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. 2015 Jun 5;6(21):18250–18264. doi: 10.18632/oncotarget.4213

Table 2. Categories of mastocytosis and corresponding type of KIT mutations.

Type of Mastocytosis Prognosis Treatment options Type/frequency of KIT and other genetic lesions
Pediatric mastocytosis (PM) Very Good Most cases regress with age 25% KIT WT
35% KIT D816V/I/Y
40% ECD KIT mutations
Indolent mastocytosis (ISM) Very good to good No cytoreductive therapy necessary > 80% KIT D816V mutations
Smoldering systemic mastocytosis (SSM) Relatively good ‘Wait and watch’ in most cases, some may require Interferon (IFN), glucocorticosteriods and cladribine (2CdA) > 80% KIT D816V mutations
Additional non-KIT mutations acquired over disease progression
Aggressive systemic mastocytosis (ASM) Poor IFN, 2CdA; resistant forms treated with TKIs/chemotherapy/hydroxyurea > 60% KIT D816V mutations
Few non-codon 816 KIT mutations
Additional non-KIT mutations
(D820G, V559I)
Systemic mastocytosis with associated non-hematological MC disease (SM-AHNMD) Depending on the type of SM and prognosis of associated AHNMD Imatinib to control AHNMD; for SML-AML and aggressive types chemotherapy followed by allogenic stem cell transplantation > 80% KIT D816V mutations
AHNMD presents with genetic lesions
Non-KIT mutations
Mast cell leukemia/Mast cell sarcoma (MCL/MCS) Very poor Polychemotherapy, allogenic stem cell transplantation, 2CdA, TKIs, Hydroxyurea MCL: KIT D816V is least (46%)
KIT ECD, JMD mutations
No KIT mutation (WT KIT)
MCS: No KIT D816V mutation till date (N822K, del419 found)
Familial mastocytosis Usually good Imatinib and TKIs Rare somatic KIT D816V mutations
Germline mutation or deletions (K509I, A533D, R634W, N821I, M835K, S849I or del419, del559-560)

Adapted and compiled from Peter Valent, Mastocytosis: a paradigmatic example of a rare disease with complex biology and pathology, Am J Can Res 2013; 3;159–172; and from M. Arock et al, KIT mutation analysis of mast cell neoplasms: recommendations of the European Competence Network on Mastocytosis, Leukemia 2015, 1–10