Systemic sclerosis sine scleroderma: clinical and serological features and relationship with other cutaneous subsets in a large series of patients from the national registry 'SPRING' of the Italian Society for Rheumatology

De Angelis, R.; Ferri, C.; Giuggioli, D.; Bajocchi, G.; Dagna, L.; Bellando-Randone, S.; Zanframundo, G.; Foti, R.; Cacciapaglia, F.; Cuomo, G.; Ariani, A.; Rosato, E.; Lepri, G.; Girelli, F.; Riccieri, V.; Zanatta, E.; Bosello, S. L.; Cavazzana, I.; Ingegnoli, F.; De Santis, M.; Murdaca, G.; Abignano, G.; Romeo, N.; Della Rossa, A.; Caminiti, M.; Iuliano, A. M.; Ciano, G.; Beretta, L.; Bagnato, G.; Lubrano, E.; De Andres, I.; Giollo, A.; Saracco, M.; Agnes, C.; Cipolletta, E.; Lumetti, F.; Spinella, A.; Magnani, L.; Campochiaro, C.; De Luca, G.; Codullo, V.; Visalli, E.; Di Vico, C.; Gigante, A.; Pellagrino, G.; Pigatto, E.; Lazzaroni, M. -G.; Franceschini, F.; Generali, E.; Mennillo, G.; Barsotti, S.; Mariano, G. P.; Furini, F.; Vultaggio, L.; Parisi, S.; Peroni, C. L.; Rozza, D.; Zanetti, A.; Carrara, G.; Landolfi, G.; Scire, C. A.; Bianchi, G.; Fusaro, E.; Sebastiani, G. D.; Govoni, M.; D'Angelo, S.; Cozzi, F.; Guiducci, S.; Doria, A.; Salvarani, C.; Iannone, F.; Matucci-Cerinic, M.

doi:10.1136/rmdopen-2022-002890

OBJECTIVE: To describe demographic, clinical and laboratory features of systemic sclerosis sine scleroderma (ssSSc) in a large multicentre systemic sclerosis (SSc) cohort. METHODS: Data involving 1808 SSc patients from Italian Systemic sclerosis PRogression INvestiGation registry were collected. The ssSSc was defined by the absence of any cutaneous sclerosis and/or puffy fingers. Clinical and serological features of ssSSc were compared with limited cutaneous (lcSSc) and diffuse cutaneous (dcSSc) subsets. RESULTS: Among patients with SSc, only 61 (3.4%) were classified as having ssSSc (F/M=19/1). Time from Raynaud's phenomenon (RP) onset to diagnosis was longer in ssSSc (3 years, IQR 1-16.5) than lcSSc (2 years, IQR 0-7), and dcSSc (1 year, IQR 0-3) (p<0.001). Clinical ssSSc phenotype was comparable to lcSSc, except for digital pitting scars (DPS) (19.7% vs 42%, p=0.01), but significantly milder than dcSSc, particularly for digital ulcers (DU) (6.6% vs 35.7%, p<0.001), oesophagus (46.2% vs 63.5%, p=0.009), lung (mean diffusion capacity for carbon monoxide 72.2±19.6 vs 62.4±22.8, p=0.009; mean forced vital capacity 105.6±21.7 vs 89.2±20.9, p<0.001) and major videocapillaroscopic alterations (late pattern 8.6% vs 47.6%, p<0.001). Moreover, in ssSSc the percentages of anticentromere and antitopoisomerase were comparable to lcSSc (40% and 18.3% vs 36.7% and 26.6%), but divergent respect to dcSSc (8.6% and 67.4%, p<0.001). CONCLUSION: The ssSSc is a quite rare disease variant characterised by clinico-serological features comparable to lcSSc, but significantly different from dcSSc. Overall, longer RP duration, low percentages of DPS and peripheral microvascular abnormalities, and increased anti-centromere seropositivity distinguish ssSSc. Further investigations based on national registries might provide useful insights on the actual relevance of the ssSSc within the scleroderma spectrum.