Your search keyword '"KIT D816V mutation"' showing total 41 results

1. Case Report: Evolution of KIT D816V-Positive Systemic Mastocytosis to Myeloid Neoplasm With PDGFRA Rearrangement Responsive to Imatinib.

Author

Sciumè, Mariarita, Ceparano, Giusy, Eller-Vainicher, Cristina, Fabris, Sonia, Lonati, Silvia, Croci, Giorgio Alberto, Baldini, Luca, and Grifoni, Federica Irene

Subjects

MAST cell disease, BLOOD diseases, IMATINIB, MYELOPROLIFERATIVE neoplasms, GENE fusion, TUMORS

Abstract

Systemic mastocytosis (SM) is a rare neoplasm resulting from extracutaneous infiltration of clonal mast cells (MC). The clinical features of SM are very heterogenous and treatment should be highly individualized. Up to 40% of all SM cases can be associated with another hematological neoplasm, most frequently myeloproliferative neoplasms. Here, we present a patient with indolent SM who subsequently developed a myeloid neoplasm with PDGFRA rearrangement with complete response to low-dose imatinib. The 63-year-old patient presented with eosinophilia and elevated serum tryptase level. Bone marrow analysis revealed aberrant MCs in aggregates co-expressing CD2/CD25 and KIT D816V mutation (0.01%), and the FIP1L1-PDGFRA fusion gene was not identified. In the absence of 'B' and 'C' findings, we diagnosed an indolent form of SM. For 2 years after the diagnosis, the absolute eosinophil count progressively increased. Bone marrow evaluation showed myeloid hyperplasia and the FIP1L1-PDGFRA fusion gene was detected. Thus, the diagnosis of myeloid neoplasm with PDGFRA rearrangement was established. The patient was treated with imatinib 100 mg daily and rapidly obtained a complete molecular remission. The clinical, biological, and therapeutic aspects of SM might be challenging, especially when another associated hematological disease is diagnosed. Little is known about the underlying molecular and immunological mechanisms that can promote one entity prevailing over the other one. Currently, the preferred concept of SM pathogenesis is a multimutated neoplasm in which KIT mutations represent a "phenotype modifier" toward SM. Our patient showed an evolution from KIT mutated indolent SM to a myeloid neoplasm with PDGFRA rearrangement; when the eosinophilic component expanded, a regression of the MC counterpart was observed. In conclusion, extensive clinical monitoring associated with molecular testing is essential to better define these rare diseases and consequently their prognosis and treatment. [ABSTRACT FROM AUTHOR]

Published

2021

2. Case Report: Evolution of KIT D816V-Positive Systemic Mastocytosis to Myeloid Neoplasm With PDGFRA Rearrangement Responsive to Imatinib

Author

Mariarita Sciumè, Giusy Ceparano, Cristina Eller-Vainicher, Sonia Fabris, Silvia Lonati, Giorgio Alberto Croci, Luca Baldini, and Federica Irene Grifoni

Subjects

systemic mastocytosis, myeloid neoplasm with PDGFRA rearrangement, imatinib, KIT D816V mutation, clonal evolution, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Systemic mastocytosis (SM) is a rare neoplasm resulting from extracutaneous infiltration of clonal mast cells (MC). The clinical features of SM are very heterogenous and treatment should be highly individualized. Up to 40% of all SM cases can be associated with another hematological neoplasm, most frequently myeloproliferative neoplasms. Here, we present a patient with indolent SM who subsequently developed a myeloid neoplasm with PDGFRA rearrangement with complete response to low-dose imatinib. The 63-year-old patient presented with eosinophilia and elevated serum tryptase level. Bone marrow analysis revealed aberrant MCs in aggregates co-expressing CD2/CD25 and KIT D816V mutation (0.01%), and the FIP1L1-PDGFRA fusion gene was not identified. In the absence of ‘B’ and ‘C’ findings, we diagnosed an indolent form of SM. For 2 years after the diagnosis, the absolute eosinophil count progressively increased. Bone marrow evaluation showed myeloid hyperplasia and the FIP1L1-PDGFRA fusion gene was detected. Thus, the diagnosis of myeloid neoplasm with PDGFRA rearrangement was established. The patient was treated with imatinib 100 mg daily and rapidly obtained a complete molecular remission. The clinical, biological, and therapeutic aspects of SM might be challenging, especially when another associated hematological disease is diagnosed. Little is known about the underlying molecular and immunological mechanisms that can promote one entity prevailing over the other one. Currently, the preferred concept of SM pathogenesis is a multimutated neoplasm in which KIT mutations represent a “phenotype modifier” toward SM. Our patient showed an evolution from KIT mutated indolent SM to a myeloid neoplasm with PDGFRA rearrangement; when the eosinophilic component expanded, a regression of the MC counterpart was observed. In conclusion, extensive clinical monitoring associated with molecular testing is essential to better define these rare diseases and consequently their prognosis and treatment.

Published

2021

3. Pathophysiologic implications of elevated prevalence of hereditary alpha-tryptasemia in all mastocytosis subtypes.

Author

Polivka, Laura, Madrange, Marine, Bulai-Livideanu, Cristina, Barete, Stéphane, Ballul, Thomas, Neuraz, Antoine, Greco, Celine, Agopian, Julie, Brenet, Fabienne, Dubreuil, Patrice, Burdet, Charles, Lemal, Richard, Tournilhac, Olivier, Terriou, Louis, Launay, David, Bouillet, Laurence, Gourguechon, Clément, Damaj, Ghandi, Frenzel, Laurent, and Meni, Cécile

Abstract

Mastocytosis and monoclonal mast cell (MC) activation syndrome (MMAS) are heterogeneous conditions characterized by the accumulation of atypical MCs. Despite the recurrent involvement of KIT mutations, the pathophysiologic origin of mastocytosis and MMAS is unclear. Although hereditary α-tryptasemia (HαT, related to TPSAB1 gene duplication) is abnormally frequent in these diseases, it is not known whether the association is coincidental or causal. We evaluated the prevalence of HαT in all mastocytosis subtypes and MMAS and assessed the pathophysiologic association with HαT. Clinical data, laboratory data, KIT mutations, TPSAB1 duplication (assessed by droplet digital PCR), and HαT prevalence were retrospectively recorded for all patients with mastocytosis and MMAS registered in the French national referral center database and compared to a control cohort. To increase the power of our analysis for advanced systemic mastocytosis (advSM), we pooled our cohort with literature cases. We included 583 patients (27 with MMAS and 556 with mastocytosis). The prevalence of HαT in mastocytosis was 12.6%, significantly higher than in the general population (5.7%, P =.002) and lower than in MMAS (33.3%, P =.02). HαT+ patients were more likely to have anaphylactic reactions and less likely to have cutaneous lesions than HαT− patients (43.0% vs 24.4%, P =.006; 57.7% vs 75.6%, respectively, P =.006). In the pooled analysis, the prevalence of HαT was higher in advSM (11.5%) than in control cohorts (5.2%, P =.01). Here we confirm the increase incidence of anaphylaxis in HαT+ mastocytosis patients. The increased prevalence of HαT in all subtypes of systemic mastocytosis (including advSM) is suggestive of pathophysiologic involvement. [ABSTRACT FROM AUTHOR]

Published

2024

4. Tyrosine Kinase Inhibitors in Non-advanced Systemic Mastocytosis.

Author

Akin C

Abstract

Systemic mastocytosis is associated with KIT D816V mutation in more than 90% of cases. Patients with non-advanced forms of mastocytosis (indolent systemic mastocytosis, bone marrow mastocytosis, and smoldering systenic mastocytosis) have a low rate of progession to advanced variants and generally have a comparable life expectancy to age-matched general population. Symptomatology in non-advanced mastocytosis is variable and is related to mast cell mediator release. While some patients require no or minimal symptomatic therapy with antimediator drugs, other may suffer from refractory symptoms impacting the quality of life despite being on multiple anti-mediator drugs. KIT tyrosine kinase inhibitors have been approved for advanced SM, and avapritinib has also been recently approved as the first such inhibitor for indolent systemic mastocytosis. Other TKIs are currently in clinical trials for patients with non-advanced SM who have persistent and severe symptoms despite optimized antimediator therapy. This article will review the current state of the science and available clinical data from trials of tyrosine kinase inhibitors in non-advanced systemic mastocytosis., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

5. KIT Mutations and Other Genetic Defects in Mastocytosis: Implications for Disease Pathology and Targeted Therapies.

Author

Chantran Y, Valent P, and Arock M

Subjects

Humans, Proto-Oncogene Proteins c-kit genetics, Mutation, Bone Marrow, Mast Cells, Mastocytosis diagnosis, Mastocytosis genetics, Mastocytosis therapy, Mastocytosis, Systemic diagnosis, Mastocytosis, Systemic drug therapy, Mastocytosis, Systemic genetics

Abstract

A KIT activating mutation (usually KIT D816V) is detected in neoplastic cells in greater than 90% of indolent patients with systemic mastocytosis (SM). In more advanced variants of SM, additional genetic defects can be found in several myeloid malignancy-related genes, which can be detected by applying next-generation sequencing. Currently, the techniques recommended to detect the KIT D816V mutation and quantify the mutational burden in peripheral blood, bone marrow, or other organs/tissues are allele specific-quantitative PCR or droplet digital PCR. These techniques are useful for diagnosis, prognostication, follow-up and monitoring of therapeutic efficacy of cytoreductive agents in patients with SM., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

6. Detection of clonal mast cell disease in wasp venom allergic patients with normal tryptase

Author

Merel C. Onnes, Abdulrazzaq Alheraky, Martijn C. Nawijn, Tim E. Sluijter, André B. Mulder, Suzanne Arends, Hanneke N. G. Oude Elberink, Groningen Research Institute for Asthma and COPD (GRIAC), Translational Immunology Groningen (TRIGR), and Stem Cell Aging Leukemia and Lymphoma (SALL)

Subjects

Pulmonary and Respiratory Medicine, mastocytosis, REMA score, KIT D816V MUTATION, ANAPHYLAXIS, DISORDERS, Immunology, tryptase, SYSTEMIC MASTOCYTOSIS, insect venom, KIT D816V analysis in peripheral blood, DIAGNOSIS, EFFICACY, PCR, SAFETY, Immunology and Allergy, IMMUNOTHERAPY

Abstract

Background: Clonal mast cell disease (CMD) is an underlying aggravating condition in wasp venom allergy (WVA) which requires a different treatment strategy. CMD is increasingly recognized in patients with normal basal serum tryptase (bsT). However, methods to identify at risk patients have not yet been assessed in large cohorts of WVA patients with normal bsT.Methods: This retrospective study evaluated the reliability of the REMA score in detecting CMD in a cohort of grade IV WVA patients with normal bsT and assessed the added value of other clinical parameters, KIT D816V mutation analysis in peripheral blood (PB) and the diagnosis of hereditary alpha tryptasemia (HAT). All patients had a conclusive bone marrow evaluation that demonstrated or excluded underlying CMD.Results: In total 35 CMD and 96 non-CMD patients were included. REMA score had a sensitivity of 72% (95% CI 56%-88%) and specificity of 79% (95% CI 70%-87%) in this cohort. Loss of consciousness during systemic reaction and bsT between 6.3 and 11.4 ng/ml were additional parameters independently associated with CMD. Sensitivity of KIT in PB was relatively low, 56% (95% CI 36%-75%), but had added value as screening method in patients with a low REMA score due to 100% specificity.Conclusion: The REMA score is a relatively reliable method to detect patients at risk of CMD among WVA patients with normal bsT. KIT mutation analysis in PB could serve as additional screening method in patients with low REMA scores.

Published

2022

7. Practical management of adverse events in patients with advanced systemic mastocytosis receiving midostaurin

Subjects

mastocytosis, midostaurin, tryptase, cytopenia, KIT D816V mutation, nausea, Advanced systemic mastocytosis, adverse events

Abstract

Introduction: Systemic mastocytosis (SM) is characterized by the overproduction and accumulation of neoplastic mast cells (MCs) in the bone marrow, skin, and visceral organs. The KIT D816V mutation is found in approximately 90% of cases. In advanced SM (advSM), inferior survival often relates to MC-induced organ damage that may impact multiple organ systems. In addition, mediator symptoms related to MC activation can severely impact the quality of life. The oral multikinase/KIT inhibitor midostaurin was approved by the US Food and Drug Administration and the European Medicines Agency as monotherapy for advSM based on data from phase 2 clinical studies.Areas covered: This review discusses the management of common adverse events (AEs) in patients with advSM who participated in phase 2 clinical studies that led to the approval of midostaurin.Expert opinion: In the advSM population undergoing treatment with midostaurin, treatment-related AEs are often difficult to distinguish from disease-related symptoms, which can lead to premature discontinuation and improper dose reduction of midostaurin therapy in patients who might have benefitted from continued therapy. Here we present strategies to help optimize AE management and maximize the potential benefits of midostaurin in advSM.

Published

2021

8. Prospective evaluation of the diagnostic value of sensitive KIT D816V mutation analysis of blood in adults with suspected systemic mastocytosis.

Author

Kristensen, T., Vestergaard, H., Bindslev‐Jensen, C., Mortz, C. G., Kjaer, H. F., Ollert, M., Møller, M. B., and Broesby‐Olsen, S.

Subjects

*MAST cell disease, *TREATMENT effectiveness, *BLOOD, *BONE marrow, *GENETIC mutation, *PATIENTS

Abstract

Background Sensitive KIT D816V mutation analysis of blood has been proposed to guide bone marrow ( BM) investigation in suspected systemic mastocytosis ( SM). The aim of this prospective study was for the first time to compare the D816V status of the 'screening blood sample' used to guide BM biopsy in suspected SM to the outcome of the subsequent BM investigation. Methods Fifty-eight adult patients with suspected SM were included. The outcome of sensitive KIT D816V analysis of blood was compared to the result of the BM investigation. Results Screening blood samples from 44 of 58 patients tested D816V-positive. In 43 of these, SM was subsequently diagnosed in the BM investigation. One patient with a D816V-positive screening sample was diagnosed with monoclonal MC activation syndrome. Screening blood samples from 14 patients tested D816V-negative. SM was subsequently diagnosed in five of these, whereas nine patients did not fulfill any diagnostic SM criteria (excluding tryptase criterion). Of the 48 SM patients, 90% tested D816V-positive. Thirteen SM patients presented with Hymenoptera venom-induced anaphylaxis, no skin lesions, and baseline serum tryptase ≤20 ng/ mL. Of these, 92% tested D816V-positive in the screening blood sample. Conclusion This prospective study demonstrates that a D816V-positive result in a screening blood sample identifies SM among patients with hymenoptera venom-induced anaphylaxis in whom the diagnosis would most probably have been missed, with potential severe implications. The observed false-negative screening results also underline that BM investigation is mandatory in all adult patients with clear signs of, or highly suspected SM, regardless of the KIT mutation status. [ABSTRACT FROM AUTHOR]

Published

2017

9. Eosinophilia in a patient with aggressive systemic mastocytosis harboring a KIT D816V mutation: A case report.

Author

Cao L, Tong H, Liu X, Pan Q, Xu Y, Lai J, Zheng W, Huang J, Wang Z, Ye S, Zhang L, Qin J, and Jin J

Abstract

Eosinophilia may result from three main causes: secondary (reactive), primary (clonal), and/or idiopathic. The diagnosis of idiopathic eosinophilia must be made based on excluding all reactive or clonal causes. However, some causes may be very rare so as to be misdiagnosed as idiopathic. We present the case of eosinophilia caused by aggressive systemic mastocytosis, originally recognized as idiopathic. Lymphadenopathy, dysmyelopoiesis, and hepatosplenomegaly gradually appeared and deteriorated with increasing eosinophils. This case carried KIT D816V mutation. The BCR::ABL fusion gene and the mutations in JAK2 V617F, PDGFRα , and PDGFRβ in bone marrow were all negative. PHF6, PPM1D , and TET2 mutations were demonstrable. The patient was prescribed to avapritinib. The condition was effectively controlled. However, the patient discontinued medication for economic reasons 5 months later. Disease progression happened and died 10 months after diagnosis. Our study indicates that gene mutation detection at diagnosis is helpful for patient accurate diagnosis and targeted therapy of such patients., Competing Interests: The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article., (© The Author(s) 2023.)

Published

2023

10. Risk factors and indicators of severe systemic insect sting reactions

Subjects

mastocytosis, EUROPEAN ACADEMY, BASAL SERUM TRYPTASE, KIT D816V MUTATION, tryptase, venom, INDUCED ANAPHYLAXIS, FATAL ANAPHYLAXIS, PLATELET-ACTIVATING-FACTOR, CONVERTING ENZYME-INHIBITORS, age, MAST-CELL DISORDERS, BEE VENOM, medication, HYMENOPTERA VENOM ALLERGY

Abstract

Hymenoptera venom allergy ranks among the top three causes of anaphylaxis worldwide, and approximately one-quarter of sting-induced reactions are classified as severe. Fatal sting reactions are exceedingly rare, but certain factors may entail a considerably higher risk. Delayed administration of epinephrine and upright posture are situational risk factors which may determine an unfavorable outcome of the acute anaphylactic episode and should be addressed during individual patient education. Systemic mastocytosis and senior age are major, unmodifiable long-term risk factors and thus reinforce the indication for venom immunotherapy. Vespid venom allergy and male sex likewise augment the risk of severe or even fatal reactions. Further studies are required to assess the impact of specific cardiovascular comorbidities. Available data regarding potential effects of beta-blockers and/or ACE inhibitors in coexisting venom allergy are inconclusive and do not justify recommendations to discontinue guideline-directed antihypertensive treatment. The absence of urticaria/angioedema during sting-induced anaphylaxis is indicative of a severe reaction, serum tryptase elevation, and mast cell clonality. Determination of basal serum tryptase levels is an established diagnostic tool for risk assessment in Hymenoptera venom-allergic patients. Measurement of platelet-activating factor acetylhydrolase activity represents a complementary approach but is not available for routine diagnostic use.

Published

2020

11. P1006: NEXT GENERATION SEQUENCING (NGS) IN PEDIATRIC MASTOCYTOSIS

Author

A. Angi, S. Bianchi, G. Palumbo, V. Filipponi, M. Rousseau, M. L. Moleti, and F. Giona

Subjects

KIT D816V mutation, pediatric mastocytosis, pediatric mastocytosis, KIT D816V mutation, Hematology

Published

2022

12. Targeted ultradeep next-generation sequencing as a method for KIT D816V mutation analysis in mastocytosis.

Author

Kristensen, Thomas, Broesby‐Olsen, Sigurd, Vestergaard, Hanne, Bindslev‐Jensen, Carsten, and Møller, Michael Boe

Subjects

*MAST cell disease, *IMMUNOLOGIC diseases, *TUMOR growth, *GENETIC disorders, *GENE frequency, *THERAPEUTICS

Abstract

Next-generation sequencing (NGS) is becoming increasingly used for diagnostic mutation analysis in myeloid neoplasms and may also represent a feasible technique in mastocytosis. However, detection of the KIT D816V mutation requires a highly sensitive method in most patients due to the typically low mutation levels. In this study, we established an NGS-based KIT mutation analysis and analyzed the sensitivity of D816V detection using the Ion Torrent platform. Eighty-two individual NGS analyses were included in the study. All samples were also analyzed using highly sensitive KIT D816V mutation-specific qPCR. Measurements of the background level in D816V-negative samples supported a cutoff for positivity of 0.2% in three different NGS panels. Clinical samples from patients with SM that tested positive using qPCR with a D816V allele burden >0.2% also tested positive using NGS. Samples that tested positive using qPCR with an allele burden <0.2% tested negative using NGS. We thereby demonstrate that caution should be taken when using the potentially very sensitive NGS technique for KIT D816V mutation analysis in mastocytosis, as many patients with SM have D816V mutation levels below the detection limit of NGS. A dedicated and highly sensitive KIT D816V mutation analysis therefore remains important in mastocytosis diagnostics. [ABSTRACT FROM AUTHOR]

Published

2016

13. Diagnosis of Mastocytosis in Children and Adults in Daily Clinical Practice.

Author

LANGE, Magdalena, ŁUGOWSKA-UMER, Hanna, NIEDOSZYTKO, Marek, WASĄG, Bartosz, LIMON, Janusz, ŻAWROCKI, Anton, NEDOSZYTKO, Bogusław, SOBJANEK, Michał, PLATA-NAZAR, Katarzyna, and NOWICKI, Roman

Subjects

*MAST cell disease, *IMMUNOLOGIC diseases in children, *DIAGNOSTIC examinations, *TRYPTASE, *CLINICAL medicine, *DIAGNOSIS

Abstract

Mastocytosis comprises a heterogeneous group of disorders characterized by clonal, neoplastic proliferation of mast cells accumulating in one or multiple organs. In the majority of cases skin involvement is the first clinical manifestation of the disease. Clinical work-up consists of a combination of morphological, immunohistochemical, flow cytometric immunophenotyping and molecular examination. Cutaneous mastocytosis predominates in children, whereas systemic mastocytosis is the most common form of the disease in adults. Therefore, different diagnostic algorithms have to be applied in adult patients and children with suspected mastocytosis. This comprehensive review presents currently defined variants of the disease and recommendations to facilitate diagnostic work-up in children and adults with suspected mastocytosis in daily clinical practice. [ABSTRACT FROM AUTHOR]

Published

2016

14. A Rare Case of Systemic Mastocytosis With Associated Clonal Hematological Non-Mast Cell Lineage Disease That Transformed to Acute Leukemia With IDH2 Mutation

Author

Andrew D. Liman, Agnes K. Liman, and Jenna Shields

Subjects

Pathology, medicine.medical_specialty, SM-AHNMD, Acute myelogenous leukemia, Case Report, Enasidenib, Myelogenous, chemistry.chemical_compound, Monocytosis, Medicine, Midostaurin, Systemic mastocytosis, Acute leukemia, biology, business.industry, CD117, IDH2 mutation, KIT D816V mutation, Serum tryptase, medicine.disease, Leukemia, chemistry, biology.protein, business

Abstract

An elderly 72-year-old man presented with anemia, thrombocytopenia, monocytosis, splenomegaly and lymphadenopathy. Bone marrow biopsy was consistent with mast cell neoplasm with positive CD117, CD25, CD34 myeloblasts and polymerase chain reaction (PCR) revealed mutation of D816V. He developed bilateral femoral neck fractures and biopsy confirmed that he has systemic mastocytosis (SM). He received cladribine and midostaurin with stable disease for 21 months. His SM with associated clonal hematological non-mast cell lineage disease (SM-AHNMD) transformed to acute myelogenous leukemia with isocitrate dehydrogenase 2 (IDH2) mutation. A trial of enasidenib was given for 5 months but without any response. Patient decided to go with home hospice and died afterwards.

Published

2020

15. Risk factors and indicators of severe systemic insect sting reactions

Author

Gunter J. Sturm, Patrizia Bonadonna, Axel Trautmann, Joanna N G Oude Elberink, and Johanna Stoevesandt

Subjects

Male, 0301 basic medicine, EUROPEAN ACADEMY, medicine.medical_specialty, Allergy, BASAL SERUM TRYPTASE, KIT D816V MUTATION, Immunology, tryptase, venom, INDUCED ANAPHYLAXIS, FATAL ANAPHYLAXIS, Tryptase, Venom, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, Internal medicine, MAST-CELL DISORDERS, medicine, Animals, Humans, Immunology and Allergy, Systemic mastocytosis, Anaphylaxis, Arthropod Venoms, mastocytosis, Angioedema, biology, business.industry, Insect Bites and Stings, medicine.disease, Hymenoptera, PLATELET-ACTIVATING-FACTOR, Sting, CONVERTING ENZYME-INHIBITORS, 030104 developmental biology, age, 030228 respiratory system, biology.protein, BEE VENOM, medication, HYMENOPTERA VENOM ALLERGY, medicine.symptom, business, Risk assessment

Abstract

Hymenoptera venom allergy ranks among the top three causes of anaphylaxis worldwide, and approximately one-quarter of sting-induced reactions are classified as severe. Fatal sting reactions are exceedingly rare, but certain factors may entail a considerably higher risk. Delayed administration of epinephrine and upright posture are situational risk factors which may determine an unfavorable outcome of the acute anaphylactic episode and should be addressed during individual patient education. Systemic mastocytosis and senior age are major, unmodifiable long-term risk factors and thus reinforce the indication for venom immunotherapy. Vespid venom allergy and male sex likewise augment the risk of severe or even fatal reactions. Further studies are required to assess the impact of specific cardiovascular comorbidities. Available data regarding potential effects of beta-blockers and/or ACE inhibitors in coexisting venom allergy are inconclusive and do not justify recommendations to discontinue guideline-directed antihypertensive treatment. The absence of urticaria/angioedema during sting-induced anaphylaxis is indicative of a severe reaction, serum tryptase elevation, and mast cell clonality. Determination of basal serum tryptase levels is an established diagnostic tool for risk assessment in Hymenoptera venom-allergic patients. Measurement of platelet-activating factor acetylhydrolase activity represents a complementary approach but is not available for routine diagnostic use.

Published

2019

16. New Insights into the Pathogenesis of Systemic Mastocytosis

Author

Zhixiong Li

Subjects

0301 basic medicine, TRK, QH301-705.5, medicine.medical_treatment, Review, systemic mastocytosis, Models, Biological, Catalysis, Myeloid Neoplasm, Targeted therapy, Inorganic Chemistry, Pathogenesis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Mastocytosis, Systemic, Medicine, Animals, Humans, Epigenetics, Midostaurin, Nerve Growth Factors, Physical and Theoretical Chemistry, Systemic mastocytosis, Biology (General), Molecular Biology, QD1-999, Spectroscopy, Oncogene, business.industry, pathogenesis, Organic Chemistry, KIT D816V mutation, General Medicine, medicine.disease, targeted therapy, Computer Science Applications, Chemistry, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Trk receptor, Mutation, Cancer research, business

Abstract

Mastocytosis is a type of myeloid neoplasm characterized by the clonal, neoplastic proliferation of morphologically and immunophenotypically abnormal mast cells that infiltrate one or more organ systems. Systemic mastocytosis (SM) is a more aggressive variant of mastocytosis with extracutaneous involvement, which might be associated with multi-organ dysfunction or failure and shortened survival. Over 80% of patients with SM carry the KIT D816V mutation. However, the KIT D816V mutation serves as a weak oncogene and appears to be a late event in the pathogenesis of mastocytosis. The management of SM is highly individualized and was largely palliative for patients without a targeted form of therapy in past decades. Targeted therapy with midostaurin, a multiple kinase inhibitor that inhibits KIT, has demonstrated efficacy in patients with advanced SM. This led to the recent approval of midostaurin by the United States Food and Drug Administration and European Medicines Agency. However, the overall survival of patients treated with midostaurin remains unsatisfactory. The identification of genetic and epigenetic alterations and understanding their interactions and the molecular mechanisms involved in mastocytosis is necessary to develop rationally targeted therapeutic strategies. This review briefly summarizes recent developments in the understanding of SM pathogenesis and potential treatment strategies for patients with SM.

Published

2021

17. Real-World Efficacy of Midostaurin in Aggressive Systemic Mastocytosis

Author

Oliwia Bachanek-Mitura, Witold Krupski, Tomasz Gromek, Aneta Szudy-Szczyrek, Justyna Szumiło, Michał Szczyrek, Grzegorz Helbig, Karolina Chromik, Marek Hus, Zuzanna Kanduła, and Andrzej Mital

Subjects

medicine.medical_specialty, Bone marrow infiltration, tryptase, lcsh:Medicine, Tryptase, mast cells, Disease, KIT D816V mutation, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Medicine, Secondary Acute Myeloid Leukemia, Midostaurin, Systemic mastocytosis, biology, business.industry, lcsh:R, aggressive systemic mastocytosis, midostaurin, General Medicine, medicine.disease, Transplantation, chemistry, 030220 oncology & carcinogenesis, biology.protein, Stem cell, business, 030215 immunology

Abstract

In April 2017 midostaurin was approved by the US Food and Drug Administration for the treatment of patients with aggressive systemic mastocytosis (ASM). So far, very limited real world data on its efficacy is available. Thirteen patients aged from 48 to 79 years, who received midostaurin in the early access program, were included in the study. Midostaurin was used both in first (n = 5) and subsequent lines of treatment (n = 8). The median duration of exposure was 9 months. Most patients (77%, n = 10) had a clinical improvement already as soon as the second month of therapy. Objective response was noted in 4 (50%) of eight evaluated patients. Among responders, we observed a decrease in serum tryptase level (median 74.14%) and bone marrow infiltration by mast cells (median 50%) in the sixth month of treatment. In one case, in the 10th month of treatment, allogenic stem cell transplantation was performed, achieving complete remission. Five patients died, three due to progression of disease, one in the course of secondary acute myeloid leukemia and one due to reasons not related to mastocytosis. Treatment is ongoing in seven patients. We found that midostaurin therapy is beneficial to patients with ASM.

Published

2021

18. Does the Aberrant Expression of CD2 and CD25 by Skin Mast Cells Truly Correlate with Systemic Involvement in Patients Presenting with Mastocytosis in the Skin?

Author

Lange, Magdalena, yawrocki, anton, Nedoszytko, Bogus"aw, Wasag, Bartosz, Niedoszytko, Marek, Jassem, Ewa, Nowicki, Roman, ymijewski, Micha" a., and Biernat, Wojciech

Subjects

*SKIN disease treatment, *MAST cell disease, *CD2 antigen, *CD25 antigen, *IMMUNOHISTOCHEMISTRY, *PATIENTS

Abstract

Background: Neoplastic mast cells involving the bone marrow (BMMCs) of patients with mastocytosis display an aberrant expression of CD25 and/or CD2 antigens. The aim of this study was to determine the frequency of CD2 and CD25 expression on skin mast cells (sMCs) of patients with mastocytosis in the skin at the early stage of the disease. Furthermore, the usefulness of the phenotypic profile of sMCs for the diagnosis of systemic mastocytosis (SM) was evaluated. Methods: The 52 adults included in the study were diagnosed with mastocytosis strictly according to the criteria of the World Health Organization. CD117, CD2 and CD25 antigen expression on sMCs was detected by immunohistochemistry. The presence of the KIT D816V mutation in the BM was analyzed using allele-specific PCR. Results: The presence of CD2- or CD25-positive sMCs was detected in 57.1% of cutaneous mastocytosis (CM) and 90.3% of SM cases (p = 0.008). In all mastocytosis patients, CD2 expression on sMCs was more frequent than CD25 expression (67.3 and 38.5%, respectively). Moreover, CD2 expression on sMCs was more frequent in SM than in CM cases (p = 0.02). The presence of one of the aberrant sMC antigens was detected in 84.2% of patients with the KIT D816V mutation in the BM. A positive correlation between densities of CD25- and CD117-positive sMCs was found in SM patients (r = 0.46, p = 0.009). Conclusions: Although sMCs displayed immunoreactivity for one of the neoplastic antigens in the majority of SM patients, the aberrant CD2 and/or CD25 expression on sMCs is not as indicative of SM as the BMMC immunophenotype. © 2014 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2014

19. Comparison of gDNA-based versus mRNA-based KIT D816V mutation analysis reveals large differences between blood and bone marrow in systemic mastocytosis.

Author

Kristensen, Thomas, Broesby‐Olsen, Sigurd, Vestergaard, Hanne, Bindslev‐Jensen, Carsten, and Møller, Michael B.

Subjects

*MESSENGER RNA, *BONE marrow, *MAST cell disease, *POLYMERASE chain reaction, *GENOMICS

Abstract

The article provides information on a study which examined genomic DNA (gDNA)-based and messenger RNA (mRNA)-based KIT D816V mutation analysis of peripheral blood (PB) and bone marrow (BM) aspirate from systemic mastocytosis (SM) patients. Topics discussed include use of a highly sensitive KIT D816V mutation-specific quantitative polymerase chain reaction assay and results of an mRNA-based assay.

Published

2017

20. The presence of mast cell clonality in patients with unexplained anaphylaxis.

Author

Gülen, T., Hägglund, H., Sander, B., Dahlén, B., and Nilsson, G.

Subjects

*MAST cell disease, *MAST cells, *PATIENT acceptance of health care, *CLINICAL trials, *CONNECTIVE tissue diseases

Abstract

Background The mechanisms by which mast cells in patients with unexplained anaphylaxis ( UEA) are triggered remain elusive. Onset of episodes is unpredictable and often recurrent. The substantial overlap between the clinical manifestations of UEA and clonal mast cell disorders ( CMD) suggests an association between these rare disorders. The two forms of CMD characterized to date are systemic mastocytosis ( SM) and monoclonal mast cell activation syndrome ( MMAS). Objective To examine the hypothesis that the pathogenesis of UEA reflects the presence of aberrant subpopulations of mast cells. Methods Thirty (14 men, 16 women) patients (≥ 18 years) suffering from UEA and with no signs of cutaneous mastocytosis were recruited. Patients underwent an initial complete allergy work-up to confirm the diagnosis of UEA. Level of baseline serum tryptase (sBT) and total IgE were determined. In addition, a bone marrow examination was performed on all 30 patients to investigate possible underlying CMD. Results Fourteen (47%) of our cases (nine men, five women) were diagnosed with CMD: 10 with SM and four with MMAS. Four of the 10 patients with SM had mast cell aggregates in their bone marrow. All patients with SM exhibited a sBT level > 11.4 ng/mL, whereas this level was elevated in only two of those with MMAS and four with UAE but not diagnosed with CMD. Total IgE levels were lower in the group of patients with CMD ( P < 0.03). Conclusion and Clinical Relevance The pathogenic mechanism underlying UEA could be explained by the presence of immunophenotypically aberrant mast cells with clonal markers in 47% of our subjects, indicating that clonal mast cell disorders are present in a substantial subset of these patients. Thus, the presence of CMD should be considered in patients with UEA if they have an elevated level of sBT (≥ 11.4 ng/mL) and cardiovascular symptoms such as syncope. [ABSTRACT FROM AUTHOR]

Published

2014

21. Practical management of adverse events in patients with advanced systemic mastocytosis receiving midostaurin

Author

Andreas Reiter, Cem Akin, Peter Valent, Jason Gotlib, Hanneke C. Kluin-Nelemans, and Karin Hartmann

Subjects

0301 basic medicine, Nausea, Clinical Biochemistry, tryptase, Tryptase, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Mastocytosis, Systemic, Drug Discovery, medicine, cytopenia, Humans, Midostaurin, Systemic mastocytosis, Adverse effect, Pharmacology, Cytopenia, mastocytosis, biology, business.industry, KIT D816V mutation, medicine.disease, nausea, Staurosporine, humanities, adverse events, Kit d816v, 030104 developmental biology, medicine.anatomical_structure, midostaurin, chemistry, 030220 oncology & carcinogenesis, Immunology, Mutation, biology.protein, Quality of Life, Bone marrow, medicine.symptom, business, Advanced systemic mastocytosis

Abstract

Introduction: Systemic mastocytosis (SM) is characterized by the overproduction and accumulation of neoplastic mast cells (MCs) in the bone marrow, skin, and visceral organs. The KIT D816V mutation is found in approximately 90% of cases. In advanced SM (advSM), inferior survival often relates to MC-induced organ damage that may impact multiple organ systems. In addition, mediator symptoms related to MC activation can severely impact the quality of life. The oral multikinase/KIT inhibitor midostaurin was approved by the US Food and Drug Administration and the European Medicines Agency as monotherapy for advSM based on data from phase 2 clinical studies. Areas covered: This review discusses the management of common adverse events (AEs) in patients with advSM who participated in phase 2 clinical studies that led to the approval of midostaurin. Expert opinion: In the advSM population undergoing treatment with midostaurin, treatment-related AEs are often difficult to distinguish from disease-related symptoms, which can lead to premature discontinuation and improper dose reduction of midostaurin therapy in patients who might have benefitted from continued therapy. Here we present strategies to help optimize AE management and maximize the potential benefits of midostaurin in advSM.

Published

2020

22. KIT D816V Mutation-Positive Cell Fractions in Lesional Skin Biopsies from Adults with Systemic Mastocytosis.

Author

Kristensen, Thomas, Broesby-Olsen, Sigurd, Vestergaard, Hanne, Bindslev-Jensen, Carsten, and Møller, Michael Boe

Abstract

Background: Most adults with systemic mastocytosis (SM) carry the somatic KIT D816V mutation, but the occurrence of the mutation in lesional skin remains to be characterized. Objective: To assess the distribution and fraction of KIT D816V mutation-positive cells in lesional skin. Methods: Lesional skin biopsies from 29 adults with SM were analysed using sensitive and quantitative qPCR KIT D816V mutation analysis. Results: The KIT D816V mutation was detected in skin in all cases. Highly similar mutation levels were observed in all patients with a median of 5% mutation-positive cells in the skin (range 1-23%). Conclusion: The KIT D816V mutation is consistently present in lesional skin in adults with SM. The low variation in mutation levels detected in lesional skin contrasts blood and bone marrow where mast cell (MC) progenitor and non-MC lineage involvement causes the mutation-positive cell fraction to be highly variable. Copyright © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2013

23. Systemic mastocytosis is uncommon in KIT D816V mutation positive core-binding factor acute myeloid leukemia.

Author

Kristensen, Thomas, Preiss, Birgitte, Broesby-Olsen, Sigurd, Vestergaard, Hanne, Friis, Lone, and Møller, Michael Boe

Subjects

*MAST cell disease, *ACUTE myeloid leukemia, *GENETIC mutation, *HUMAN chromosomes, *CELL fractionation, *LEUKEMIA etiology

Abstract

The KIT D816V mutation is detected in the vast majority of adult cases of systemic mastocytosis (SM). The mutation is also frequently detected in core-binding factor acute myeloid leukemia (CBF AML) defined by the presence of t(8;21)(q22;q22); RUNX1-RUNX1T1 or inv(16)(p13.1;q22)/t(16;16)(p13.1;q22); CBFB-MYH11 chromosomal rearrangements, but whether the mutation is indicative of associated SM is unclear. In the present study, patients with CBF AML were therefore analyzed for the KIT D816V mutation and mutation positive cases subsequently analyzed for the presence of SM. The KIT D816V mutation was detected in eight of 20 cases of CBF AML, with the frequency in t(8;21)(q22;q22) and inv(16)(p13.1;q22) positive cases being 31% and 57%, respectively. The fraction of KIT D816V mutation positive cells was highly variable among the eight mutation positive patients, with levels ranging from 0.04 to 98% in a pretreatment blood sample. Five of the eight cases carried the mutation in a cell fraction below one-tenth of the blast cell fraction, thus suggesting that KIT mutation is often a late event in leukemogenesis. None of the eight KIT D816V mutation positive cases fulfilled the World Health Organization diagnostic criteria of SM. The presence of the KIT D816V mutation in the CBF AML subgroup can therefore not be considered indicative of associated SM. [ABSTRACT FROM AUTHOR]

Published

2012

24. Phase II study of imatinib mesylate as therapy for patients with systemic mastocytosis

Author

Vega-Ruiz, Arturo, Cortes, Jorge E., Sever, Matjaz, Manshouri, Taghi, Quintás-Cardama, Alfonso, Luthra, Raja, Kantarjian, Hagop M., and Verstovsek, Srdan

Subjects

*IMATINIB, *METHANESULFONATES, *MAST cell disease, *GENETIC mutation, *BIOLOGICAL membranes, *TARGETED drug delivery, *CLINICAL trials, *PATIENTS

Abstract

Abstract: Gain-of-function D816V point mutation within the kinase domain of the transmembrane receptor KIT is found in the great majority of patients with systemic mastocytosis (SM) and is attractive therapeutic target. Twenty patients with SM were enrolled during 2003–2005 in phase II clinical trial with imatinib mesylate (400mg daily), a KIT inhibitor. Median time on therapy was 9 months (range, 0.5–44+). Only one patient, with D816V KIT mutation-negative FIP1L1-PDGFRα-negative SM-HES, achieved complete remission (now lasting for 44 months). Six other patients reported symptomatic improvement, including two with D816V KIT mutation-positive SM (one reported improvement in diarrhea and the other in fatigue). Other patients had no benefit. Imatinib was relatively well tolerated. Our study confirms that imatinib therapy does not result in appreciable clinical activity in patients with D816V mutation-positive SM, but may result in a significant benefit in occasional patient with D816V mutation-negative SM. [Copyright &y& Elsevier]

Published

2009

25. KIT D816V–associated systemic mastocytosis with eosinophilia and FIP1L1/PDGFRA-associated chronic eosinophilic leukemia are distinct entities.

Author

Maric, Irina, Robyn, Jamie, Metcalfe, Dean D., Fay, Michael P., Carter, Melody, Wilson, Todd, Fu, Weiming, Stoddard, Jennifer, Scott, Linda, Hartsell, Marilyn, Kirshenbaum, Arnold, Akin, Cem, Nutman, Thomas B., Noel, Pierre, and Klion, Amy D.

Subjects

DISEASES, PUBLIC health, SKIN inflammation, DIAGNOSIS

Abstract

Background: The broad and overlapping clinical manifestations of D816V KIT–associated systemic mastocytosis with eosinophilia and FIP1L1/PDGFRA-associated chronic eosinophilic leukemia (CEL), coupled with the increase in activated eosinophils and mast cells seen in both disorders, have led to confusion in the nomenclature. It is of paramount importance, however, to distinguish between these 2 groups of patients because of differences in clinical sequelae, prognoses, and selection of treatment. Objective: We thus sought to identify clinical and laboratory features that could be used to distinguish these 2 diagnoses. Methods: We compared 12 patients with D816V-positive systemic mastocytosis with eosinophilia with 17 patients with FIP1L1/PDGFRA-positive CEL. Distinguishing features were used to create a risk factor scoring system. Results: This system correctly classified 16 of 17 FIP1L1/PDGFRA-positive patients with CEL and all 12 patients with systemic mastocytosis with eosinophilia. Thirty-four FIP1L1/PDGFRA-positive patients described in the literature were also classified using this system, and although a complete set of data was not available for any of the historical patients, 21 were correctly classified. Conclusion: These results reinforce the hypothesis that the FIP1L1/PDGFRA gene fusion and D816V-KIT mutation cause distinct clinical syndromes. Clinical implications: This novel diagnostic approach should prove helpful in clinical practice in the evaluation of patients with increased mast cells and peripheral eosinophilia. [Copyright &y& Elsevier]

Published

2007

26. Advances in the Classification and Treatment of Mastocytosis

Subjects

OF-THE-ART, C-KIT, URTICARIA PIGMENTOSA, NEOPLASTIC MAST-CELLS, KIT D816V MUTATION, IN-VITRO, ADVANCED SYSTEMIC MASTOCYTOSIS, BONE-MARROW MASTOCYTOSIS, PERIPHERAL-BLOOD, CONSENSUS PROPOSAL

Abstract

Mastocytosis is a term used to denote a heterogeneous group of conditions defined by the expansion and accumulation of clonal (neoplastic) tissue mast cells in various organs. The classification of the World Health Organization (WHO) divides the disease into cutaneous mastocytosis, systemic mastocytosis, and localized mast cell tumors. On the basis of histomorphologic criteria, clinical parameters, and organ involvement, systemic mastocytosis is further divided into indolent systemic mastocytosis and advanced systemic mastocytosis variants, including aggressive systemic mastocytosis and mast cell leukemia. The clinical impact and prognostic value of this classification has been confirmed in numerous studies, and its basic concept remains valid. However, refinements have recently been proposed by the consensus group, the WHO, and the European Competence Network on Mastocytosis. In addition, new treatment options are available for patients with advanced systemic mastocytosis, including allogeneic hematopoietic stem cell transplantation and multikinase inhibitors directed against KIT D816V and other key signaling molecules. Our current article provides an overview of recent advances in the field of mastocytosis, with emphasis on classification, prognostication, and emerging new treatment options in advanced systemic mastocytosis. (C)2017 AACR.

Published

2017

27. Therapeutic challenge during the long-term follow-up of a patient with indolent systemic mastocytosis with extensive cutaneous involvement.

Author

MARTON, I., PÓSFAI, É., BORBÉNYI, Z., BÖDÖR, C., PAPP, G., DEMETER, J., KOROM, I., VARGA, E., and BATA-CSÖRGO, Z.

Abstract

From a dermatological aspect, it posed a considerable challenge the skin-limited form of mastocytosis, urticaria pigmentosa and indolent systemic mastocytosis (ISM) with cutaneous lesions. Despite the favourable prognosis, lifelong dermatological control is needed, during which the average symptomatic therapy does not always seem adequate. We report here the case of a female ISM patient with recurrent cutaneous symptoms that impaired her quality of life, with a follow-up time of 27 years. During this long follow-up period, the cutaneous lesions could be controlled by antihistamines, leukotriene antagonists, glucocorticoids, local immunosuppressants or local UV radiation for only relatively short periods. Imatinib mesylate was, therefore, introduced in an attempt to control the cutaneous lesions. Tyrosine kinase inhibition is an unusual dermatological therapeutic option. This case illustrates that imatinib mesylate was a good choice with which to achieve a reduction of the skin lesions in this KIT D816V mutation-negative disease: it led to a temporary appreciable improvement of the patient's quality of life. [ABSTRACT FROM AUTHOR]

Published

2015

28. Clinical and Molecular Diagnostic Evaluation of Systemic Mastocytosis in the South-Eastern Hungarian Population Between 2001–2013 – A Single Centre Experience

Author

Marton, Imelda, Krenács, László, Bagdi, Enikő, Bakos, Annamária, Demeter, Judit, and Borbényi, Zita

Published

2016

29. New Insights into the Pathogenesis of Systemic Mastocytosis.

Author

Li, Zhixiong and Martín, Margarita

Subjects

*MAST cell disease, *OVERALL survival, *MAST cells, *MOLECULAR interactions, *KINASE inhibitors

Abstract

Mastocytosis is a type of myeloid neoplasm characterized by the clonal, neoplastic proliferation of morphologically and immunophenotypically abnormal mast cells that infiltrate one or more organ systems. Systemic mastocytosis (SM) is a more aggressive variant of mastocytosis with extracutaneous involvement, which might be associated with multi-organ dysfunction or failure and shortened survival. Over 80% of patients with SM carry the KIT D816V mutation. However, the KIT D816V mutation serves as a weak oncogene and appears to be a late event in the pathogenesis of mastocytosis. The management of SM is highly individualized and was largely palliative for patients without a targeted form of therapy in past decades. Targeted therapy with midostaurin, a multiple kinase inhibitor that inhibits KIT, has demonstrated efficacy in patients with advanced SM. This led to the recent approval of midostaurin by the United States Food and Drug Administration and European Medicines Agency. However, the overall survival of patients treated with midostaurin remains unsatisfactory. The identification of genetic and epigenetic alterations and understanding their interactions and the molecular mechanisms involved in mastocytosis is necessary to develop rationally targeted therapeutic strategies. This review briefly summarizes recent developments in the understanding of SM pathogenesis and potential treatment strategies for patients with SM. [ABSTRACT FROM AUTHOR]

Published

2021

30. Real-World Efficacy of Midostaurin in Aggressive Systemic Mastocytosis.

Author

Szudy-Szczyrek, Aneta, Bachanek-Mitura, Oliwia, Gromek, Tomasz, Chromik, Karolina, Mital, Andrzej, Szczyrek, Michał, Krupski, Witold, Szumiło, Justyna, Kanduła, Zuzanna, Helbig, Grzegorz, Hus, Marek, and Mannelli, Francesco

Subjects

*MAST cell disease, *ACUTE myeloid leukemia, *STEM cell transplantation, *MAST cells, *BONE marrow

Abstract

In April 2017 midostaurin was approved by the US Food and Drug Administration for the treatment of patients with aggressive systemic mastocytosis (ASM). So far, very limited real world data on its efficacy is available. Thirteen patients aged from 48 to 79 years, who received midostaurin in the early access program, were included in the study. Midostaurin was used both in first (n = 5) and subsequent lines of treatment (n = 8). The median duration of exposure was 9 months. Most patients (77%, n = 10) had a clinical improvement already as soon as the second month of therapy. Objective response was noted in 4 (50%) of eight evaluated patients. Among responders, we observed a decrease in serum tryptase level (median 74.14%) and bone marrow infiltration by mast cells (median 50%) in the sixth month of treatment. In one case, in the 10th month of treatment, allogenic stem cell transplantation was performed, achieving complete remission. Five patients died, three due to progression of disease, one in the course of secondary acute myeloid leukemia and one due to reasons not related to mastocytosis. Treatment is ongoing in seven patients. We found that midostaurin therapy is beneficial to patients with ASM. [ABSTRACT FROM AUTHOR]

Published

2021

31. Diagnosis of Primary Mast Cell Disorders in Anaphylaxis: Value of KIT D816V in Peripheral Blood.

Author

De Puysseleyr LP, Ebo DG, Elst J, Faber MA, Poorten MV, Van Gasse AL, Bridts CH, Mertens C, Van Houdt M, Hagendorens MM, Verlinden A, Vermeulen K, Maes MB, Berneman ZN, and Sabato V

Subjects

Humans, Mast Cells, Mutation, Proto-Oncogene Proteins c-kit genetics, Anaphylaxis diagnosis, Mastocytosis, Mastocytosis, Systemic diagnosis, Mastocytosis, Systemic genetics

Abstract

Background: Anaphylaxis is frequent in patients suffering from primary mast cell disorders (PMCDs). In patients without mastocytosis in the skin (MIS) and a baseline serum tryptase (bST) less than 30 ng/mL, the diagnosis of PMCD is challenging. In these patients, detection of the KIT D816V mutation in peripheral blood (PB) has been suggested as screening tool for a PMCD., Objective: In this study, we investigated whether KIT D816V in PB can contribute to the decision to perform a bone marrow (BM) biopsy in patients with anaphylaxis without MIS and a bST less than 30 ng/mL., Methods: We selected 74 patients with severe anaphylaxis without MIS and a bST less than 30 ng/mL. All underwent a BM biopsy. KIT D816V mutation was quantified in both PB and BM using digital droplet polymerase chain reaction (ddPCR)., Results: Diagnosis of a PMCD was established in 40 patients (54%). Median bST for patients with and without PMCD was, respectively, 9.5 ng/mL (range 4.2-27 ng/mL) and 4.9 ng/mL (range 2.2-20.3 ng/mL) (P <.001). KIT D816V in PB was detected in 16 out of 40 (40%) patients with PMCD. KIT D816V in BM was detected in 22 out of 40 (55%) patients with PMCD., Conclusions: In patients without MIS and a bST less than < 30 ng/mL who experience anaphylaxis, determination of KIT D816V mutation in PB is of limited help in deciding when to proceed to a BM biopsy. Therefore, KIT D816V in PB mutation analysis should be interpreted together with scoring tools to make a better assessment in identifying patients who should undergo BM biopsy., (Copyright © 2021 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)

Published

2021

32. Comparison of gDNA-based versus mRNA-based KIT D816V mutation analysis reveals large differences between blood and bone marrow in systemic mastocytosis

Author

Sigurd Broesby-Olsen, Carsten Bindslev-Jensen, Hanne Vestergaard, Thomas Kielsgaard Kristensen, and Michael Boe Møller

Subjects

0301 basic medicine, genomic DNA, DNA Mutational Analysis, Bone Marrow Cells, systemic mastocytosis, Biology, Real-Time Polymerase Chain Reaction, Sensitivity and Specificity, 03 medical and health sciences, 0302 clinical medicine, Mastocytosis, Systemic, blood, medicine, Humans, RNA, Messenger, Systemic mastocytosis, Alleles, Messenger RNA, Blood Cells, messenger RNA, Reproducibility of Results, KIT D816V mutation, DNA, Hematology, medicine.disease, Molecular biology, Kit d816v, Proto-Oncogene Proteins c-kit, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Cancer research, Bone marrow, human activities

Abstract

Keywords: systemic mastocytosis; KIT D816V mutation; blood; genomic DNA; messenger RNA

Published

2016

33. Advances in the classification and treatment of mastocytosis: Current status and outlook toward the future

Author

Wolfgang R. Sperr, Alberto Orfao, Michel Arock, Andreas Reiter, Cem Akin, K. Frank Austen, Luis Escribano, Karl Sotlar, Massimo Triggiani, Peter Valent, Daniel A. Arber, Gunnar Nilsson, Stephen J. Galli, Hans-Peter Horny, Karin Hartmann, Knut Brockow, Carsten Bindslev-Jensen, Hanneke C. Kluin-Nelemans, Petri T. Kovanen, Sigurd Broesby-Olsen, Tracy I. George, Dean D. Metcalfe, Lawrence B. Schwartz, Jason Gotlib, Olivier Hermine, Celalettin Ustun, National Institute of Allergy and Infectious Diseases (US), German Research Foundation, and Austrian Science Fund

Subjects

0301 basic medicine, Cancer Research, KIT D816V MUTATION, medicine.medical_treatment, Tryptase, Disease, Hematopoietic stem cell transplantation, Prognostication, PERIPHERAL-BLOOD, Article, Mastocytosis/classification, 03 medical and health sciences, chemistry.chemical_compound, URTICARIA PIGMENTOSA, 0302 clinical medicine, medicine, Humans, Midostaurin, Systemic mastocytosis, ADVANCED SYSTEMIC MASTOCYTOSIS, CONSENSUS PROPOSAL, OF-THE-ART, biology, Cutaneous Mastocytosis, business.industry, IN-VITRO, Mast cell leukemia, medicine.disease, C-KIT, 030104 developmental biology, chemistry, NEOPLASTIC MAST-CELLS, Oncology, 030220 oncology & carcinogenesis, Immunology, biology.protein, Mast cells, Disease Progression, Urticaria pigmentosa, BONE-MARROW MASTOCYTOSIS, business, KIT D816V, Mastocytosis

Abstract

Mastocytosis is a term used to denote a heterogeneous group of conditions defined by the expansion and accumulation of clonal (neoplastic) tissue mast cells in various organs. The classification of the World Health Organization (WHO) divides the disease into cutaneous mastocytosis, systemic mastocytosis, and localized mast cell tumors. On the basis of histomorphologic criteria, clinical parameters, and organ involvement, systemic mastocytosis is further divided into indolent systemic mastocytosis and advanced systemic mastocytosis variants, including aggressive systemic mastocytosis and mast cell leukemia. The clinical impact and prognostic value of this classification has been confirmed in numerous studies, and its basic concept remains valid. However, refinements have recently been proposed by the consensus group, the WHO, and the European Competence Network on Mastocytosis. In addition, new treatment options are available for patients with advanced systemic mastocytosis, including allogeneic hematopoietic stem cell transplantation and multikinase inhibitors directed against KIT D816V and other key signaling molecules. Our current article provides an overview of recent advances in the field of mastocytosis, with emphasis on classification, prognostication, and emerging new treatment options in advanced SM., This study was supported by the Austrian Science Funds, SFB grant F47-04 (to P.V.), by the German Research Council, grant HA 2393/6-1 (to K.H.) and by the NIAID Division of Intramural Research (to D.M.).

Published

2017

34. Proposed diagnostic algorithm for patients with suspected mastocytosis

Subjects

OF-THE-ART, mastocytosis, CONSECUTIVE ADULTS, KIT D816V MUTATION, tryptase, INDOLENT SYSTEMIC MASTOCYTOSIS, FUTURE PERSPECTIVES, mast cells, diagnostic algorithm, PROLIFERATIVE DISORDERS, SERUM TRYPTASE, TRYPTASE LEVELS, KIT D816V, MAST-CELL ACTIVATION, CONSENSUS PROPOSAL

Abstract

Mastocytosis is an emerging differential diagnosis in patients with more or less specific mediator-related symptoms. In some of these patients, typical skin lesions are found and the diagnosis of mastocytosis can be established. In other cases, however, skin lesions are absent, which represents a diagnostic challenge. In the light of this unmet need, we developed a diagnostic algorithm for patients with suspected mastocytosis. In adult patients with typical lesions of mastocytosis in the skin, a bone marrow (BM) biopsy should be considered, regardless of the basal serum tryptase concentration. In adults without skin lesions who suffer from mediator-related or other typical symptoms, the basal tryptase level is an important parameter. In those with a slightly increased tryptase level, additional investigations, including a sensitive KIT mutation analysis of blood leucocytes or measurement of urinary histamine metabolites, may be helpful. In adult patients in whom (i) KIT D816V is detected and/or (ii) the basal serum tryptase level is clearly increased (>25-30ng/ml) and/or (iii) other clinical or laboratory features suggest the presence of occult' mastocytosis or another haematologic neoplasm, a BM investigation is recommended. In the absence of KIT D816V and other signs or symptoms of mastocytosis or another haematopoietic disease, no BM investigation is required, but the clinical course and tryptase levels are monitored in the follow-up. In paediatric patients, a BM investigation is usually not required, even if the tryptase level is increased. Although validation is required, it can be expected that the algorithm proposed herein will facilitate the management of patients with suspected mastocytosis and help avoid unnecessary referrals and investigations.

Published

2014

35. Proposed diagnostic algorithm for patients with suspected mastocytosis: a proposal of the European Competence Network on Mastocytosis

Author

Knut Brockow, Cem Akin, Jason Gotlib, Peter Valent, H.-P. Horny, Thomas Kielsgaard Kristensen, Hanneke C. Kluin-Nelemans, J. J. Van Doormaal, Joseph H. Butterfield, Karin Hartmann, Lawrence B. Schwartz, Clive Grattan, Olivier Hermine, Bogusław Nedoszytko, Andreas Reiter, Dean D. Metcalfe, Marek Niedoszytko, Karl Sotlar, Iván Álvarez-Twose, Wolfgang R. Sperr, J. N. G. Oude Elberink, Michel Arock, Massimo Triggiani, Marcus Maurer, Mariana Castells, Luis Escribano, A. Orfao, Selim Yavuz, Deepti Radia, Sigurd Broesby-Olsen, Frank Siebenhaar, Austrian Science Fund, and National Institute of Allergy and Infectious Diseases (US)

Subjects

KIT D816V MUTATION, Urinary system, Immunology, tryptase, INDOLENT SYSTEMIC MASTOCYTOSIS, Tryptase, Diagnostic algorithm, mast cells, Disease, Biopsy, Humans, Immunology and Allergy, Medicine, TRYPTASE LEVELS, CONSENSUS PROPOSAL, OF-THE-ART, CONSECUTIVE ADULTS, biology, medicine.diagnostic_test, business.industry, FUTURE PERSPECTIVES, diagnostic algorithm, Occult, PROLIFERATIVE DISORDERS, Kit d816v, SERUM TRYPTASE, medicine.anatomical_structure, Mast cells, biology.protein, Bone marrow, Differential diagnosis, business, Algorithm, KIT D816V, MAST-CELL ACTIVATION, Algorithms, Mastocytosis

Abstract

Mastocytosis is an emerging differential diagnosis in patients with more or less specific mediator-related symptoms. In some of these patients, typical skin lesions are found and the diagnosis of mastocytosis can be established. In other cases, however, skin lesions are absent, which represents a diagnostic challenge. In the light of this unmet need, we developed a diagnostic algorithm for patients with suspected mastocytosis. In adult patients with typical lesions of mastocytosis in the skin, a bone marrow (BM) biopsy should be considered, regardless of the basal serum tryptase concentration. In adults without skin lesions who suffer from mediator-related or other typical symptoms, the basal tryptase level is an important parameter. In those with a slightly increased tryptase level, additional investigations, including a sensitive KIT mutation analysis of blood leucocytes or measurement of urinary histamine metabolites, may be helpful. In adult patients in whom (i) KIT D816V is detected and/or (ii) the basal serum tryptase level is clearly increased (>25-30 ng/ ml) and/or (iii) other clinical or laboratory features suggest the presence of 'occult' mastocytosis or another haematologic neoplasm, a BM investigation is recommended. In the absence of KIT D816V and other signs or symptoms of mastocytosis or another haematopoietic disease, no BM investigation is required, but the clinical course and tryptase levels are monitored in the follow-up. In paediatric patients, a BM investigation is usually not required, even if the tryptase level is increased. Although validation is required, it can be expected that the algorithm proposed herein will facilitate the management of patients with suspected mastocytosis and help avoid unnecessary referrals and investigations., This work was supported in part by the Austrian Science Funds (FWF) Project SFB F4611 and SFB F4704-B20 and the Division of Intramural Research, NIAID.

Published

2014

36. Practical management of adverse events in patients with advanced systemic mastocytosis receiving midostaurin.

Author

Gotlib J, Kluin-Nelemans HC, Akin C, Hartmann K, Valent P, and Reiter A

Subjects

Humans, Mutation, Quality of Life, Staurosporine adverse effects, Staurosporine analogs & derivatives, Mastocytosis, Systemic diagnosis, Mastocytosis, Systemic drug therapy

Abstract

Introduction: Systemic mastocytosis (SM) is characterized by the overproduction and accumulation of neoplastic mast cells (MCs) in the bone marrow, skin, and visceral organs. The KIT D816V mutation is found in approximately 90% of cases. In advanced SM (advSM), inferior survival often relates to MC-induced organ damage that may impact multiple organ systems. In addition, mediator symptoms related to MC activation can severely impact the quality of life. The oral multikinase/KIT inhibitor midostaurin was approved by the US Food and Drug Administration and the European Medicines Agency as monotherapy for advSM based on data from phase 2 clinical studies., Areas Covered: This review discusses the management of common adverse events (AEs) in patients with advSM who participated in phase 2 clinical studies that led to the approval of midostaurin., Expert Opinion: In the advSM population undergoing treatment with midostaurin, treatment-related AEs are often difficult to distinguish from disease-related symptoms, which can lead to premature discontinuation and improper dose reduction of midostaurin therapy in patients who might have benefitted from continued therapy. Here we present strategies to help optimize AE management and maximize the potential benefits of midostaurin in advSM.

Published

2021

37. Clinical presentation and management practice of systemic mastocytosis. A survey on 460 Italian patients

Author

Pieri, Lisa, Bonadonna, Patrizia, Elena, Chiara, Papayannidis, Cristina, Grifoni, Federica Irene, Rondoni, Michela, Girlanda, Stefania, Mauro, Marina, Magliacane, Diomira, Elli, Elena Maria, Iorno, Maria Loredana, Almerigogna, Fabio, Scarfì, Federica, Salerno, Roberto, Fanelli, Tiziana, Gesullo, Francesca, Corbizi Fattori, Giuditta, Bonifacio, Massimiliano, Perbellini, Omar, Artuso, Anna, Soverini, Simona, De Benedittis, Caterina, Muratori, Simona, Pravettoni, Valerio, Cova, Vittoria, Cortellini, Gabriele, Cortelezzi, Agostino, Martinelli, Giovanni, Triggiani, Massimo, Merante, Serena, Vannucchi, Alessandro Maria, Zanotti, Roberta, CICERI, FABIO, Pieri, L, Bonadonna, P, Elena, C, Papayannidis, C, Grifoni, Fi, Rondoni, M, Girlanda, S, Mauro, M, Magliacane, D, Elli, Em, Iorno, Ml, Almerigogna, F, Scarfì, F, Salerno, R, Fanelli, T, Gesullo, F, Corbizi Fattori, G, Bonifacio, M, Perbellini, O, Artuso, A, Soverini, S, De Benedittis, C, Muratori, S, Pravettoni, V, Cova, V, Cortellini, G, Ciceri, F, Cortelezzi, A, Martinelli, G, Triggiani, M, Merante, S, Vannucchi, Am, Zanotti, R., Pieri, Lisa, Bonadonna, Patrizia, Elena, Chiara, Papayannidis, Cristina, Grifoni, Federica Irene, Rondoni, Michela, Girlanda, Stefania, Mauro, Marina, Magliacane, Diomira, Elli, Elena Maria, Iorno, Maria Loredana, Almerigogna, Fabio, Scarfì, Federica, Salerno, Roberto, Fanelli, Tiziana, Gesullo, Francesca, Corbizi Fattori, Giuditta, Bonifacio, Massimiliano, Perbellini, Omar, Artuso, Anna, Soverini, Simona, De Benedittis, Caterina, Muratori, Simona, Pravettoni, Valerio, Cova, Vittoria, Cortellini, Gabriele, Ciceri, Fabio, Cortelezzi, Agostino, Martinelli, Giovanni, Triggiani, Massimo, Merante, Serena, Vannucchi, Alessandro Maria, and Zanotti, Roberta

Subjects

Adult, Male, Adolescent, KIT D816V MUTATION, PERIPHERAL-BLOOD, DIAGNOSIS, Young Adult, Mastocytosis, Systemic, indolent, Surveys and Questionnaires, Humans, mastocytosis,prognosis,indolent, POPULATION, Aged, Retrospective Studies, Aged, 80 and over, mastocytosis, Age Factors, Disease Management, Hematology, Middle Aged, Prognosis, Survival Rate, C-KIT, Early Diagnosis, Italy, Disease Progression, MAST-CELLS, Female, SPANISH NETWORK, BONE-MARROW MASTOCYTOSIS, CONSENSUS, LEUKEMIA

Abstract

Systemic mastocytosis is a rare heterogeneous myeloproliferative neoplasm characterized by abnormal proliferation and activation of mast cells. We describe a large multicentre series of 460 adult patients with systemic mastocytosis, with a diagnosis based on WHO 2008 criteria, in a “real-life” setting of ten Italian centers with dedicated multidisciplinary programs. We included indolent forms with (n = 255) and without (n = 165) skin lesions, smouldering (n = 20), aggressive (n = 28), associated with other hematological diseases mastocytosis (n = 21) and mast cell leukemia (n = 1). This series was uniquely characterized by a substantial proportion of patients with low burden of neoplastic mast cells; notably, 38% of cases were diagnosed using only minor diagnostic criteria according to WHO 2008 classification, underlying the feasibility of early diagnosis where all diagnostic approaches are made available. This has particular clinical relevance for prevention of anaphylaxis manifestations, that were typically associated with indolent forms. In multivariate analysis, the most important features associated with shortened overall survival were disease subtype and age at diagnosis >60 years. Disease progression was correlated with mastocytosis subtype and thrombocytopenia. As many as 32% of patients with aggressive mastocytosis suffered from early evolution into acute leukemia. Overall, this study provides novel information about diagnostic approaches and current presentation of patients with SM and underlines the importance of networks and specialized centers to facilitate early diagnosis and prevent disease-associated manifestations. Am. J. Hematol. 91:692–699, 2016. © 2016 Wiley Periodicals, Inc.

Published

2016

38. Multidisciplinary Management of Mastocytosis: Nordic Expert Group Consensus

Author

Lene H. Garvey, Charlotte G. Mortz, Gunnar Nilsson, Peter Valent, Thomas Kielsgaard Kristensen, Ole Weis Bjerrum, Leena Ackermann, Trine Torfing, Theo Gülen, Maria Sääf, Eva Stylianou, Carsten Bindslev-Jensen, Ingunn Dybedal, Hanne Vestergaard, Birgitta Sander, Michael Boe Møller, Troels Havelund, Marie Bendix, Sigurd Broesby-Olsen, Anna Bergström, Maria A Karlsson, Lone Agertoft, Kim Brixen, Hans Hägglund, Pernille Hermann, Department of Dermatology, Allergology and Venereology, and Clinicum

Subjects

Diagnostic criteria, Disease, BONE-MARROW HISTOPATHOLOGY, 030207 dermatology & venereal diseases, 0302 clinical medicine, Multidisciplinary approach, multidisciplinary management, Prevalence, TRYPTASE LEVELS, Systemic mastocytosis, CUTANEOUS-MASTOCYTOSIS, Mast cell activation, General Medicine, Classification, Expert group, 3. Good health, classification, 030220 oncology & carcinogenesis, Practice Guidelines as Topic, GASTROINTESTINAL-TRACT, MAST-CELL ACTIVATION, Mastocytosis, medicine.medical_specialty, Consensus, KIT D816V MUTATION, INDOLENT SYSTEMIC MASTOCYTOSIS, Dermatology, systemic mastocytosis, Scandinavian and Nordic Countries, World Health Organization, PEDIATRIC MASTOCYTOSIS, Mast cell, EUROPEAN COMPETENCE NETWORK, Diagnosis, Differential, 03 medical and health sciences, Multidisciplinary management, medicine, Humans, Intensive care medicine, RESPONSE CRITERIA, Urticaria pigmentosa, business.industry, Cutaneous Mastocytosis, Congresses as Topic, medicine.disease, 3121 General medicine, internal medicine and other clinical medicine, diagnostic criteria, Immunology, Differential diagnosis, mast cell, business, urticaria pigmentosa

Abstract

Mastocytosis is a heterogeneous group of diseases defined by an increased number and accumulation of mast cells, and often also by signs and symptoms of mast cell activation. Disease subtypes range from indolent to rare aggressive forms. Mastocytosis affects people of all ages and has been considered rare; however, it is probably underdiagnosed with potential severe implications. Diagnosis can be challenging and symptoms may be complex and involve multiple organ-systems. In general it is advised that patients should be referred to centres with experience in the disease offering an individualized, multidisciplinary approach. We present here consensus recommendations from a Nordic expert group for the diagnosis and general management of patients with mastocytosis.

Published

2015

39. A Rare Case of Systemic Mastocytosis With Associated Clonal Hematological Non-Mast Cell Lineage Disease That Transformed to Acute Leukemia With IDH2 Mutation.

Author

Liman AD, Shields J, and Liman AK

Abstract

An elderly 72-year-old man presented with anemia, thrombocytopenia, monocytosis, splenomegaly and lymphadenopathy. Bone marrow biopsy was consistent with mast cell neoplasm with positive CD117, CD25, CD34 myeloblasts and polymerase chain reaction (PCR) revealed mutation of D816V. He developed bilateral femoral neck fractures and biopsy confirmed that he has systemic mastocytosis (SM). He received cladribine and midostaurin with stable disease for 21 months. His SM with associated clonal hematological non-mast cell lineage disease (SM-AHNMD) transformed to acute myelogenous leukemia with isocitrate dehydrogenase 2 ( IDH2 ) mutation. A trial of enasidenib was given for 5 months but without any response. Patient decided to go with home hospice and died afterwards., Competing Interests: None to declare., (Copyright 2020, Liman et al.)

Published

2020

40. New Approach to Paediatric Mastocytosis: Implications of KIT D816V Mutation Detection in Peripheral Blood.

Author

Czarny J, Żuk M, Zawrocki A, Plata-Nazar K, Biernat W, Niedoszytko M, Ługowska-Umer H, Nedoszytko B, Wasąg B, Nowicki RJ, and Lange M

Subjects

Adolescent, Age Factors, Child, Child, Preschool, Female, Genetic Predisposition to Disease, Humans, Infant, Male, Mastocytosis, Cutaneous diagnosis, Mastocytosis, Systemic diagnosis, Phenotype, Predictive Value of Tests, Skin pathology, DNA Mutational Analysis, Mastocytosis, Cutaneous genetics, Mastocytosis, Systemic genetics, Mutation, Proto-Oncogene Proteins c-kit genetics

Abstract

is missing (Short communication).

Published

2020

41. Highly sensitive assays are mandatory for the differential diagnosis of patients presenting with symptoms of mast cell activation: diagnostic work-up of 38 patients.

Author

Van den Poel B, Kochuyt AM, Del Biondo E, Dewaele B, Lierman E, Tousseyn T, de Hertogh G, Vandenberghe P, and Boeckx N

Subjects

Adolescent, Adult, Aged, Child, Diagnosis, Differential, Female, Humans, Male, Middle Aged, Retrospective Studies, Young Adult, Mastocytosis, Systemic diagnosis

Abstract

Mastocytosis is a heterogeneous disease caused by excessive mast cell (MC) proliferation. Diagnosis of systemic mastocytosis (SM) is based on the presence of major and minor criteria defined by the World Health Organization. Symptoms of MC activation can also occur in patients without SM or without allergic or inflammatory disease. These MC activation syndromes (MCAS) can be divided into primary (monoclonal) MCAS (MMAS) vs. secondary and idiopathic MCAS. In this single center study, the diagnostic work-up of 38 patients with a clinical suspicion of SM and/or with elevated basic tryptase levels is presented. Clinical symptoms, biochemical parameters, results of bone marrow investigation, flow cytometric immunophenotyping, and molecular analysis were retrospectively reviewed. Twenty-three patients were found to have a monoclonal MC disorder of which 19 were diagnosed with SM and 4 with MMAS. In 13/19 SM patients, multifocal MC infiltrates in the bone marrow were found (major criterion), while in 6 the diagnosis was based on the presence of ≥3 minor criteria. Flow cytometric analysis of bone marrow showed CD25 expression of MCs in all patients with SM and MMAS (range: 0.002-0.3% of cells). In bone marrow, the KIT D816V mutation was detected in all SM patients but in only 2 patients with MMAS (range: 0.007-9% mutated cells). Basic tryptase elevation was demonstrated in 16/19 patients with SM but also in 9/19 patients without SM. Our study reveals the heterogeneity of primary MC disorders and the importance of sensitive assays in patients suspected of having SM.

Published

2017