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ROLE OF ANTIBODIES
IN MUSCLE DISEASES
MOHAMED E. ABD-ELHADY, MSC
APRIL 2023
MUSCLE’S
ANATOMY
(I) IDIOPATHIC INFLAMMATORY MYOPATHIES
INFLAMMATORY MYOPATHIES
• Dermatomyositis, Polymyositis, and Inclusion Body Myositis (IBM)
• Immune Mediated Necrotizing Myopathy (IMNM): AB against HMG-CoA
reductases.
• Systemic Autoimmune Rheumatic Diseases (SARD)
• Overlap Syndrome and ADM/CADM
• The main concern is their association with tumors and/or auto-autoimmune
disorders, which guides the investigations and management.
ANTIBODIES IN INFLAMMATORY MYOPATHIES
• Myositis-Specific Antibodies (MSA) and Myositis-Associated Antibodies (MAA).
• MSA: is defined as autoantibody specificities that are considered relatively specific for
PM/DM.
• MAA: autoantibody specificity found in PM/DM but not specific for this diagnosis and
may be found in other SARD
• Role of AB in inflammatory myopathies:
I) For associated autoimmune disease (MAA): ESR, RF, ANA, ANCA C & P, anti-
Ds-DNA, anti phospholipid AB, anti-PM-Scl, anti-Ku, anti-
U1ribonucleoprotein (RNP) U1/U2RNP, anti-Ro 60 and anti-La.
II) For associated malignancies: Tumor Markers
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-ARS (aminoacyl tRNA synthetases):
autoantibodies that recognize the cytoplasmic amino acid-charging enzymes,
aminoacyl tRNA synthetases. Eight of them including histidyl (Jo-1), threonyl (PL-7),
alanyl (PL-12), glycyl (EJ), isoleucyl (OJ), asparaginyl (KS), phenylalanyl (ZO), and
tyrosyl (YRS/HA) tRNA synthetases have been reported.
They can be further classified into either anti-Jo-1 or anti-non-Jo-1 Abs.
Anti-Jo-1 (anti-synthetase syndrome) is the 1st identified MSA and is associated
with ILD, polyarteritis, and Raynaud’s phenomenon.
Anti-Jo-1 antibodies, usually found in 15–25 % of PM/DM patients, are by far the
most common among anti-ARS antibodies; all others are usually found only in 0.5–
6 % of patients
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-ARS (aminoacyl tRNA synthetases):
anti-PL-7/PL-12 was associated with early and severe ILD and less myositis (CADM).
In summary, patients with any anti-ARS have a similar clinical syndrome known as
anti- synthetase syndrome; however, several recent studies suggest that antibodies
to non-Jo-1 ARS are associated with earlier and more severe ILD and poor
prognosis compared with anti-Jo-1 (+) patients. Also, non-Jo-1 anti-ARS (+)
patients are more likely to have ILD without typical myositis.
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-SRP (anti-signal recognition particle):
anti-SRP is associated with classic PM and some were unusually severe and/or rapid
onset, with low prevalence of ILD or Raynaud’s phenomenon.
The most common Ab in patients with necrotizing myopathy.
anti-SRP is specific for PM and associated with treatment-resistant severe myopathy,
which is histologically characterized by necrotizing myopathy
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-Mi-2
Anti-Mi-2 was associated with classic DM (classic features of DM including Gottron’s
papules, heliotrope rash, shawl sign, and V-sign), but a risk to develop clinically
significant ILD is low and cancer is uncommon, good response to steroids, and
good prognosis.
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-MDA5/CADM140 (anti-melanoma differentiation-associated gene 5):
A subset of DM patients may have typical DM skin rash but have little or no muscle
involvement (Amyopathic DM).
Anti-CADM 140: A subset of CADM may develop rapidly progressive interstitial lung
disease, resistant to treatment and with poor prognosis.
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-TIF1γ/α and β (Antibodies to transcription intermediary factor 1γ/α):
TIF1α, TIF1β, and TIF1γ belong to the TIF family of transcription cofactors
It has a striking association with cancer-associated DM (42–100 %).
Almost all anti-TIF1γ/α positive patients have DM with typical skin rash but a low
prevalence of ILD.
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-MJ/NXP-2
nuclear matrix protein. NXP-2 localizes in the promyelocytic leukemia (PML) nuclear
bodies, where it recruits and activates p53 to induce cellular senescence.
Anti-MJ/NXP-2-positive patients showed typical DM skin rash with a higher
prevalence of ILD, and was specifically associated with cancer in males.
Absent in PM.
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-SAE (small ubiquitin-like modifier-activating enzyme)
SAE-1: small ubiquitin-like modifier-activating enzyme A subunit
SAE-2: SUMO-1(small ubiquitin-like modifier-1) activating enzyme B subunit
Found in DM but not PM.
In patients with anti-SAE, a high frequency of cutaneous lesions including
heliotrope and Gottron rash were identified, patients with anti-SAE, a high
frequency of cutaneous lesions including heliotrope (82 %) and Gottron rash (82 %)
were identified
MYOSITIS-SPECIFIC ANTIBODIES
• Anti-Cn1A (antibody against cytosolic 5’nucleotidase 1A):
In IBM
(II) MUSCULAR DYSTROPHIES
• Addition of these new antibodies to clinical practice in the future will help in
making earlier and more accurate diagnoses and better management for patients.
IS IT APPLICABLE?
REFERENCES
• LUNDBERG IE, MILLER FW, TJÄRNLUND A, BOTTAI M. DIAGNOSIS AND CLASSIFICATION OF IDIOPATHIC
INFLAMMATORY MYOPATHIES. J INTERN MED. 2016;280(1):39-51. DOI:10.1111/JOIM.12524
• LUNDBERG, I. E., TJÄRNLUND, A., BOTTAI, M., ET AL., … INTERNATIONAL MYOSITIS CLASSIFICATION CRITERIA
PROJECT CONSORTIUM, THE EUROMYOSITIS REGISTER AND THE JUVENILE DERMATOMYOSITIS COHORT
BIOMARKER STUDY AND REPOSITORY (JDRG) (UK AND IRELAND) (2017). 2017 EUROPEAN LEAGUE AGAINST
RHEUMATISM/AMERICAN COLLEGE OF RHEUMATOLOGY CLASSIFICATION CRITERIA FOR ADULT AND JUVENILE
IDIOPATHIC INFLAMMATORY MYOPATHIES AND THEIR MAJOR SUBGROUPS. ANNALS OF THE RHEUMATIC
DISEASES, 76(12), 1955–1964
• SATOH, M., TANAKA, S., CERIBELLI, A., CALISE, S. J., & CHAN, E. K. (2017). A COMPREHENSIVE OVERVIEW ON
MYOSITIS-SPECIFIC ANTIBODIES: NEW AND OLD BIOMARKERS IN IDIOPATHIC INFLAMMATORY
MYOPATHY. CLINICAL REVIEWS IN ALLERGY & IMMUNOLOGY, 52(1), 1–19.
• MALAVIYA, ANAND N; KAPOOR, SANJIV. ROLE OF MYOSITIS-SPECIFIC AUTOANTIBODIES IN PERSONALIZED
THERAPY. INDIAN JOURNAL OF RHEUMATOLOGY 13(3):P 186-194, SEPTEMBER 2018. | DOI:
10.4103/INJR.INJR_135_17
• FARINI, A., VILLA, C., TRIPODI, L., LEGATO, M., & TORRENTE, Y. (2021). ROLE OF IMMUNOGLOBULINS IN MUSCULAR
DYSTROPHIES AND INFLAMMATORY MYOPATHIES. FRONTIERS IN IMMUNOLOGY, 12, 666879.
HTTPS://DOI.ORG/10.3389/FIMMU.2021.666879
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THE ROLE OF ANTIBODIES IN MUSCLE DISORDERS

  • 1. ROLE OF ANTIBODIES IN MUSCLE DISEASES MOHAMED E. ABD-ELHADY, MSC APRIL 2023
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  • 8. INFLAMMATORY MYOPATHIES • Dermatomyositis, Polymyositis, and Inclusion Body Myositis (IBM) • Immune Mediated Necrotizing Myopathy (IMNM): AB against HMG-CoA reductases. • Systemic Autoimmune Rheumatic Diseases (SARD) • Overlap Syndrome and ADM/CADM • The main concern is their association with tumors and/or auto-autoimmune disorders, which guides the investigations and management.
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  • 11. ANTIBODIES IN INFLAMMATORY MYOPATHIES • Myositis-Specific Antibodies (MSA) and Myositis-Associated Antibodies (MAA). • MSA: is defined as autoantibody specificities that are considered relatively specific for PM/DM. • MAA: autoantibody specificity found in PM/DM but not specific for this diagnosis and may be found in other SARD
  • 12. • Role of AB in inflammatory myopathies: I) For associated autoimmune disease (MAA): ESR, RF, ANA, ANCA C & P, anti- Ds-DNA, anti phospholipid AB, anti-PM-Scl, anti-Ku, anti- U1ribonucleoprotein (RNP) U1/U2RNP, anti-Ro 60 and anti-La. II) For associated malignancies: Tumor Markers
  • 13. MYOSITIS-SPECIFIC ANTIBODIES • Anti-ARS (aminoacyl tRNA synthetases): autoantibodies that recognize the cytoplasmic amino acid-charging enzymes, aminoacyl tRNA synthetases. Eight of them including histidyl (Jo-1), threonyl (PL-7), alanyl (PL-12), glycyl (EJ), isoleucyl (OJ), asparaginyl (KS), phenylalanyl (ZO), and tyrosyl (YRS/HA) tRNA synthetases have been reported. They can be further classified into either anti-Jo-1 or anti-non-Jo-1 Abs. Anti-Jo-1 (anti-synthetase syndrome) is the 1st identified MSA and is associated with ILD, polyarteritis, and Raynaud’s phenomenon. Anti-Jo-1 antibodies, usually found in 15–25 % of PM/DM patients, are by far the most common among anti-ARS antibodies; all others are usually found only in 0.5– 6 % of patients
  • 14. MYOSITIS-SPECIFIC ANTIBODIES • Anti-ARS (aminoacyl tRNA synthetases): anti-PL-7/PL-12 was associated with early and severe ILD and less myositis (CADM). In summary, patients with any anti-ARS have a similar clinical syndrome known as anti- synthetase syndrome; however, several recent studies suggest that antibodies to non-Jo-1 ARS are associated with earlier and more severe ILD and poor prognosis compared with anti-Jo-1 (+) patients. Also, non-Jo-1 anti-ARS (+) patients are more likely to have ILD without typical myositis.
  • 15. MYOSITIS-SPECIFIC ANTIBODIES • Anti-SRP (anti-signal recognition particle): anti-SRP is associated with classic PM and some were unusually severe and/or rapid onset, with low prevalence of ILD or Raynaud’s phenomenon. The most common Ab in patients with necrotizing myopathy. anti-SRP is specific for PM and associated with treatment-resistant severe myopathy, which is histologically characterized by necrotizing myopathy
  • 16. MYOSITIS-SPECIFIC ANTIBODIES • Anti-Mi-2 Anti-Mi-2 was associated with classic DM (classic features of DM including Gottron’s papules, heliotrope rash, shawl sign, and V-sign), but a risk to develop clinically significant ILD is low and cancer is uncommon, good response to steroids, and good prognosis.
  • 17. MYOSITIS-SPECIFIC ANTIBODIES • Anti-MDA5/CADM140 (anti-melanoma differentiation-associated gene 5): A subset of DM patients may have typical DM skin rash but have little or no muscle involvement (Amyopathic DM). Anti-CADM 140: A subset of CADM may develop rapidly progressive interstitial lung disease, resistant to treatment and with poor prognosis.
  • 18. MYOSITIS-SPECIFIC ANTIBODIES • Anti-TIF1γ/α and β (Antibodies to transcription intermediary factor 1γ/α): TIF1α, TIF1β, and TIF1γ belong to the TIF family of transcription cofactors It has a striking association with cancer-associated DM (42–100 %). Almost all anti-TIF1γ/α positive patients have DM with typical skin rash but a low prevalence of ILD.
  • 19. MYOSITIS-SPECIFIC ANTIBODIES • Anti-MJ/NXP-2 nuclear matrix protein. NXP-2 localizes in the promyelocytic leukemia (PML) nuclear bodies, where it recruits and activates p53 to induce cellular senescence. Anti-MJ/NXP-2-positive patients showed typical DM skin rash with a higher prevalence of ILD, and was specifically associated with cancer in males. Absent in PM.
  • 20. MYOSITIS-SPECIFIC ANTIBODIES • Anti-SAE (small ubiquitin-like modifier-activating enzyme) SAE-1: small ubiquitin-like modifier-activating enzyme A subunit SAE-2: SUMO-1(small ubiquitin-like modifier-1) activating enzyme B subunit Found in DM but not PM. In patients with anti-SAE, a high frequency of cutaneous lesions including heliotrope and Gottron rash were identified, patients with anti-SAE, a high frequency of cutaneous lesions including heliotrope (82 %) and Gottron rash (82 %) were identified
  • 21. MYOSITIS-SPECIFIC ANTIBODIES • Anti-Cn1A (antibody against cytosolic 5’nucleotidase 1A): In IBM
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  • 30. • Addition of these new antibodies to clinical practice in the future will help in making earlier and more accurate diagnoses and better management for patients.
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  • 34. REFERENCES • LUNDBERG IE, MILLER FW, TJÄRNLUND A, BOTTAI M. DIAGNOSIS AND CLASSIFICATION OF IDIOPATHIC INFLAMMATORY MYOPATHIES. J INTERN MED. 2016;280(1):39-51. DOI:10.1111/JOIM.12524 • LUNDBERG, I. E., TJÄRNLUND, A., BOTTAI, M., ET AL., … INTERNATIONAL MYOSITIS CLASSIFICATION CRITERIA PROJECT CONSORTIUM, THE EUROMYOSITIS REGISTER AND THE JUVENILE DERMATOMYOSITIS COHORT BIOMARKER STUDY AND REPOSITORY (JDRG) (UK AND IRELAND) (2017). 2017 EUROPEAN LEAGUE AGAINST RHEUMATISM/AMERICAN COLLEGE OF RHEUMATOLOGY CLASSIFICATION CRITERIA FOR ADULT AND JUVENILE IDIOPATHIC INFLAMMATORY MYOPATHIES AND THEIR MAJOR SUBGROUPS. ANNALS OF THE RHEUMATIC DISEASES, 76(12), 1955–1964 • SATOH, M., TANAKA, S., CERIBELLI, A., CALISE, S. J., & CHAN, E. K. (2017). A COMPREHENSIVE OVERVIEW ON MYOSITIS-SPECIFIC ANTIBODIES: NEW AND OLD BIOMARKERS IN IDIOPATHIC INFLAMMATORY MYOPATHY. CLINICAL REVIEWS IN ALLERGY & IMMUNOLOGY, 52(1), 1–19. • MALAVIYA, ANAND N; KAPOOR, SANJIV. ROLE OF MYOSITIS-SPECIFIC AUTOANTIBODIES IN PERSONALIZED THERAPY. INDIAN JOURNAL OF RHEUMATOLOGY 13(3):P 186-194, SEPTEMBER 2018. | DOI: 10.4103/INJR.INJR_135_17 • FARINI, A., VILLA, C., TRIPODI, L., LEGATO, M., & TORRENTE, Y. (2021). ROLE OF IMMUNOGLOBULINS IN MUSCULAR DYSTROPHIES AND INFLAMMATORY MYOPATHIES. FRONTIERS IN IMMUNOLOGY, 12, 666879. HTTPS://DOI.ORG/10.3389/FIMMU.2021.666879