Highly variable mutational profile of ASXL1 in myelofibrosis.

Objective Somatic mutations in ASXL1 seem to have a negative prognostic impact in patients with several myeloid neoplasms, including myelofibrosis ( MF). The aim of this work was to determine the prevalence and profile of ASXL1 mutations in MF. Methods We analyzed mutations in ASXL1 in 70 consecutive MF patients from 8 Spanish hospitals by means of Sanger sequencing, as well as JAK2, CALR , and MPL mutations. Results ASXL1 mutations were found in 16/70 (23%) of cases, most commonly p.Gly646TrpfsX12 (5/16). Most mutations (13/16) were frameshift mutations. Of 54 ASXL1- wild-type patients, 32 (59%) had at least one single nucleotide polymorphism ( SNP), 27 of them had g.78128 C> T, g.79017 A> C, and g.79085 T> C [triple SNP ( TSNP) patients]. The 5-yr overall survival probability of TSNP patients was 67% (95% CI, 43-91%) vs. 90% (95% CI, 77-100%) in ASXL1- WT patients ( P = 0.152). Conclusion ASXL1 mutations were found in 23% of cases, p.Gly646TrpfsX12 being the most frequent. About 85% of mutations were found only in individual cases and 46% had not previously been reported, a pattern also seen in other series. Fifty percent of ASXL1- WT patients had a combination of three specific SNPs that might have a prognostic correlation that needs to be determined in larger series. [ABSTRACT FROM AUTHOR]