Clinical Features and Genomic Landscape of Myeloproliferative Neoplasm (MPN) Patients with Autoimmune and Inflammatory Diseases (AID)

Author:

Elessa Dikelele1ORCID,Zhao Lin-Pierre2ORCID,de Oliveira Rafael Daltro3,Maslah Nabih4,Soret Juliette3,VERGER Emmanuelle5,Marcault Clémence3,Parquet Nathalie6,Fenaux Pierre7,Adès Lionel8ORCID,Raffoux Emmanuel9,GIRAUDIER Stéphane10ORCID,Fain Olivier11,Cassinat Bruno12,Kiladjian Jean-Jacques13,MEKINIAN Arsène14ORCID,Benajiba Lina15

Affiliation:

1. Sorbonne Université, Service de médecine interne et inflammation, Saint-Antoine hospital

2. Université Paris Cité, Saint-Louis hospital, APHP

3. Université Paris Cité, Clinical Investigations Center, Saint-Louis hospital, APHP

4. INSERM U1131

5. INSERM U1133

6. Saint Louis Hospital

7. Hôpital Saint-Louis, Université Paris 7

8. St Louis Hospital

9. Hopital Saint-Louis and Paris University

10. Saint Louis Hospital, APHP

11. Hôpital Saint Antoine, Assistance Publique des Hôpitaux de Paris, université Paris VI Sorbonne

12. AP-HP, Hopital Saint-Louis

13. Hôpital Saint-Louis et Université Paris Diderot

14. Hôpital Saint-Antoine

15. Université de Paris, Hôpital Saint-Louis, AP-HP, Paris, FRANCE

Abstract

Abstract There are few data regarding the association of autoimmune and inflammatory diseases (AID) with Philadelphia negative myeloproliferative neoplasms (MPN). In this retrospective study, we describe the prevalence, clinical and biological features and outcome of AID association in MPN. A total of 1541 MPN patients were included, encompassing 95 (6%) patients with AID. Female patients were predominant within the AID group (65% versus 54%, p=0.03). A total of 103 AID diagnoses were reported in 95 patients, including 48 organ-specific AID, 13 inflammatory arthritis, 9 connective tissue diseases, 9 dermatosis, 6 systemic vasculitis and 18 unclassified AID. The prevalence of TET2 mutations was higher in the AID cohort (32% versus 22%), although not statistically significant (p=0.08). In subgroup analysis of patients with myelofibrosis, TET2 mutations were more prevalent in AID group (p=0.025). The prevalence of driver and other additional mutations did not differ between the 2 groups. The association with AID did not impact overall survival (p=0.67), transformation-free survival (p=0.37) or secondary myelofibrosis-free survival (p=0.91). Our data suggest that the prevalence of AID is similar in MPN patients to that of the general population. TET2 mutations are highly prevalent in MPN patients with AID potentially suggesting a shared physiopathology.

Publisher

Research Square Platform LLC

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