ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 908

Early Prediction of Long-Term Evolutionary Profiles of Eosinophilic Granulomatosis with Polyangiitis (Churg–Strauss) Based on Baseline and Follow-up Characteristics

Matthias Papo1, Giacomo Emmi2, Franco Schiavon3, Matthieu Groh4, Maria-Letizia Urban2, Chiara Marvisi5, Jean-Emmanuel Kahn4, Alberto Sinico6, Maxime Samson7, Pascal Cohen1, Xavier Puéchal1, Luc Mouthon1, Loïc Guillevin1, Augusto Vaglio5 and Benjamin Terrier8, 1Department of Internal Medicine, INSERM Unité 1016, Centre de Référence pour les Maladies Auto-immunes Rares, Hôpital Cochin, Université Paris Descartes, Sorbonne Paris Cité, Paris, France, 2Department of Experimental and Clinical Medicine, University of Florence, Florence, Italy, 3Operative Unit of Rheumatology, Department of Medicine DIMED, University of Padova, Padova, Italy, 4Service de Médecine Interne, Centre de Référence des Syndromes Hyperéosinophiliques-CEREO, Hôpital Foch, Université Versailles–Saint-Quentin-en-Yvelines, Suresnes, France, 5Nephrology Unit, Parma University Hospital, Parma, Italy, 6UOS di Immunologia Clinica e UOC di Nefrologia, Azienda Ospedaliera San Carlo Borromeo, Milan, Italy, 7Department of Internal Medicine and Clinical Immunology, François-Mitterrand Teaching Hospital, University of Bourgogne-Franche-Comté, Dijon, France, 8Department of Internal Medicine, Centre de Référence pour les Maladies Auto-immunes Rares, Paris, France, Hôpital Cochin, Université Paris Descartes, Sorbonne Paris Cité, Paris, France

Meeting: 2018 ACR/ARHP Annual Meeting

Keywords:

Session Information

Date: Sunday, October 21, 2018

Title: 3S090 ACR Abstract: Vasculitis–ANCA-Assocd (904–909)

Session Type: ACR Concurrent Abstract Session

Session Time: 2:30PM-4:00PM

Background/Purpose: Eosinophilic granulomatosis with polyangiitis (EGPA) (Churg–Strauss) is a small-vessel necrotizing vasculitis characterized by blood and tissue eosinophilia and asthma. Glucocorticoids (GCs) effectively control the disease, but relapses and/or GC-dependence are frequent. Recently, efforts were made to improve nosology of EGPA patients. Evolving concepts tend to distinguish vasculitis-related symptoms from asthma and/or ENT manifestations. That distinction has become even more important, since the development of new targeted biotherapies. This study aimed to describe and identify characteristics predicting long-term EGPA outcomes.

Methods: We created a multicenter European collaborative initiative that included 257 EGPA patients from tertiary referral centers. Based on recent consensus, we distinguished 4 EGPA-evolutionary profiles: GC-dependent asthma and/or ENT manifestations (requiring prednisone >7.5 mg/d), at least 1 vasculitis relapse (excluding asthma and/or ENT manifestations), both phenotypes, and prolonged remission (no GC-dependent asthma/ENT signs and no vasculitis relapse). Baseline and follow-up characteristics predicting those outcomes were analyzed.

Results: After median follow-up of 60 months, 24% had GC-dependent asthma and/or ENT manifestations, 18% had at least 1 vasculitis relapse, 8% had both phenotypes, and 50% were in prolonged remission (Table). Patients with GC-dependent asthma/ENT manifestations were younger at diagnosis, had more frequent asthma requiring GCs before overt EGPA and pulmonary infiltrates, less frequent general symptoms and ANCA-positivity, and tended to have lower eosinophil counts. Their daily GC dose and eosinophil counts were higher at every time point; at last follow-up, they had more active asthma and less frequent neurological sequelae. In contrast, patients with only vasculitis relapse(s) had more frequent general symptoms at diagnosis, ANCA-positivity and higher BVAS, and less frequent pulmonary infiltrates. Median diagnosis-to-1st-vasculitis-relapse interval was 15 (9–42) months. During follow-up, their daily GC dose was lower than for those with GC-dependent asthma and/or ENT manifestations but similar to that of those in prolonged remission. At last follow-up, neurological sequelae were more frequent but active asthma less common. Finally, patients in prolonged remission were older, had less frequent asthma requiring GCs before EGPA, and lower daily GC dose and eosinophil counts during follow-up and less frequent sequelae.

Conclusion: Distinct baseline and follow-up characteristics defined 4 evolutionary EGPA profiles predicting patients’ long-term outcomes. Each evolutionary pattern was identifiable soon after diagnosis, which would allow early choices of the best therapeutic option in the future.


Table

Evolutionary profile

Characteristic

Prolonged remission (n=129)

GC-dependent asthma/ENT (n=62)

Vasculitis relapse (n=45)

GC-dependent asthma/ENT & vasculitis relapse (n=21)

P

Age at diagnosis, yr

57 (44–67)

47 (36–58.2)

52 (44.5–66.5)

43 (31.5–52.2)

<0.0001

Asthma before EGPA

109/129 (84.5)

55/59 (93.2)

36/45 (80)

21/21 (100)

0.0498

Asthma duration, yr

5 (2.1–15.4)

5 (2–14.7)

3 (1–10.3)

2 (1–4.3)

0.02

General symptoms

102/129 (79.1)

41/62 (66.1)

39/45 (86.7)

13/21 (61.9)

0.03

Manifestation

Cutaneous

45/129 (34.9)

24/62 (38.7)

22/45 (48.9)

8/21 (38.1)

0.43

ENT

91/129 (70.5)

48/62 (77.4)

35/45 (77.8)

15/21 (71.4)

0.67

Pulmonary

123/129 (95.3)

61/62 (98.4)

44/45 (97.8)

21/21 (100)

0.52

Infiltrates

74/129 (57.4)

38/62 (61.2)

19/45 (42.2)

17/21 (81)

0.024

Cardiac

39/129 (30.2)

25/62 (40.3)

16/45 (35.6)

7/21 (33.3)

0.57

Gastrointestinal

30/129 (23.3)

10/62 (16.1)

9/45 (20)

3/21 (14.3)

0.81

Renal

23/129 (17.8)

7/62 (11.3)

8/45 (17.8)

3/21 (14.3)

0.68

Neurological

87/129 (67.4)

34/62 (54.8)

35/45 (77.8)

15/21 (71.4)

0.084

ANCA+

52/129 (40.3)

14/61 (23)

22/45 (48.9)

9/21 (42.9)

0.034

Anti-MPO+

40/106 (37.7)

7/39 (17.9)

18/39 (46.2)

8/16 (50.0)

0.026

CRP, mg/L

35 (13–75)

35 (15–84.2)

59 (29–91)

11 (3.5–49)

0.055

Eosinophils, /mm3

6680 (3000–11300)

4000 (2185–9125)

4500 (1808–10093)

3900 (1940–6187)

0.055

BVAS

16 (9–21)

10.5 (6–20)

17 (11–23.5)

15 (8–24)

0.038

Deaths

10/119 (8.4)

3/62 (4.8)

2/45 (4.4)

1/21 (4.8)

0.7

GC dose, mg/d

At 6 months

10 (7–12.8)

14.5 (10–20)

8 (6–20)

16.2 (10–20)

0.0007

A 24 months

5 (5–7)

10 (6–15)

8.2 (5–10.5)

21 (10–40)

<0.0001

Eosinophils, /mm3

At 6 months

300 (100–540)

490 (104–980)

628 (142–1422)

610 (288–3300)

0.046

 At 60 months

472 (300–847)

900 (400–1200)

568 (409–2235)

1220 (825–6250)

0.065

At last follow-up

GC dose, mg/d

5 (3–7)

10 (6.7–12.5)

5 (4–10)

10 (7.5–23)

<0.0001

No GCs

25/123 (20.3)

2/61 (3.3)

6/44 (13.6)

0/21 (0)

0.0031

EGPA sequelae

48/84 (57.1)

54/58 (93.1)

13/21 (61.9)

17/20 (85)

0.0007

Values are expressed as n (%) or median [IQR], with respective P values computed with c2 or Kruskall–Wallis test.

Disclosure: M. Papo, None; G. Emmi, None; F. Schiavon, None; M. Groh, None; M. L. Urban, None; C. Marvisi, None; J. E. Kahn, None; A. Sinico, None; M. Samson, None; P. Cohen, None; X. Puéchal, None; L. Mouthon, None; L. Guillevin, None; A. Vaglio, None; B. Terrier, None.

To cite this abstract in AMA style:

Papo M, Emmi G, Schiavon F, Groh M, Urban ML, Marvisi C, Kahn JE, Sinico A, Samson M, Cohen P, Puéchal X, Mouthon L, Guillevin L, Vaglio A, Terrier B. Early Prediction of Long-Term Evolutionary Profiles of Eosinophilic Granulomatosis with Polyangiitis (Churg–Strauss) Based on Baseline and Follow-up Characteristics [abstract]. Arthritis Rheumatol. 2018; 70 (suppl 9). https://acrabstracts.org/abstract/early-prediction-of-long-term-evolutionary-profiles-of-eosinophilic-granulomatosis-with-polyangiitis-churg-strauss-based-on-baseline-and-follow-up-characteristics/. Accessed .

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