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Anti NXP2 myositis - A
review
RITASMAN BAISYA
Introduction
NXP-2 (anti-MJ) antibody targeting NXP2( nuclear matrix protein )
A myositis-specific antibody ( MSA )
Common in juvenile dermatomyositis patients, found in adults also
Association with calcinosis and malignancy
Severe muscle weakness and edema are important feature
Potential for gastrointestinal involvement
/
Aouizerate, J. et al. Muscle ischaemia associated with NXP2 autoantibodies: a severe subtype of juvenile
dermatomyositis. Rheumatology
Results
MSAs ( anti-NXP2 (9/23), anti-TIF1g (4/23), anti-MDA5 (2/23)) and no MSAs
(8/23) yielded two histopathological clusters.
Compared with cluster 2, patients in cluster 1 had-
1. Strikingly more often antiNXP2 antibodies (7/11 in cluster 1 vs 2/12 in cluster2 ),
2. More pronounced muscle weakness,
3. More gastrointestinal involvement
4. Required more aggressive treatment
Cluster 1 – more NXP2 positive patients , more severe disease
Cluster 1 (n = 11) with more NXP2 positivity showed a more severe and ischaemic pattern than
cluster 2 (n = 12) assessed by:
1. Total score severity > 20 (100.0% vs 25.0%);
2. Visual analogic score >6 (100.0% vs 25.0%);
3. The vascular domain score >1 (100.0% vs 41.7%);
4. Microinfarcts (100% vs 58.3%);
5. Ischaemic myofibrillary loss (focal punched-out vacuoles) (90.9 vs 25%) ,
6. Obvious capillary loss (81.8% vs 16.7)
Cluster 1 with more NXP2 positive
patients had more severe muscle
disease
D- CMAS (P = 0.003) and E- the % of patients in remission over a 1-year follow-up (P = 0.043). Dark blue
shading represents the NXP2+ group (9/23).
NXP2-positive subjects were more likely to present severe muscle involvement (MMT, P = 0.014; CMAS, P =
0.003) and required more treatment lines (P = 0.028)
Albayda J, Pinal-Fernandez I, Huang W, et al. Antinuclear Matrix Protein 2 Autoantibodies and Edema,
Muscle Disease, and Malignancy Risk in Dermatomyositis Patients. Arthritis Care Res (Hoboken).
2017;69(11):1771-1776. doi:10.1002/acr.23188
Results
In anti NXP2 group -
More severe muscle weakness .
More distal arm weakness (35% vs. 20%, p=0.02) & distal leg weakness
More neck weakness (48% vs. 23%, p<0.001)
More likely to present with myalgias (46% vs. 25%, p=0.002) and
develop dysphagia
No evidence for more diaphragmatic weakness
tMRIs showed increased muscle atrophy
Extramuscular features
Subcutaneous edema - 36% of patients with anti-NXP2 & 19% of anti-NXP-2-negative
patients
Calcinosis was more common in adult patients with anti-NXP-2 autoantibodies (30% vs
17%, p=0.02)
Patients with anti-NXP2 were found to have a 3.68-fold increased risk of cancer (95%CI
1.2-8.6).
Tansley et al , Juvenile Dermatomyositis Research Group. Calcinosis in juvenile dermatomyositis is influenced
by both anti-NXP2 autoantibody status and age at disease onset. Rheumatology (Oxford). 2014
Dec;53(12):2204-8.
Results
Anti-NXP2 autoantibodiess substantially increased the risk of calcinosis across all
ages (P = 0.025)
They were detectable prior to calcinosis development
Children with anti-NXP2 autoantibodies had a greater degree of weakness (median
lowest CMAS ever 29.6 vs 42)
They were less likely to be in remission at 2 years post-diagnosis.
Demographic data in NXP2 patients
• Anti-NXP2 seemed to be the most common antibody (30.6%) in the cohort
• Anti-NXP2 antibody-positive JDM of Chinese children was characterized by rash and
severe muscle weakness.
• Calcification high in NXP2 group .
• ILD in anti NXP2 is mild
Take home points
1. Anti-NXP2 autoantibodies ( originally called anti-MJ )were first reported in JDM cohort
2. They target NXP2 (MORC3), a protein involved in transcriptional regulation
3. First regarded as more specifically associated with calcinosis in JDM
4. They are also detected in adults & associated with malignancy
5. Muscle pain, subcutaneous edema, dysphagia, and both proximal and distal muscle
weakness
6. can be considered as complementary biomarkers associated with clinical severity and
poor prognosis

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Presentation1.pptx

  • 1. Anti NXP2 myositis - A review RITASMAN BAISYA
  • 2. Introduction NXP-2 (anti-MJ) antibody targeting NXP2( nuclear matrix protein ) A myositis-specific antibody ( MSA ) Common in juvenile dermatomyositis patients, found in adults also Association with calcinosis and malignancy Severe muscle weakness and edema are important feature Potential for gastrointestinal involvement
  • 3. / Aouizerate, J. et al. Muscle ischaemia associated with NXP2 autoantibodies: a severe subtype of juvenile dermatomyositis. Rheumatology
  • 4. Results MSAs ( anti-NXP2 (9/23), anti-TIF1g (4/23), anti-MDA5 (2/23)) and no MSAs (8/23) yielded two histopathological clusters. Compared with cluster 2, patients in cluster 1 had- 1. Strikingly more often antiNXP2 antibodies (7/11 in cluster 1 vs 2/12 in cluster2 ), 2. More pronounced muscle weakness, 3. More gastrointestinal involvement 4. Required more aggressive treatment
  • 5. Cluster 1 – more NXP2 positive patients , more severe disease Cluster 1 (n = 11) with more NXP2 positivity showed a more severe and ischaemic pattern than cluster 2 (n = 12) assessed by: 1. Total score severity > 20 (100.0% vs 25.0%); 2. Visual analogic score >6 (100.0% vs 25.0%); 3. The vascular domain score >1 (100.0% vs 41.7%); 4. Microinfarcts (100% vs 58.3%); 5. Ischaemic myofibrillary loss (focal punched-out vacuoles) (90.9 vs 25%) , 6. Obvious capillary loss (81.8% vs 16.7)
  • 6. Cluster 1 with more NXP2 positive patients had more severe muscle disease
  • 7. D- CMAS (P = 0.003) and E- the % of patients in remission over a 1-year follow-up (P = 0.043). Dark blue shading represents the NXP2+ group (9/23). NXP2-positive subjects were more likely to present severe muscle involvement (MMT, P = 0.014; CMAS, P = 0.003) and required more treatment lines (P = 0.028)
  • 8. Albayda J, Pinal-Fernandez I, Huang W, et al. Antinuclear Matrix Protein 2 Autoantibodies and Edema, Muscle Disease, and Malignancy Risk in Dermatomyositis Patients. Arthritis Care Res (Hoboken). 2017;69(11):1771-1776. doi:10.1002/acr.23188
  • 9. Results In anti NXP2 group - More severe muscle weakness . More distal arm weakness (35% vs. 20%, p=0.02) & distal leg weakness More neck weakness (48% vs. 23%, p<0.001) More likely to present with myalgias (46% vs. 25%, p=0.002) and develop dysphagia No evidence for more diaphragmatic weakness tMRIs showed increased muscle atrophy
  • 10. Extramuscular features Subcutaneous edema - 36% of patients with anti-NXP2 & 19% of anti-NXP-2-negative patients Calcinosis was more common in adult patients with anti-NXP-2 autoantibodies (30% vs 17%, p=0.02) Patients with anti-NXP2 were found to have a 3.68-fold increased risk of cancer (95%CI 1.2-8.6).
  • 11. Tansley et al , Juvenile Dermatomyositis Research Group. Calcinosis in juvenile dermatomyositis is influenced by both anti-NXP2 autoantibody status and age at disease onset. Rheumatology (Oxford). 2014 Dec;53(12):2204-8.
  • 12. Results Anti-NXP2 autoantibodiess substantially increased the risk of calcinosis across all ages (P = 0.025) They were detectable prior to calcinosis development Children with anti-NXP2 autoantibodies had a greater degree of weakness (median lowest CMAS ever 29.6 vs 42) They were less likely to be in remission at 2 years post-diagnosis.
  • 13. Demographic data in NXP2 patients
  • 14. • Anti-NXP2 seemed to be the most common antibody (30.6%) in the cohort • Anti-NXP2 antibody-positive JDM of Chinese children was characterized by rash and severe muscle weakness. • Calcification high in NXP2 group . • ILD in anti NXP2 is mild
  • 15. Take home points 1. Anti-NXP2 autoantibodies ( originally called anti-MJ )were first reported in JDM cohort 2. They target NXP2 (MORC3), a protein involved in transcriptional regulation 3. First regarded as more specifically associated with calcinosis in JDM 4. They are also detected in adults & associated with malignancy 5. Muscle pain, subcutaneous edema, dysphagia, and both proximal and distal muscle weakness 6. can be considered as complementary biomarkers associated with clinical severity and poor prognosis