy in a child.

Author

Mohassel, Payam, Foley, A. Reghan, Donkervoort, Sandra, Fequiere, Pierre R., Pak, Katherine, Bönnemann, Carsten G., and Mammen, Andrew L.

Subjects

AUTOANTIBODIES, DIFFERENTIAL diagnosis, MUSCLE diseases, MUSCULAR dystrophy, NECROSIS, OXIDOREDUCTASES

Abstract

Introduction: Immune-mediated necrotizing myopathies (IMNMs) are characterized by progressive weakness, elevated serum creatine kinase levels, and necrotizing myopathic features on muscle biopsy. Presence of highly specific autoantibodies against signal recognition particle (SRP) or 3-hydroxy-3-methylglutaryl- coenzyme A reductase (HMGCR) can aid in recognition and confirmation of IMNMs.Methods: In this study we describe a boy with HMGCR-positive necrotizing myopathy and highlight the clinical features of the patient.Results: In contrast to most adults, the patient described had a more indolent disease course, reminiscent of a muscular dystrophy. Intravenous immunoglobulin monotherapy resulted in a dramatic clinical response with return to normal strength.Conclusions: Systematic consideration of IMNMs and testing for relevant autoantibodies in children with suspected but genetically unconfirmed muscular dystrophy may help improve diagnostic accuracy and allow timely treatment with potentially highly effective immunotherapies. Muscle Nerve 56: 175-179, 2017. [ABSTRACT FROM AUTHOR]

Published

2017

20. Increased risk of statin‐associated autoimmune myopathy among American Indians.

Author

Wei, Jennie, Ketner, Elizabeth, and Mammen, Andrew L.

Subjects

STATINS (Cardiovascular agents), MUSCLE diseases, NATIVE Americans, ANTILIPEMIC agents, BLACK people, AUTOIMMUNE diseases, RACE, ETHNIC groups, WHITE people, DISEASE risk factors

Published

2022

21. Antinuclear Matrix Protein 2 Autoantibodies and Edema, Muscle Disease, and Malignancy Risk in Dermatomyositis Patients.

Author

Albayda, Jemima, Pinal-Fernandez, Iago, Huang, Wilson, Parks, Cassie, Paik, Julie, Casciola-Rosen, Livia, Danoff, Sonye K., Johnson, Cheilonda, Christopher-Stine, Lisa, and Mammen, Andrew L.

Subjects

DIAGNOSIS of edema, ADENOSINE triphosphatase, AUTOANTIBODIES, DERMATOMYOSITIS, EDEMA, LONGITUDINAL method, RESEARCH funding, DNA-binding proteins, MUSCLE weakness, CALCINOSIS, DIAGNOSIS

Abstract

Objective: Dermatomyositis (DM) patients typically present with proximal weakness and autoantibodies that are associated with distinct clinical phenotypes. We observed that DM patients with autoantibodies recognizing the nuclear matrix protein NXP-2 often presented with especially severe weakness. The aim of this study was to characterize the clinical features associated with anti-NXP-2 autoantibodies.Methods: There were 235 DM patients who underwent testing for anti-NXP-2 autoantibodies. Patient characteristics, including muscle strength, were compared between those with and without these autoantibodies. The number of cancer cases observed in anti-NXP-2-positive subjects was compared with the number expected in the general population.Results: Of the DM patients, 56 (23.8%) were anti-NXP-2-positive. There was no significant difference in the prevalence of proximal extremity weakness in patients with and without anti-NXP-2. In contrast, anti-NXP-2-positive patients had more prevalent weakness in the distal arms (35% versus 20%; P = 0.02), distal legs (25% versus 8%; P < 0.001), and neck (48% versus 23%; P < 0.001). Anti-NXP-2-positive subjects were also more likely to have dysphagia (62% versus 35%; P < 0.001), myalgia (46% versus 25%; P = 0.002), calcinosis (30% versus 17%; P = 0.02), and subcutaneous edema (36% versus 19%; P = 0.01) than anti-NXP-2-negative patients. Five anti-NXP-2-positive subjects (9%) had cancer-associated myositis, representing a 3.68-fold increased risk (95% confidence interval 1.2-8.6) compared to the expected prevalence in the general population.Conclusion: In DM, anti-NXP-2 autoantibodies are associated with subcutaneous edema, calcinosis, and a muscle phenotype characterized by myalgia, proximal and distal weakness, and dysphagia. As anti-NXP-2-positive patients have an increased risk of cancer, we suggest that they undergo comprehensive cancer screening. [ABSTRACT FROM AUTHOR]

Published

2017

22. Association of Fibrosing Myopathy in Systemic Sclerosis and Higher Mortality.

Author

Paik, Julie J., Wigley, Fredrick M., Shah, Ami A., Corse, Andrea M., Casciola-Rosen, Livia, Hummers, Laura K., and Mammen, Andrew L.

Subjects

DIAGNOSIS of muscle diseases, LONGITUDINAL method, MORTALITY, MUSCLE diseases, RESEARCH funding, SYSTEMIC scleroderma, CROSS-sectional method, FIBROSIS, RETROSPECTIVE studies, SKELETAL muscle, DIAGNOSIS

Abstract

Objective: To determine if a unique subtype of scleroderma muscle disease exists by comparing the clinical features of systemic sclerosis (SSc; scleroderma) patients with predominant fibrosis on muscle biopsy to those with inflammatory muscle histopathology.Methods: This retrospective, cross-sectional study included SSc patients with muscle weakness and an available muscle biopsy. Biopsies with fibrosis but without inflammation/necrosis were designated as "fibrosing myopathy," and those with inflammation and/or necrosis were assigned a category of "inflammatory myopathy." Clinical data, including features of SSc, serum creatine kinase (CK) levels, electromyography, autoantibody profile, and survival, were compared between the 2 groups.Results: The study population consisted of 37 weak SSc patients, 8 with fibrosing myopathy and 29 with inflammatory myopathy. Compared to those with inflammatory myopathy, patients with fibrosing myopathy were more likely to have diffuse SSc skin subtype (87% versus 62%; P = 0.18), African American race (62.5% versus 37.9%; P = 0.20), and a lower mean ± SD forced vital capacity (55.5 ± 31.9 versus 66.4 ± 17.6; P = 0.23). They also had lower mean ± SD CK values (516 ± 391 versus 2,477 ± 3,511 IU/liter; P = 0.007) and lower aldolase values (13.8 ± 4.7 versus 27.3 ± 4.7; P = 0.01). Patients with fibrosing myopathy had a significantly higher mortality (5 of 8 [62.5%] versus 4 of 29 [14.3%]; P = 0.005).Conclusion: Fibrosing myopathy is a unique histologic subtype of muscle disease among weak patients with SSc and is associated with significantly worse mortality compared to those with inflammation and/or necrosis on muscle biopsy. [ABSTRACT FROM AUTHOR]

Published

2017

23. Association of Anti-3-Hydroxy-3-Methylglutaryl-Coenzyme A Reductase Autoantibodies With DRB1*07:01 and Severe Myositis in Juvenile Myositis Patients.

Author

Kishi, Takayuki, Rider, Lisa G., Pak, Katherine, Barillas-Arias, Lilliana, Henrickson, Michael, McCarthy, Paul L., Shaham, Bracha, Weiss, Pamela F., Horkayne-Szakaly, Iren, Targoff, Ira N., Miller, Frederick W., Mammen, Andrew L., and Childhood Myositis Heterogeneity Study Group

Subjects

AUTOANTIBODIES, COENZYMES, MYOSITIS, NERVE tissue proteins, PROTEINS, RESEARCH funding, SEVERITY of illness index, DIAGNOSIS

Abstract

Objective: Autoantibodies recognizing 3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR) are associated with statin exposure, the HLA allele DRB1*11:01, and necrotizing muscle biopsies in adult myositis patients. The aim of this study was to characterize the features of juvenile anti-HMGCR-positive myositis patients.Methods: The sera of 440 juvenile myositis patients were screened for anti-HMGCR autoantibodies. Demographic and clinical features, responses to therapy, and HLA alleles were assessed. The features of anti-HMGCR-positive patients were compared to those of previously described adult patients with this autoantibody and to children with other myositis-specific autoantibodies (MSAs).Results: Five of 440 patients (1.1%) were anti-HMGCR-positive; none had taken statin medications. Three patients had rashes characteristic of juvenile dermatomyositis and 2 patients had immune-mediated necrotizing myopathies. The median highest creatine kinase (CK) level of anti-HMGCR-positive subjects was 17,000 IU/liter. All patients had severe proximal muscle weakness, distal weakness, muscle atrophy, joint contractures, and arthralgias, which were all more prevalent in HMGCR-positive subjects compared to MSA-negative patients or those with other MSAs. Anti-HMGCR-positive patients had only partial responses to multiple immunosuppressive medications, and their disease often took a chronic course. The DRB1*07:01 allele was present in all 5 patients, compared to 26.25% of healthy controls (corrected P = 0.01); none of the 5 juvenile patients had DRB1*11:01.Conclusion: Compared to children with other MSAs, muscle disease appears to be more severe in those with anti-HMGCR autoantibodies. Like adults, children with anti-HMGCR autoantibodies have severe weakness and high CK levels. In contrast to adults, in anti-HMGCR-positive children, there is a strong association with HLA-DRB1*07:01. [ABSTRACT FROM AUTHOR]

Published

2017

24. 2016 American College of Rheumatology/European League Against Rheumatism Criteria for Minimal, Moderate, and Major Clinical Response in Adult Dermatomyositis and Polymyositis: An International Myositis Assessment and Clinical Studies Group/Paediatric Rheumatology International Trials Organisation Collaborative Initiative

Author

Aggarwal, Rohit, Rider, Lisa G., Ruperto, Nicolino, Bayat, Nastaran, Erman, Brian, Feldman, Brian M., Oddis, Chester V., Amato, Anthony A., Chinoy, Hector, Cooper, Robert G., Dastmalchi, Maryam, Fiorentino, David, Isenberg, David, Katz, James D., Mammen, Andrew, de Visser, Marianne, Ytterberg, Steven R., Lundberg, Ingrid E., Chung, Lorinda, and Danko, Katalin

Subjects

BRAINSTORMING, CLINICAL trials, CONSENSUS (Social sciences), DERMATOMYOSITIS, RESEARCH methodology, MEDICAL needs assessment, POLYMYOSITIS, SURVEYS, LOGISTIC regression analysis, TREATMENT effectiveness, ADULTS, THERAPEUTICS

Abstract

Objective To develop response criteria for adult dermatomyositis (DM) and polymyositis (PM). Methods Expert surveys, logistic regression, and conjoint analysis were used to develop 287 definitions using core set measures. Myositis experts rated greater improvement among multiple pairwise scenarios in conjoint analysis surveys, where different levels of improvement in 2 core set measures were presented. The PAPRIKA (Potentially All Pairwise Rankings of All Possible Alternatives) method determined the relative weights of core set measures and conjoint analysis definitions. The performance characteristics of the definitions were evaluated on patient profiles using expert consensus (gold standard) and were validated using data from a clinical trial. The nominal group technique was used to reach consensus. Results Consensus was reached for a conjoint analysis-based continuous model using absolute percent change in core set measures (physician, patient, and extramuscular global activity, muscle strength, Health Assessment Questionnaire, and muscle enzyme levels). A total improvement score (range 0-100), determined by summing scores for each core set measure, was based on improvement in and relative weight of each core set measure. Thresholds for minimal, moderate, and major improvement were ≥20, ≥40, and ≥60 points in the total improvement score. The same criteria were chosen for juvenile DM, with different improvement thresholds. Sensitivity and specificity in DM/PM patient cohorts were 85% and 92%, 90% and 96%, and 92% and 98% for minimal, moderate, and major improvement, respectively. Definitions were validated in the clinical trial analysis for differentiating the physician rating of improvement ( P < 0.001). Conclusion The response criteria for adult DM/PM consisted of the conjoint analysis model based on absolute percent change in 6 core set measures, with thresholds for minimal, moderate, and major improvement. [ABSTRACT FROM AUTHOR]

Published

2017

25. Longitudinal Course of Disease in a Large Cohort of Myositis Patients With Autoantibodies Recognizing the Signal Recognition Particle.

Author

Pinal-Fernandez, Iago, Parks, Cassie, Werner, Jessie L., Albayda, Jemima, Paik, Julie J., Danoff, Sonye K., Casciola-Rosen, Livia, Christopher-Stine, Lisa, Mammen, Andrew L., Albayda, Jemyma, and Paik, Julie

Subjects

ANTIGENS, AUTOANTIBODIES, AUTOIMMUNE diseases, CARRIER proteins, LONGITUDINAL method, MYOSITIS, OXIDOREDUCTASES, RESEARCH funding, MUSCLE weakness, DISEASE complications

Abstract

Objective: Patients with immune-mediated necrotizing myopathy (IMNM) often have autoantibodies recognizing the signal recognition particle (SRP) or HMG-CoA reductase (HMGCR). Here, we studied a cohort of anti-SRP patients to identify factors associated with disease severity and clinical improvement; we also compared the severity of weakness in those with anti-SRP versus anti-HMGCR autoantibodies.Methods: All anti-SRP patients in the Johns Hopkins Myositis Cohort from 2002 to 2015 were included. Longitudinal information regarding proximal muscle strength, creatine kinase (CK) levels, and immunosuppressive therapy was recorded at each visit. Univariate and multivariate multilevel regression models were used to assess prognostic factors influencing recovery. Strength in the anti-SRP patients was compared to strength in 49 previously described anti-HMGCR subjects.Results: Data from 37 anti-SRP patients and 380 total clinic visits were analyzed. Younger age at onset was associated with more severe weakness at the first visit (P = 0.02) and all subsequent visits (P = 0.002). Only 50% of patients reached near-full or full strength after 4 years of treatment, and most of these continued to have elevated CK levels. Rituximab appeared to be effective in 13 of 17 anti-SRP patients. Anti-SRP patients were significantly weaker than those with anti-HMGCR autoantibodies (-1.3 strength points; P = 0.001).Conclusion: Younger age at onset is associated with more severe weakness in anti-SRP myositis. Furthermore, even among anti-SRP patients whose strength improved with immunosuppression, most had ongoing disease activity as demonstrated by elevated CK levels. Finally, anti-SRP patients were significantly weaker than anti-HMGCR patients, providing evidence that these autoantibodies are associated with distinct forms of IMNM. [ABSTRACT FROM AUTHOR]

Published

2017

26. Conflicting reports of anti–cytosolic 5′‐nucleotidase 1A autoantibodies in juvenile dermatomyositis: comment on the article by Rietveld et al.

Author

Mammen, Andrew L., Pinal‐Fernandez, Iago, and Rider, Lisa G.

Subjects

*AUTOANTIBODIES, *DERMATOMYOSITIS, *IMMUNOBLOTTING, *ENZYME-linked immunosorbent assay

Published

2022

27. Symptomatic and Electrodiagnostic Features of Peripheral Neuropathy in Scleroderma.

Author

Paik, Julie J., Mammen, Andrew L., Wigley, Fredrick M., Shah, Ami A., Hummers, Laura K., and Polydefkis, Michael

Subjects

ELECTROPHYSIOLOGY, PERIPHERAL neuropathy, SYSTEMIC scleroderma, DISEASE prevalence, DISEASE complications

Abstract

Objective: To determine the prevalence of peripheral neuropathy in scleroderma.Methods: The prevalence of length-dependent peripheral neuropathy was rigorously assessed using signs and symptoms of neuropathy derived from the Total Neuropathy Score (TNS), and standardized nerve conduction study (NCS). All subjects underwent TNS and NCS. Those who were symptomatic or had NCS evidence of peripheral neuropathy underwent laboratory evaluation for secondary causes of neuropathy.Results: A total of 130 subjects were approached for participation and 60 enrolled. Of the 60 subjects, 50 (83.3%) were female and 37 (61.7%) were of the limited cutaneous subtype. The mean ± SD age was 55 ± 11.1 years, and mean ± SD disease duration was 15.3 ± 10.1 years. A total of 17 of 60 (28%) had evidence of a peripheral neuropathy as defined by the presence of neuropathic symptoms on the TNS (12 of 60) and/or electrophysiologic evidence of neuropathy (5 subjects with neuropathic symptoms and 5 without neuropathic symptoms). Subjects with neuropathy were more likely to be male (60% versus 40%; P = 0.02), African American (41% versus 4.6%; P = 0.001), have diabetes mellitus (17.7% versus 0%; P = 0.02), have limited cutaneous scleroderma (82.3% versus 53.5%; P = 0.04), and have anti-U1 RNP antibodies (23.5% versus 0%; P = 0.009) than those without neuropathy. A potential nonscleroderma etiology for the peripheral neuropathy such as diabetes mellitus was found in 82.3% (14 of 17) of subjects with neuropathy.Conclusion: While symptoms or objective evidence of peripheral neuropathy are common among patients with scleroderma, the cause may often be attributed to comorbid nonscleroderma-related conditions. [ABSTRACT FROM AUTHOR]

Published

2016

28. Absence of anti-HMG-CoA reductase autoantibodies in severe self-limited statin-related myopathy.

Author

Floyd, James S., Brody, Jennifer A., Tiniakou, Eleni, Psaty, Bruce M., and Mammen, Andrew

Abstract

Introduction: Patients with self-limited statin-related myopathy improve spontaneously when statins are stopped. In contrast, patients with statin-associated autoimmune myopathy have autoantibodies recognizing 3-hydroxy-3-methyl-glutaryl-coenzyme A reductase (HMGCR) and usually require immunosuppressive therapy to control their disease. On initial presentation, it can sometimes be difficult to distinguish between these 2 diseases, as both present with muscle pain, weakness, and elevated serum creatine kinase (CK) levels. The goal of this study was to determine whether patients with severe self-limited statin-related myopathy also make anti-HMGCR autoantibodies.Methods: We screened 101 subjects with severe self-limited cerivastatin-related myopathy for anti-HMGCR autoantibodies.Results: No patient with severe self-limited cerivastatin-related myopathy had anti-HMGCR autoantibodies.Conclusion: Anti-HMGCR autoantibody testing can be used to help differentiate whether a patient has self-limited myopathy due to cerivastatin or autoimmune statin-associated myopathy; these findings may apply to other statins as well. Muscle Nerve 54: 142-144, 2016. [ABSTRACT FROM AUTHOR]

Published

2016

29. Cytosolic 5'-Nucleotidase 1A As a Target of Circulating Autoantibodies in Autoimmune Diseases.

Author

LLOYD, THOMAS E., CHRISTOPHER-STINE, LISA, PINAL-FERNANDEZ, IAGO, TINIAKOU, ELENI, PETRI, MICHELLE, BAER, ALAN, DANOFF, SONYE K., PAK, KATHERINE, CASCIOLA-ROSEN, LIVIA A., and MAMMEN, ANDREW L.

Subjects

AUTOIMMUNE disease diagnosis, AUTOANTIBODIES, AUTOIMMUNE diseases, COMPARATIVE studies, DERMATOMYOSITIS, DIFFERENTIAL diagnosis, RESEARCH methodology, MEDICAL cooperation, RESEARCH, RESEARCH funding, SERODIAGNOSIS, EVALUATION research, PREDICTIVE tests, CASE-control method, DIAGNOSIS

Abstract

Objective: Prior investigations demonstrated that autoantibodies recognizing cytosolic 5'-nucleotidase 1A (NT5C1A) are found in 33-76% of patients with inclusion body myositis (IBM) but are observed only rarely in patients with polymyositis (PM). Thus, anti-NT5C1A may help distinguish IBM from PM. Although 4-21% of patients with dermatomyositis (DM) were shown to be anti-NT5C1A antibody positive, the clinical features of anti-NT5C1A-positive patients with DM have not been described. Furthermore, the prevalence of anti-NT5C1A antibodies in other rheumatic conditions has not been reported. This study was undertaken to define the prevalence and clinical features of anti-NT5C1A-positive patients with DM, PM, IBM, or other systemic autoimmune diseases.Methods: We screened for anti-NT5C1A autoantibodies in patients with IBM, DM, PM, Sjögren's syndrome (SS), or systemic lupus erythematosus (SLE) and in healthy volunteers. Clinical characteristics were compared between patients who were anti-NT5C1A positive and those who were anti-NT5C1A negative.Results: Anti-NT5C1A autoantibodies were detected in 71 (61%) of 117 patients with IBM, 2 (5%) of 42 patients with PM, 2 (5%) of 42 healthy volunteers, 24 (15%) of 159 patients with DM, 10 (23%) of 44 patients with SS, and 13 (14%) of 96 patients with SLE. No anti-NT5C1A antibody-positive patients with SS or SLE had muscle involvement. Anti-NT5C1A-positive patients with IBM had a lower prevalence of rimmed vacuoles (62% versus 83% of antibody-negative patients; P = 0.02). No differences in the clinical characteristics of antibody-positive and antibody-negative patients with DM, SS, or SLE were observed.Conclusion: Anti-NT5C1A is a common target of circulating autoantibodies, especially in IBM but also in several different autoimmune diseases. In SLE and SS, anti-NT5C1A autoreactivity is not associated with muscle disease. [ABSTRACT FROM AUTHOR]

Published

2016

30. Spectrum of Muscle Histopathologic Findings in Forty-Two Scleroderma Patients With Weakness.

Author

Paik, Julie J., Wigley, Fredrick M., Lloyd, Thomas E., Corse, Andrea M., Casciola-Rosen, Livia, Shah, Ami A., Boin, Francesco, Hummers, Laura K., and Mammen, Andrew L.

Subjects

AGE distribution, DATABASES, ELECTROMYOGRAPHY, IMMUNOHISTOCHEMISTRY, LONGITUDINAL method, MUSCLE diseases, NEEDLE biopsy, POLYMYOSITIS, RESEARCH funding, SEX distribution, SYSTEMIC scleroderma, TIME, RETROSPECTIVE studies, SEVERITY of illness index, DISEASE progression, MUSCLE weakness

Abstract

Objective: To determine if distinct muscle pathologic features exist in scleroderma subjects with weakness.Methods: This retrospective study included weak scleroderma subjects with muscle biopsies available for review. Biopsies were systematically assessed for individual pathologic features, including inflammation, necrosis, fibrosis, and acute neurogenic atrophy. Based on the aggregate individual features, biopsies were assigned a histopathologic category of polymyositis, dermatomyositis, necrotizing myopathy, nonspecific myositis, "acute denervation," "fibrosis only," or "other." Clinical data analyzed included autoantibody profiles, scleroderma subtype and disease duration, Medsger muscle severity scores, creatine kinase, electromyography, and muscle magnetic resonance imaging.Results: A total of 42 subjects (79% female and 64% diffuse scleroderma) were included in this study. Necrosis (67%), inflammation (48%), acute neurogenic atrophy (48%), and fibrosis (33%) were the most prevalent pathologic features. The presence of fibrosis was strongly associated with anti-PM-Scl antibodies. Histopathologic categories included nonspecific myositis (36%), necrotizing myopathy (21%), dermatomyositis (7%), "acute denervation" (7%), "fibrosis only" (7%), and polymyositis (5%). Disease duration of scleroderma at the time of muscle biopsy was shorter in polymyositis than other histopathologic categories. Patients with anti-PM-Scl and Scl-70 antibodies also had a shorter disease duration than those with other autoantibody profiles.Conclusion: Nonspecific myositis and necrotizing myopathy were the most common histopathologic categories in weak scleroderma subjects. Surprisingly, nearly half of the subjects studied had histologic evidence of acute motor denervation (acute neurogenic atrophy); this has not been previously reported. Taken together, these observations suggest that a variety of pathologic mechanisms may underlie the development of myopathy in scleroderma. [ABSTRACT FROM AUTHOR]

Published

2015

31. The composition of cellular infiltrates in anti-HMG-CoA reductase-associated myopathy.

Author

Chung, Tae, Christopher‐Stine, Lisa, Paik, Julie J., Corse, Andrea, and Mammen, Andrew L.

Abstract

Introduction: To characterize cellular infiltrates in muscle biopsies from patients with anti-3-hydroxy-3-methyl-gulatryl-CoA reductase (HMGCR)-associated myopathy. Methods: Biopsies from 18 anti-HMGCR myopathy and 7 control dermatomyositis patients were analyzed. Results: CD4+ and CD8+ T-cells were scattered within the endomysium in 50% of anti-HMGCR biopsies. All anti-HMGCR biopsies included increased endomysial and/or perivascular CD163+ M2 macrophages; CD11c+ M1 macrophages were present in 18.8%. CD123+ plasmacytoid dendritic (PD) cells were observed within the endomysium and perivascular spaces in 62.5% of anti-HMGCR biopsies. Membrane attack complex was deposited on endothelial cells in 50% and on the sarcolemma of nonnecrotic muscle fibers in 85.7% of anti-HMGCR cases. Major histocompatibility complex class I antigen was up-regulated in 87.5% of the anti-HMGCR cases. Conclusions: In addition to necrosis, scattered CD4+, CD8+, and PD cells are characteristic of anti-HMGCR myopathy. Predominant M2 polarization suggests infiltrating macrophages are more likely to be involved with tissue repair than destruction. [ABSTRACT FROM AUTHOR]

Published

2015

32. Diagnostic evaluation of rhabdomyolysis.

Author

Nance, Jessica R. and Mammen, Andrew L.

Abstract

ABSTRACT Rhabdomyolysis is characterized by severe acute muscle injury resulting in muscle pain, weakness, and/or swelling with release of myofiber contents into the bloodstream. Symptoms develop over hours to days after an inciting factor and may be associated with dark pigmentation of the urine. Serum creatine kinase and urine myoglobin levels are markedly elevated. Clinical examination, history, laboratory studies, muscle biopsy, and genetic testing are useful tools for diagnosis of rhabdomyolysis, and they can help differentiate acquired from inherited causes of rhabdomyolysis. Acquired causes include substance abuse, medication or toxic exposures, electrolyte abnormalities, endocrine disturbances, and autoimmune myopathies. Inherited predisposition to rhabdomyolysis can occur with disorders of glycogen metabolism, fatty acid β-oxidation, and mitochondrial oxidative phosphorylation. Less common inherited causes of rhabdomyolysis include structural myopathies, channelopathies, and sickle-cell disease. This review focuses on the differentiation of acquired and inherited causes of rhabdomyolysis and proposes a practical diagnostic algorithm. Muscle Nerve 51: 793-810, 2015 [ABSTRACT FROM AUTHOR]

Published

2015

33. Expression of the Dermatomyositis Autoantigen Transcription Intermediary Factor 1γ in Regenerating Muscle.

Author

Mohassel, Payam, Rosen, Paul, Casciola-Rosen, Livia, Pak, Katherine, and Mammen, Andrew L.

Published

2015

34. Laing distal myopathy pathologically resembling inclusion body myositis.

Author

Roda, Ricardo H., Schindler, Alice B., Blackstone, Craig, Mammen, Andrew L., Corse, Andrea M., and Lloyd, Thomas E.

Subjects

MUSCLE diseases, MHC antibodies, AUTOSOMAL recessive polycystic kidney, MYOSITIS, GENETIC mutation

Abstract

Mutations in MYH7 cause autosomal dominant Laing distal myopathy. We present a family with a previously reported deletion (c.5186_5188del AGA, p.K1729del). Muscle pathology in one family member was characterized by an inflammatory myopathy with rimmed vacuoles, increased MHC Class I expression, and perivascular and endomysial muscle inflammation comprising CD3+, CD4+, CD8+, and CD68+ inflammatory cells. Interestingly, this biopsy specimen contained TDP-43, p62, and SMI-31-positive protein aggregates typical of inclusion body myositis. These findings should alert physicians to the possibility that patients with MYH7 mutations may have muscle biopsies showing pathologic findings similar to inclusion body myositis. [ABSTRACT FROM AUTHOR]

Published

2014

35. A Case of Progressive Quadriceps Weakness and Elevated Creatine Kinase Level Mimicking Inclusion Body Myositis.

Author

Leung, Doris G., Taylor, Harold A., Lindy, Amanda S., Basehore, Monica J., and Mammen, Andrew L.

Published

2014

36. Most Patients With Cancer-Associated Dermatomyositis Have Antibodies to Nuclear Matrix Protein NXP-2 or Transcription Intermediary Factor 1γ.

Author

Fiorentino, David F., Chung, Lorinda S., Christopher-Stine, Lisa, Zaba, Lisa, Li, Shufeng, Mammen, Andrew L., Rosen, Antony, and Casciola-Rosen, Livia

Abstract

Objective Since dermatomyositis (DM) is associated with an increased risk of malignancy, accurate identification of patients likely to harbor cancers is important. Using immunoprecipitations from radiolabeled cell lysates, several groups recently showed that anti-transcription intermediary factor 1γ (anti-TIF-1γ) antibodies are associated with malignancy in DM. We undertook this study to develop sensitive, specific assays to detect antibodies against TIF-1γ and nuclear matrix protein NXP-2 and to evaluate their association with malignancy in DM. Methods To detect anti-TIF-1γ antibodies, immunoprecipitations were performed using lysates made from HeLa cells overexpressing TIF-1γ, with detection by immunoblotting. Anti-NXP-2 antibodies were assayed by immunoprecipitation using 35S-methionine-labeled NXP-2 generated by in vitro transcription/translation. We analyzed patient sera from DM cohorts seen at the Stanford University Dermatology Clinic (n = 111) and the Johns Hopkins Myositis Center (n = 102). Results A total of 17% and 38% of patients had antibodies against NXP-2 and TIF-1γ, respectively. Reactivity against either NXP-2 or TIF-1γ identified 83% of patients with cancer-associated DM. In addition to older age and male sex, cancer was associated with antibodies to NXP-2 or TIF-1γ on multivariate analysis (odds ratio 3.78 [95% confidence interval 1.33-10.8]). Stratification by sex revealed that anti-NXP-2 was specifically associated with cancer in males (odds ratio 5.78 [95% confidence interval 1.35-24.7]). Conclusion These studies demonstrate that anti-NXP-2 and anti-TIF-1γ antibodies are frequent DM specificities (found in 55% of patients) and are present in most patients with cancer-associated DM. [ABSTRACT FROM AUTHOR]

Published

2013

37. Statin-associated autoimmune myopathy and anti-HMGCR autoantibodies.

Author

Mohassel, Payam and Mammen, Andrew L.

Abstract

ABSTRACT Statins are among the most commonly prescribed medications that significantly reduce cardiovascular risk in selected individuals. However, these drugs can also be associated with muscle symptoms ranging from mild myalgias to severe rhabdomyolysis. Although statin myotoxicity is usually self-limited, in some instances statin-exposed subjects can develop an autoimmune myopathy typically characterized by progressive weakness, muscle enzyme elevations, a necrotizing myopathy on muscle biopsy, and autoantibodies that recognize 3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR), the pharmacologic target of statins. These antibodies are also found in some autoimmune myopathy patients without statin exposure. Importantly, anti-HMGCR antibodies are not found in the vast majority of statin-exposed subjects without autoimmune myopathy, including those with self-limited statin intolerance. Thus, testing for these antibodies may help differentiate those with self-limited statin myopathy who recover after statin discontinuation from those with a progressive statin-associated autoimmune myopathy who typically require immunosuppressive therapy. Muscle Nerve 48: 477-483, 2013 [ABSTRACT FROM AUTHOR]

Published

2013

38. Antibody levels correlate with creatine kinase levels and strength in anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase-associated autoimmune myopathy.

Author

Werner, Jessie L., Christopher-Stine, Lisa, Ghazarian, Sharon R., Pak, Katherine S., Kus, Jordan E., Daya, Natalie R., Lloyd, Thomas E., and Mammen, Andrew L.

Subjects

AUTOIMMUNE disease diagnosis, DIAGNOSIS of muscle diseases, ANALYSIS of variance, BLOOD testing, ENZYME-linked immunosorbent assay, IMMUNOGLOBULINS, REGRESSION analysis, RESEARCH funding, T-test (Statistics), STATINS (Cardiovascular agents), SEVERITY of illness index, DATA analysis software, DESCRIPTIVE statistics

Abstract

Objective Autoantibodies recognizing 3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR) are found in patients with statin-associated immune-mediated necrotizing myopathy and, less commonly, in statin-unexposed patients with autoimmune myopathy. The main objective of this study was to define the association of anti-HMGCR antibody levels with disease activity. Methods Anti-HMGCR levels, creatine kinase (CK) levels, and strength were assessed in anti-HMGCR-positive patients. Associations of antibody level with CK level and strength at visit 1 were analyzed in 55 patients, 40 of whom were exposed to statins. In 12 statin-exposed and 5 statin-unexposed patients with serum from 5 serial visits, the evolution of antibody levels, CK levels, and strength was investigated. Results Antibody levels were associated with CK levels ( P < 0.001), arm strength ( P < 0.05), and leg strength ( P < 0.05) at visit 1, but these associations were only significant among statin-exposed patients in stratified analyses. With immunosuppressive treatment over 26.2 ± 12.6 months (mean ± SD), antibody levels declined ( P < 0.05) and arm abduction strength improved ( P < 0.05) in the 17 patients followed up longitudinally. The separate analysis showed that statin-exposed patients developed decreased antibody levels ( P < 0.01), decreased CK levels ( P < 0.001), improved arm strength ( P < 0.05), and improved hip flexion strength ( P < 0.05) with treatment. Anti-HMGCR antibody levels did not normalize in any patient. Conclusion In the entire cohort, initial anti-HMGCR levels correlated with indicators of disease activity; with immunosuppressive treatment, antibody levels declined and arm strength improved. Statin-exposed patients had significant improvements in CK levels and strength whereas statin-unexposed patients did not, suggesting a phenotypic difference between statin-exposed and statin-unexposed anti-HMGCR-positive patients. [ABSTRACT FROM AUTHOR]

Published

2012

39. Increased frequency of DRB1*11:01 in anti-hydroxymethylglutaryl-coenzyme a reductase-associated autoimmune myopathy.

Author

Mammen, Andrew L., Gaudet, Daniel, Brisson, Diane, Christopher-Stine, Lisa, Lloyd, Thomas E., Leffell, Mary S., and Zachary, Andrea A.

Abstract

Objective To investigate the association of anti-hydroxymethylglutaryl-coenzyme A reductase (anti-HMGCR) myopathy with HLA class I and II antigens. Methods HLA antigens were determined in 1) 20 white and 8 African American anti-HMGCR patients, 2) 487 white and 167 African American controls, and 3) 51 white subjects with mild self-limited statin intolerance. Results White anti-HMGCR patients had a higher frequency of the combination HLA-DR11, DQA5, and DQB7 than controls or statin-intolerant subjects (70% versus 17%; odds ratio [OR] 11.7 [95% confidence interval (95% CI) 4.0-35.3], P = 4.1 × 10−7 and 70% versus 21%; OR 8.3 [95% CI 2.2-33.9], P = 5.4 × 10−4, respectively). This combination was not increased in African American anti-HMGCR subjects compared to controls (13% versus 3%; OR 4.6 [95% CI 0.2-53.3], P = 0.2). However, DR11 was increased in African American anti-HMGCR patients compared to controls (88% versus 21%; OR 26.4 [95% CI 3.1-590.3], P = 0.0002). High-resolution mapping showed that 95% with DR11 had DRB1*11:01. DQA1 and DQB6 were less frequent in white anti-HMGCR-positive patients compared to controls (25% versus 65%; OR 0.2 [95% CI 0.1-0.5], P = 5.5 × 10−4 and 0% versus 45%; OR 0.0 [95% CI 0.0-0.3], P = 2.1 × 10−5, respectively). DRB11 was not associated with particular disease features. Conclusion DRB1*11:01 is associated with an increased risk of anti-HMGCR myopathy in whites and African Americans. These findings suggest a mechanistic link between statin exposure, increased HMGCR expression, and the possible presentation of HMGCR-derived peptide(s) by DRB1*11:01. [ABSTRACT FROM AUTHOR]

Published

2012

40. Expanding the spectrum of monoclonal light chain deposition disease in muscle.

Author

Ostrow, Lyle W., Corse, Andrea M., Morrison, Brett M., Huff, Carol A., Carrino, John A., Hoke, Ahmet, and Mammen, Andrew L.

Abstract

Introduction: The diagnosis of amyloid myopathy is delayed when monoclonal gammopathies are not detected on initial testing and muscle biopsies are nondiagnostic, and the EMG and symptoms can mimic an inflammatory myopathy. Methods: Case report of a patient presenting with severe progressive muscle weakness of unclear etiology despite an extensive workup including two nondiagnostic muscle biopsies. Results: Directed by MRI, a third biopsy revealed amyloid angiopathy and noncongophilic kappa light chain deposition in scattered subsarcolemmal rings and perimysial regions. A serum free light chain (FLC) assay revealed a kappa monoclonal gammopathy, which was not detected by multiple immunofixations. Conclusions: The spectrum of immunoglobulin deposition in muscle is similar to other organs. It comprises a continuum that includes parenchymal amyloid deposition, amyloid angiopathy, and noncongophilic Light Chain Deposition Disease (LCDD). We recommend including the FLC assay in the routine investigation for monoclonal gammopathies. This case also highlights the value of MRI-guided muscle biopsy. Muscle Nerve, 2012 [ABSTRACT FROM AUTHOR]

Published

2012

41. Rarity of anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase antibodies in statin users, including those with self-limited musculoskeletal side effects.

Author

Mammen, Andrew L., Pak, Katherine, Williams, Emma K., Brisson, Diane, Coresh, Joe, Selvin, Elizabeth, and Gaudet, Daniel

Abstract

Objective Statins, among the most commonly prescribed medications, are associated with a wide range of musculoskeletal side effects. These include a progressive autoimmune myopathy with anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase (anti-HMGCR) antibodies that requires immunosuppression. However, it remains unknown whether these antibodies are found in statin users with and without self-limited musculoskeletal side effects; this limits their diagnostic utility. The current work assessed the prevalence of anti-HMGCR antibodies in these groups of statin users. Methods We determined the prevalence of anti-HMGCR antibodies in 1,966 participants (including 763 current statin users) in a substudy of the community-based Atherosclerosis Risk in Communities (ARIC) Study and 98 French Canadian subjects with familial hypercholesterolemia, including 51 with documented statin intolerance. Results No participant in the ARIC substudy, including those with past or current statin exposure at the time of sample collection, had anti-HMGCR antibodies. Similarly, none of 51 patients with self-limited statin intolerance or 47 statin-tolerant patients receiving maximal statin therapy were anti-HMGCR positive. Conclusion The majority of patients with and without statin exposure, including those with self-limited statin intolerance, do not develop anti-HMGCR antibodies. Therefore, anti-HMGCR antibodies are highly specific for those with an autoimmune myopathy. [ABSTRACT FROM AUTHOR]

Published

2012

42. A novel autoantibody recognizing 200-kd and 100-kd proteins is associated with an immune-mediated necrotizing myopathy.

Author

Christopher-Stine, Lisa, Casciola-Rosen, Livia A, Hong, Grace, Chung, Tae, Corse, Andrea M, and Mammen, Andrew L

Abstract

OBJECTIVE: Myofiber necrosis without prominent inflammation is a nonspecific finding in patients with dystrophies and toxic or immune-mediated myopathies. However, the etiology of a necrotizing myopathy is often obscure, and the question of which patients would benefit from immunosuppression remains unanswered. The aim of this study was to identify novel autoantibodies in patients with necrotizing myopathy. METHODS: Muscle biopsy specimens and serum samples were available for 225 patients with myopathy. Antibody specificities were determined by performing immunoprecipitations from (35)S-methionine-labeled HeLa cell lysates. Selected biopsy specimens were stained for membrane attack complex, class I major histocompatibility complex (MHC), and endothelial cell marker CD31. RESULTS: Muscle biopsy specimens from 38 of 225 patients showed predominantly myofiber necrosis. Twelve of these patients had a known autoantibody association with or other etiology for their myopathy. Sixteen of the remaining 26 sera immunoprecipitated 200-kd and 100-kd proteins; this specificity was observed in only 1 of 187 patients without necrotizing myopathy. Patients with the anti-200/100 autoantibody specificity had proximal weakness (100%), high creatine kinase levels (mean maximum 10,333 IU/liter), and an irritable myopathy on electromyography (88%). Sixty-three percent of these patients had been exposed to statins prior to the onset of weakness. All patients responded to immunosuppressive therapy, and many experienced a relapse of weakness when the medication was tapered. Immunohistochemical studies showed membrane attack complex on small blood vessels in 6 of 8 patients and on the surface of non-necrotic myofibers in 4 of 8 patients. Five of 8 patients had abnormal capillary morphology, and 4 of 8 patients expressed class I MHC on the surface of non-necrotic myofibers. CONCLUSION: An anti-200/100-kd specificity defines a subgroup of patients with necrotizing myopathy who previously were considered to be autoantibody negative. We propose that these patients have an immune-mediated myopathy that is frequently associated with prior statin use and should be treated with immunosuppressive therapy. [ABSTRACT FROM AUTHOR]

Published

2010

43. Dermatomyositis and polymyositis.

Author

Mammen, Andrew L.

Subjects

*DERMATOMYOSITIS, *POLYMYOSITIS, *AUTOIMMUNE diseases, *MUSCLE diseases, *AUTOANTIBODIES

Abstract

Dermatomyositis (DM) and polymyositis (PM) are autoimmune myopathies characterized clinically by proximal muscle weakness, muscle inflammation, extramuscular manifestations, and frequently, the presence of autoantibodies. Although there is some overlap, DM and PM are separate diseases with different pathophysiological mechanisms. Furthermore, unique clinical phenotypes are associated with each of the myositis-specific autoantibodies (MSAs) associated with these disorders. This review will focus on the clinical features, pathology, and immunogenetics of PM and DM with an emphasis on the importance of autoantibodies in defining unique phenotypes and, perhaps, as clues to help elucidate the mechanisms of disease. [ABSTRACT FROM AUTHOR]

Published

2010

44. Expression of the Dermatomyositis Autoantigen Mi-2 in Regenerating Muscle.

Author

Mammen, Andrew L., Casciola-Rosen, Livia A., Hall, John C., Christopher-Stine, Lisa, Corse, Andrea M., and Rosen, Antony

Subjects

*DERMATOMYOSITIS, *CHROMATIN, *GENETIC regulation, *MUSCLES, *GENE expression, *MOLECULAR cell differentiation

Abstract

The article presents a study on the expression of the chromatin remodeler Mi-2 in dermatomyositis (DM) muscle. It is stated in the study that Mi-2 protein levels are regulated in DM muscle, which produce myositis-specific autoantibodies. It notes that the study analyzed Mi-2 expression and utilized a cell culture system of muscle differentiation. It also mentions that the study found that the presence of incompletely differentiated muscle cells is reflected in the high level of Mi-2 expression.

Published

2009

45. Anti-3-hydroxy-3-methylglutaryl-coenzyme a reductase autoantibody-positive necrotizing autoimmune myopathy with dermatomyositis-like eruption.

Author

Parikh, Prachi, Tavee, Jinny, Soltanzadeh, Payam, Mammen, Andrew L., McKeever, Paul, and Li, Yuebing

Published

2018

46. Necrotizing myopathy caused by central hypothyroidism.

Author

Tiniakou, Eleni and Mammen, Andrew L.

Published

2015

47. Reply.

Author

Valiyil, Ritu, Casciola-Rosen, Livia, Hong, Grace, Mammen, Andrew L., and Christopher-Stine, Lisa

Published

2011

48. Autoantibodies against 3-hydroxy-3-methylglutaryl-coenzyme A reductase in patients with statin-associated autoimmune myopathy.

Author

Mammen AL, Chung T, Christopher-Stine L, Rosen P, Rosen A, Doering KR, and Casciola-Rosen LA

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Autoantibodies immunology, Autoantigens immunology, Autoimmune Diseases epidemiology, Autoimmune Diseases immunology, Child, Preschool, Enzyme-Linked Immunosorbent Assay methods, Female, HeLa Cells, Humans, Hydroxymethylglutaryl CoA Reductases chemistry, Male, Middle Aged, Muscle Fibers, Skeletal immunology, Muscle Fibers, Skeletal pathology, Myositis epidemiology, Myositis immunology, Necrosis, Protein Structure, Tertiary, Regeneration immunology, Seroepidemiologic Studies, Young Adult, Autoantibodies blood, Autoimmune Diseases chemically induced, Hydroxymethylglutaryl CoA Reductases immunology, Hydroxymethylglutaryl-CoA Reductase Inhibitors adverse effects, Myositis chemically induced

Abstract

Objective: In addition to inducing a self-limited myopathy, statin use is associated with an immune-mediated necrotizing myopathy (IMNM), with autoantibodies that recognize ∼200-kd and ∼100-kd autoantigens. The purpose of this study was to identify these molecules to help clarify the disease mechanism and facilitate diagnosis., Methods: The effect of statin treatment on autoantigen expression was addressed by immunoprecipitation using sera from patients. The identity of the ∼100-kd autoantigen was confirmed by immunoprecipitation of in vitro-translated 3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR) protein. HMGCR expression in muscle was analyzed by immunofluorescence. A cohort of myopathy patients was screened for anti-HMGCR autoantibodies by enzyme-linked immunosorbent assay and genotyped for the rs4149056 C allele, a predictor of self-limited statin myopathy., Results: Statin exposure induced expression of the ∼200-kd/∼100-kd autoantigens in cultured cells. HMGCR was identified as the ∼100-kd autoantigen. Competition experiments demonstrated no distinct autoantibodies recognizing the ∼200-kd protein. In muscle biopsy tissues from anti-HMGCR-positive patients, HMGCR expression was up-regulated in cells expressing neural cell adhesion molecule, a marker of muscle regeneration. Anti-HMGCR autoantibodies were found in 45 of 750 patients presenting to the Johns Hopkins Myositis Center (6%). Among patients ages 50 years and older, 92.3% had taken statins. The prevalence of the rs4149056 C allele was not increased in patients with anti-HMGCR., Conclusion: Statins up-regulate the expression of HMGCR, the major target of autoantibodies in statin-associated IMNM. Regenerating muscle cells express high levels of HMGCR, which may sustain the immune response even after statins are discontinued. These studies demonstrate a mechanistic link between an environmental trigger and the development of sustained autoimmunity. Detection of anti-HMGCR autoantibodies may facilitate diagnosis and direct therapy., (Copyright © 2011 by the American College of Rheumatology.)

Published

2011