Your search keyword '"Arock, Michel"' showing total 29 results

1. Proposed European Competence Network on Mastocytosis—American Initiative in Mast Cell Diseases (ECNM-AIM) Response Criteria in Advanced Systemic Mastocytosis

Author

Charles and Ann Johnson Foundation, Josep Carreras Leukemia Foundation, National Institute of Allergy and Infectious Diseases (US), Gotlib, Jason, Schwaab, Juliana, Shomali, William, George, Tracy I., Radia, Deepti, Castells, Mariana, Carter, Melody C., Hartmann, Karin, Álvarez-Twos, Iván, Brockow, Knut, Bonadonna, Patrizia, Hermine, Olivier, Niedoszytko, Marek, Hoermann, Gregor, Sperr, Wolfgang R., Oude Elberink, Hanneke, Siebenhaar, Frank, Butterfield, Joseph H., Ustun, Celalettin, Zanotti, Roberta, Triggiani, Massimo, Schwartz, Lawrence B., Lyons, Jonathan J., Orfao, Alberto, Sotlar, Karl, Horny, Hans-Peter, Arock, Michel, Metcalfe, Dean D., Akin, Cem, Lübke, Johannes, Valent, Peter, Reiter, Andreas, Charles and Ann Johnson Foundation, Josep Carreras Leukemia Foundation, National Institute of Allergy and Infectious Diseases (US), Gotlib, Jason, Schwaab, Juliana, Shomali, William, George, Tracy I., Radia, Deepti, Castells, Mariana, Carter, Melody C., Hartmann, Karin, Álvarez-Twos, Iván, Brockow, Knut, Bonadonna, Patrizia, Hermine, Olivier, Niedoszytko, Marek, Hoermann, Gregor, Sperr, Wolfgang R., Oude Elberink, Hanneke, Siebenhaar, Frank, Butterfield, Joseph H., Ustun, Celalettin, Zanotti, Roberta, Triggiani, Massimo, Schwartz, Lawrence B., Lyons, Jonathan J., Orfao, Alberto, Sotlar, Karl, Horny, Hans-Peter, Arock, Michel, Metcalfe, Dean D., Akin, Cem, Lübke, Johannes, Valent, Peter, and Reiter, Andreas

Abstract

Advanced systemic mastocytosis (AdvSM) is characterized by the presence of KIT D816V and other somatic mutations (eg, in SRSF2, ASXL1, and RUNX1) in 95% and 60% to 70% of patients, respectively. The biological and clinical consequences of AdvSM include multilineage involvement (eg, associated hematologic neoplasm) in 60% to 80% of patients, variable infiltration and damage (C-findings) of predominantly bone marrow and visceral organs through affected mast cell (MC) and non-MC lineages, and elevated levels of serum tryptase. Recently, the treatment landscape has substantially changed with the introduction of the multikinase/KIT inhibitor midostaurin and the selective KIT D816V inhibitor avapritinib. In this review, we discuss the evolution of AdvSM response criteria that have been developed to better capture clinical benefit (eg, improved responses and progression-free and overall survival). We propose refined response criteria from European Competence Network on Mastocytosis and American Initiative in Mast Cell Diseases investigators that use a tiered approach to segregate the effects of histopathologic (eg, bone marrow MC burden, tryptase), molecular (eg, KIT D816V variant allele frequency), clinical (eg, C-findings), and symptom response on long-term outcomes. These response criteria require evaluation in future prospective clinical trials of selective KIT inhibitors and other novel agents.

Published

2022

2. Refined treatment response criteria for indolent systemic mastocytosis proposed by the ECNM-AIM consortium

Author

National Institute of Allergy and Infectious Diseases (US), National Institutes of Health (US), Medical University of Gdańsk, Austrian Science Fund, Pyatilova, Polina, Akin, Cem, Álvarez-Twose, Iván, Arock, Michel, Bonadonna, Patrizia, Brockow, Knut, Butterfield, Joseph H., Broesby-Olsen, Sigurd, Carter, Melody C., Castells, Mariana, George, Tracy I., Gotlib, Jason, Greiner, Georg, Gulen, Theo, Hartmann, Karin, Hermine, Olivier, Horny, Hans-Peter, Jawhar, Mohamad, Lange, Magdalena, Lyons, Jonathan J., Maurer, Marcus, Metcalfe, Dean D., Nedoszytko, Boguslaw, Niedoszytko, Marek, Orfao, Alberto, Reiter, Andreas, Schwaab, Juliana, Sotlar, Karl, Sperr, Wolfgang R., Triggiani, Massimo, Valent, Peter, Siebenhaar, Frank, National Institute of Allergy and Infectious Diseases (US), National Institutes of Health (US), Medical University of Gdańsk, Austrian Science Fund, Pyatilova, Polina, Akin, Cem, Álvarez-Twose, Iván, Arock, Michel, Bonadonna, Patrizia, Brockow, Knut, Butterfield, Joseph H., Broesby-Olsen, Sigurd, Carter, Melody C., Castells, Mariana, George, Tracy I., Gotlib, Jason, Greiner, Georg, Gulen, Theo, Hartmann, Karin, Hermine, Olivier, Horny, Hans-Peter, Jawhar, Mohamad, Lange, Magdalena, Lyons, Jonathan J., Maurer, Marcus, Metcalfe, Dean D., Nedoszytko, Boguslaw, Niedoszytko, Marek, Orfao, Alberto, Reiter, Andreas, Schwaab, Juliana, Sotlar, Karl, Sperr, Wolfgang R., Triggiani, Massimo, Valent, Peter, and Siebenhaar, Frank

Abstract

Indolent systemic mastocytosis (ISM) has a favorable prognosis and normal life expectancy. However, many patients suffer from mast cell (MC) mediator-related symptoms, which significantly affect quality of life (QoL). Cutaneous, gastrointestinal, and neurological complaints, musculoskeletal pain, and the presence of skin lesions, anaphylaxis, and osteoporosis are the main symptoms and signs in ISM and must be assessed in all patients before and during treatment. Validated mastocytosis-specific patient-reported outcome measures (PROMs) should be used for this purpose. Serum tryptase and KIT D816V allele burden are recommended as secondary outcome parameters, noting that they do not reflect the severity of signs, symptoms, and related QoL impairment, but indirectly express MC burden. Changes from baseline of 90%, 60%, and 30% indicate complete response >90%, major response 60% to 90%, partial response 30% to 60%, and no response <30% to treatment. To conclude, we recommend the use of PROMs as primary outcome parameters to define treatment response in patients with ISM in clinical trials and in everyday clinical practice.

Published

2022

3. Standards of genetic testing in the diagnosis and prognostication of systemic mastocytosis in 2022: Recommendations of the EU-US cooperative group

Author

National Institute of Allergy and Infectious Diseases (US), National Institutes of Health (US), Austrian Science Fund, Hoermann, Gregor, Sotlar, Karl, Jawhar, Mohamad, Kristensen, Thomas K., Bachelot, Guillaume, Nedoszytko, Boguslaw, Carter, Melody C., Horny, Hans-Peter, Bonadonna, Patrizia, Sperr, Wolfgang R., Hartmann, Karin, Brockow, Knut, Lyons, Jonathan J., Kluin-Nelemans, Hanneke C., Hermine, Olivier, Akin, Cem, Broesby-Olsen, Sigurd, Triggiani, Massimo, Butterfield, Joseph H., Schwaab, Juliana, Arock, Michel, National Institute of Allergy and Infectious Diseases (US), National Institutes of Health (US), Austrian Science Fund, Hoermann, Gregor, Sotlar, Karl, Jawhar, Mohamad, Kristensen, Thomas K., Bachelot, Guillaume, Nedoszytko, Boguslaw, Carter, Melody C., Horny, Hans-Peter, Bonadonna, Patrizia, Sperr, Wolfgang R., Hartmann, Karin, Brockow, Knut, Lyons, Jonathan J., Kluin-Nelemans, Hanneke C., Hermine, Olivier, Akin, Cem, Broesby-Olsen, Sigurd, Triggiani, Massimo, Butterfield, Joseph H., Schwaab, Juliana, and Arock, Michel

Abstract

Mastocytosis comprises rare heterogeneous diseases characterized by an increased accumulation of abnormal mast cells in various organs/tissues. The pathogenesis of mastocytosis is strongly linked to the presence of KIT-activating mutations. In systemic mastocytosis (SM), the most frequent mutation encountered is KIT p.D816V, whose presence constitutes one of the minor diagnostic criteria. Different techniques are used to search and quantify the KIT p.D816V mutant; however, allele-specific quantitative PCR and droplet digital PCR are today the most sensitive. The analysis of the KIT p.D816V allele burden has undeniable interest for diagnostic, prognostic, and therapeutic monitoring. The analysis of non–mast cell hematological compartments in SM is similarly important because KIT p.D816V multilineage involvement is associated with a worse prognosis. In addition, in advanced forms of SM, mutations in genes other than KIT are frequently identified and affect negatively disease outcome and response to therapy. Thus, combined quantitative and sensitive analysis of KIT mutations and next-generation sequencing of other recurrently involved myeloid genes make it possible to better characterize the extent of the affected cellular compartments and additional molecular aberrations, providing a more detailed overview of the complex mutational landscape of SM, in relation with the clinical heterogeneity of the disease. In this article, we report the latest recommendations of the EU-US Cooperative Group presented in September 2020 in Vienna during an international working conference, on the techniques we consider standard to detect and quantify the KIT p.D816V mutant in SM and additional myeloid mutations found in SM subtypes.

Published

2022

4. Clinical impact and proposed application of molecular markers, genetic variants, and cytogenetic analysis in mast cell neoplasms: Status 2022

Author

Arock, Michel, Hoermann, Gregor, Sotlar, Karl, Hermine, Olivier, Sperr, Wolfgang R., Hartmann, Karin, Brockow, Knut, Akin, Cem, Triggiani, Massimo, Broesby-Olsen, Sigurd, Reiter, Andreas, Gotlib, Jason, Horny, Hans-Peter, Orfao, Alberto, Metcalfe, Dean D., Valent, Peter, Arock, Michel, Hoermann, Gregor, Sotlar, Karl, Hermine, Olivier, Sperr, Wolfgang R., Hartmann, Karin, Brockow, Knut, Akin, Cem, Triggiani, Massimo, Broesby-Olsen, Sigurd, Reiter, Andreas, Gotlib, Jason, Horny, Hans-Peter, Orfao, Alberto, Metcalfe, Dean D., and Valent, Peter

Abstract

Mast cell neoplasms are an emerging challenge in the fields of internal medicine, allergy, immunology, dermatology, laboratory medicine, and pathology. In this review, we discuss the current standards for the diagnosis and prognostication of mast cell neoplasms with special reference to clinically relevant germline and somatic gene variants. In patients with cutaneous mastocytosis or with indolent systemic mastocytosis (SM), various KIT-activating mutations act as key molecular drivers of the disease. In adults, KIT p.D816V is by far the most prevalent driver, whereas other KIT mutants are detected in nearly 40% of children. In advanced SM, including aggressive SM, SM with an associated hematological neoplasm, and mast cell leukemia, additional somatic mutations in other genes, such as SRSF2, JAK2, RUNX1, ASXL1, or RAS, may be detected. These drivers are more frequently detected in SM with an associated hematological neoplasm, particularly in male patients. Recently, hereditary alpha-tryptasemia has been identified as a genetic trait more prevalent in SM compared with healthy controls. Moreover, hereditary alpha-tryptasemia is more frequent in patients with SM with Hymenoptera venom allergy and severe mediator-related symptoms than in patients with SM without symptoms. On the basis of this knowledge, we propose a diagnostic algorithm in which genetic markers are applied together with clinical and histopathologic criteria to establish the diagnosis and prognosis in SM.

Published

2022

5. Scoring the Risk of Having Systemic Mastocytosis in Adult Patients with Mastocytosis in the Skin

Author

Fuchs, David, Kilbertus, Alex, Kofler, Karin, von Bubnoff, Nikolas, Shoumariyeh, Khalid, Zanotti, Roberta, Bonadonna, Patrizia, Scaffidi, Luigi, Doubek, Michael, Elberink, Hanneke Oude, Span, Lambert F. R., Hermine, Olivier, Elena, Chiara, Benvenuti, Pietro, Yavuz, Akif Selim, Brockow, Knut, Zink, Alexander, Aberer, Elisabeth, Gorska, Aleksandra, Romantowski, Jan, Hadzijusufovic, Emir, Fortina, Anna Belloni, Caroppo, Francesca, Perkins, Cecelia, Illerhaus, Anja, Panse, Jens, Vucinic, Vladan, Jawhar, Mohamad, Sabato, Vito, Triggiani, Massimo, Parente, Roberta, Bergstrom, Anna, Breynaert, Christine, Gotlib, Jason, Reiter, Andreas, Hartmann, Karin, Niedoszytko, Marek, Arock, Michel, Kluin-Nelemans, Hanneke C., Sperr, Wolfgang R., Greul, Rosemarie, Valent, Peter, Fuchs, David, Kilbertus, Alex, Kofler, Karin, von Bubnoff, Nikolas, Shoumariyeh, Khalid, Zanotti, Roberta, Bonadonna, Patrizia, Scaffidi, Luigi, Doubek, Michael, Elberink, Hanneke Oude, Span, Lambert F. R., Hermine, Olivier, Elena, Chiara, Benvenuti, Pietro, Yavuz, Akif Selim, Brockow, Knut, Zink, Alexander, Aberer, Elisabeth, Gorska, Aleksandra, Romantowski, Jan, Hadzijusufovic, Emir, Fortina, Anna Belloni, Caroppo, Francesca, Perkins, Cecelia, Illerhaus, Anja, Panse, Jens, Vucinic, Vladan, Jawhar, Mohamad, Sabato, Vito, Triggiani, Massimo, Parente, Roberta, Bergstrom, Anna, Breynaert, Christine, Gotlib, Jason, Reiter, Andreas, Hartmann, Karin, Niedoszytko, Marek, Arock, Michel, Kluin-Nelemans, Hanneke C., Sperr, Wolfgang R., Greul, Rosemarie, and Valent, Peter

Abstract

BACKGROUND: Mastocytosis in adults often presents with skin lesions. A bone marrow biopsy is necessary to confirm or exclude the presence of systemic mastocytosis (SM) in these cases. When a bone marrow biopsy is not performed, the provisional diagnosis is mastocytosis in the skin (MIS). No generally accepted scoring system has been established to estimate the risk of SM in these patients. OBJECTIVE: To develop a risk score to predict SM in adults with MIS. METHODS: We examined 1145 patients with MIS from the European Competence Network on Mastocytosis Registry who underwent a bone marrow biopsy. A total of 944 patients had SM and 201 patients had cutaneous mastocytosis; 63.7% were female, and 36.3% were male. Median age was 44 +/- 13.3 years. The median serum tryptase level amounted to 29.3 +/- 81.9 ng/mL. We established a multivariate regression model using the whole population of patients as a training and validation set (bootstrapping). A risk score was developed and validated with receiver-operating curves. RESULTS: In the multivariate model, the tryptase level (P < .001), constitutional/cardiovascular symptoms (P = .014), and bone symptoms/osteoporosis (P < .001) were independent predictors of SM (P < .001; sensitivity, 90.7%; specificity, 69.1%). A 6-point risk score was established (risk, 10.7%-98.0%) and validated. CONCLUSIONS: Using a large data set of the European Competence Network on Mastocytosis Registry, we created a risk score to predict the presence of SM in patients with MIS. Although the score will need further validation in independent cohorts, our score seems to discriminate safely between patients with SM and with pure cutaneous mastocytosis. (C) 2020 American Academy of Allergy, Asthma & Immunology

Published

2021

6. COVID-19 Vaccination in Mastocytosis: Recommendations of the European Competence Network on Mastocytosis (ECNM) and American Initiative in Mast Cell Diseases (AIM)

Author

Bonadonna, Patrizia, Brockow, Knut, Niedoszytko, Marek, Elberink, Hanneke Oude, Akin, Cem, Nedoszytko, Boguslaw, Butterfield, Joseph H., Alvarez-Twose, Ivan, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Castells, Mariana, Sperr, Wolfgang R., Hermine, Olivier, Gotlib, Jason, Zanotti, Roberta, Reiter, Andreas, Broesby-Olsen, Sigurd, Bindslev-Jensen, Carsten, Schwartz, Lawrence B., Horny, Hans-Peter, Radia, Deepti, Triggiani, Massimo, Sabato, Vito, Carter, Melody C., Siebenhaar, Frank, Orfao, Alberto, Grattan, Clive, Metcalfe, Dean D., Arock, Michel, Gulen, Theo, Hartmann, Karin, Valent, Peter, Bonadonna, Patrizia, Brockow, Knut, Niedoszytko, Marek, Elberink, Hanneke Oude, Akin, Cem, Nedoszytko, Boguslaw, Butterfield, Joseph H., Alvarez-Twose, Ivan, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Castells, Mariana, Sperr, Wolfgang R., Hermine, Olivier, Gotlib, Jason, Zanotti, Roberta, Reiter, Andreas, Broesby-Olsen, Sigurd, Bindslev-Jensen, Carsten, Schwartz, Lawrence B., Horny, Hans-Peter, Radia, Deepti, Triggiani, Massimo, Sabato, Vito, Carter, Melody C., Siebenhaar, Frank, Orfao, Alberto, Grattan, Clive, Metcalfe, Dean D., Arock, Michel, Gulen, Theo, Hartmann, Karin, and Valent, Peter

Abstract

Mastocytosis is a neoplasm characterized by an accumulation of mast cells in various organs and increased risk for severe anaphylaxis in patients with concomitant allergies. Coronavirus disease 2019 (COVID-19) is a pandemic that is associated with a relatively high rate of severe lung disease and mortality. The mortality is particularly high in those with certain comorbidities and increases with age. Recently, several companies have developed an effective vaccination against COVID-19. Although the reported frequency of severe side effects is low, there is an emerging discussion about the safety of COVID-19 vaccination in patients with severe allergies and mastocytosis. However, even in these patients, severe adverse reactions are rare. We therefore recommend the broad use of COVID-19 vaccination in patients with mastocytosis on a global basis. The only well-established exception is a known or suspected allergy against a constituent of the vaccine. Safety measures, including premedication and postvaccination observation, should be considered in all patients with mastocytosis, depending on the individual personal risk and overall situation in each case. The current article provides a summary of published data, observations, and expert opinion that form the basis of these recommendations. (C) 2021 American Academy of Allergy, Asthma & Immunology

Published

2021

7. Selecting the Right Criteria and Proper Classification to Diagnose Mast Cell Activation Syndromes: A Critical Review

Author

Gulen, Theo, Akin, Cem, Bonadonna, Patrizia, Siebenhaar, Frank, Broesby-Olsen, Sigurd, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Oude Elberink, Hanneke, Butterfield, Joseph H., Sperr, Wolfgang R., Álvarez-Twose, Iván, Horny, Hans-Peter, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Zanotti, Roberta, Nilsson, Gunnar, Lyons, Jonathan J., Carter, Melody C., George, Tracy I., Hermine, Olivier, Gotlib, Jason, Orfao, Alberto, Triggiani, Massimo, Reiter, Andreas, Hartmann, Karin, Castells, Mariana, Arock, Michel, Schwartz, Lawrence B., Metcalfe, Dean D., Valent, Peter, Gulen, Theo, Akin, Cem, Bonadonna, Patrizia, Siebenhaar, Frank, Broesby-Olsen, Sigurd, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Oude Elberink, Hanneke, Butterfield, Joseph H., Sperr, Wolfgang R., Álvarez-Twose, Iván, Horny, Hans-Peter, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Zanotti, Roberta, Nilsson, Gunnar, Lyons, Jonathan J., Carter, Melody C., George, Tracy I., Hermine, Olivier, Gotlib, Jason, Orfao, Alberto, Triggiani, Massimo, Reiter, Andreas, Hartmann, Karin, Castells, Mariana, Arock, Michel, Schwartz, Lawrence B., Metcalfe, Dean D., and Valent, Peter

Abstract

In recent years, knowledge about mechanisms underlying mast cell activation (MCA) and accumulation in various pathologic conditions increased substantially. In addition, criteria and a classification of MCA syndromes (MCASs) have been set forth. MCAS is defined by typical clinical symptoms, a substantial increase in serum tryptase level during an attack over the patient's baseline tryptase, and a response of the symptoms to drugs targeting mast cells, mediator production, and/or mediator effects. Alternative diagnostic criteria of MCAS have also been suggested, but these alternative criteria often lack specificity and validation. In this report, we critically review the contemporary literature relating to MCAS and compare the specificity, sensitivity, and strength of MCAS-related parameters within proposals to diagnose and classify MCAS and its variants. Furthermore, we highlight the need to apply specific consensus criteria in the evaluation and classification of MCAS in individual patients. This is an urgent and important medical necessity because as an increasing number of patients are being given a misdiagnosis of MCAS based on nonspecific criteria, which contributes to confusion and frustration by patients and caregivers and sometimes may delay recognition and treatment of correct medical conditions that often turn out to be unrelated to MCA.

Published

2021

8. Proceedings from the Inaugural American Initiative in Mast Cell Diseases (AIM) Investigator Conference

Author

National Institutes of Health (US), Charles and Ann Johnson Foundation, National Institute of Allergy and Infectious Diseases (US), American Academy of Allergy Asthma and Immunology, Austrian Science Fund, Gotlib, Jason, George, Tracy I., Carter, Melody C., Austen, K. Frank, Bochner, Bruce, Dwyer, Daniel, Lyons, Jonathan J., Hamilton, Matthew J., Butterfield, Joseph H., Bonadonna, Patrizia, Weiler, Catherine, Galli, Stephen J., Schwartz, Lawrence B., Oude Elberink, Hanneke, Maitland, Anne, Theoharides, Theoharis, Ustun, Celalettin, Horny, Hans-Peter, Orfao, Alberto, Deininger, Michael, Radia, Deepti, Jawhar, Mohamad, Kluin-Nelemans, Hanneke C., Metcalfe, Dean D., Arock, Michel, Sperr, Wolfgang R., Valent, Peter, Castells, Mariana, Akin, Cem, National Institutes of Health (US), Charles and Ann Johnson Foundation, National Institute of Allergy and Infectious Diseases (US), American Academy of Allergy Asthma and Immunology, Austrian Science Fund, Gotlib, Jason, George, Tracy I., Carter, Melody C., Austen, K. Frank, Bochner, Bruce, Dwyer, Daniel, Lyons, Jonathan J., Hamilton, Matthew J., Butterfield, Joseph H., Bonadonna, Patrizia, Weiler, Catherine, Galli, Stephen J., Schwartz, Lawrence B., Oude Elberink, Hanneke, Maitland, Anne, Theoharides, Theoharis, Ustun, Celalettin, Horny, Hans-Peter, Orfao, Alberto, Deininger, Michael, Radia, Deepti, Jawhar, Mohamad, Kluin-Nelemans, Hanneke C., Metcalfe, Dean D., Arock, Michel, Sperr, Wolfgang R., Valent, Peter, Castells, Mariana, and Akin, Cem

Abstract

The American Initiative in Mast Cell Diseases (AIM) held its inaugural investigator conference at Stanford University School of Medicine in May 2019. The overarching goal of this meeting was to establish a Pan-American organization of physicians and scientists with multidisciplinary expertise in mast cell disease. To serve this unmet need, AIM envisions a network where basic, translational, and clinical researchers could establish collaborations with both academia and biopharma to support the development of new diagnostic methods, enhanced understanding of the biology of mast cells in human health and disease, and the testing of novel therapies. In these AIM proceedings, we highlight selected topics relevant to mast cell biology and provide updates regarding the recently described hereditary alpha-tryptasemia. In addition, we discuss the evaluation and treatment of mast cell activation (syndromes), allergy and anaphylaxis in mast cell disorders, and the clinical and biologic heterogeneity of the more indolent forms of mastocytosis. Because mast cell disorders are relatively rare, AIM hopes to achieve a coordination of scientific efforts not only in the Americas but also in Europe by collaborating with the well-established European Competence Network on Mastocytosis.

Published

2021

9. SARS-CoV-2 in Mast Cell Disorders

Author

Valent, Peter, Akin, Cem, Bonadonna, Patrizia, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Butterfield, Joseph H., Álvarez-Twose, Iván, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Reiter, Andreas, Castells, Mariana, Sperr, Wolfgang R., Kluin-Nelemans, Hanneke C., Hermine, Olivier, Gotlib, Jason, Zanotti, Roberta, Broesby-Olsen, Sigurd, Horny, Hans-Peter, Triggiani, Massimo, Siebenhaar, Frank, Orfao, Alberto, Metcalfe, Dean D., Arock, Michel, Hartmann, Karin, Austrian Science Fund, Charles and Ann Johnson Foundation, and National Institute of Allergy and Infectious Diseases (US)

Subjects

Coronavirus, SARS-CoV-2, Mast Cell Activation Syndrome, Tryptase, COVID-19, Mast Cells, Mastocytosis, KITD816V

Abstract

The COVID-19 (SARS-CoV-2) pandemic has massively distorted our health care systems and caused catastrophic consequences in our affected communities. The number of victims continues to increase and patients at risk can only be protected to a degree, since the virulent state may be asymptomatic. Risk factors concerning COVID-19-induced morbidity and mortality include advanced age, an impaired immune system, cardiovascular or pulmonary diseases, obesity, diabetes mellitus, and cancer treated with chemotherapy. Here within, we discuss the risk and impact of COVID-19 in patients with mastocytosis and mast cell activation syndromes. As no published data are yet available, expert opinions are, by necessity, based on case experience and reports from patients. Whereas the overall risk to acquire the SARS-CoV-2 virus may not be elevated in mast cell disease, certain conditions may increase the risk of infected patients to develop severe COVID-19. These factors include certain co-morbidities, mast cell activation-related events affecting the cardiovascular or bronchopulmonary system and chemotherapy or immunosuppressive drugs. Therefore, such treatments should be carefully evaluated on a case-by-case basis during a COVID-19 infection. By contrast, other therapies, such as anti-mediator-type drugs, venom immunotherapy, or vitamin D, should be continued. Overall, patients with mast cell disorders should follow the general and local guidelines in the COVID-19 pandemic and advice from their medical provider., P.V. was supported by the Austrian Science Fund (FWF), projects P32470-B and 46 F4704-B20. J.G. is supported by the Charles and Ann Johnson Foundation. 47 D.D.M. is supported by the Division of Intramural Research, NIAID.

Published

2020

10. Risk and management of patients with mastocytosis and MCAS in the SARS-CoV-2 (COVID-19) pandemic: Expert opinions

Author

Austrian Science Fund, Charles and Ann Johnson Foundation, National Institute of Allergy and Infectious Diseases (US), Valent, Peter, Akin, Cem, Bonadonna, Patrizia, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Butterfield, Joseph H., Álvarez-Twose, Iván, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Reiter, Andreas, Castells, Mariana, Sperr, Wolfgang R., Kluin-Nelemans, Hanneke C., Hermine, Olivier, Gotlib, Jason, Zanotti, Roberta, Broesby-Olsen, Sigurd, Horny, Hans-Peter, Triggiani, Massimo, Siebenhaar, Frank, Orfao, Alberto, Metcalfe, Dean D., Arock, Michel, Hartmann, Karin, Austrian Science Fund, Charles and Ann Johnson Foundation, National Institute of Allergy and Infectious Diseases (US), Valent, Peter, Akin, Cem, Bonadonna, Patrizia, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Butterfield, Joseph H., Álvarez-Twose, Iván, Sotlar, Karl, Schwaab, Juliana, Jawhar, Mohamad, Reiter, Andreas, Castells, Mariana, Sperr, Wolfgang R., Kluin-Nelemans, Hanneke C., Hermine, Olivier, Gotlib, Jason, Zanotti, Roberta, Broesby-Olsen, Sigurd, Horny, Hans-Peter, Triggiani, Massimo, Siebenhaar, Frank, Orfao, Alberto, Metcalfe, Dean D., Arock, Michel, and Hartmann, Karin

Abstract

The COVID-19 (SARS-CoV-2) pandemic has massively distorted our health care systems and caused catastrophic consequences in our affected communities. The number of victims continues to increase and patients at risk can only be protected to a degree, since the virulent state may be asymptomatic. Risk factors concerning COVID-19-induced morbidity and mortality include advanced age, an impaired immune system, cardiovascular or pulmonary diseases, obesity, diabetes mellitus, and cancer treated with chemotherapy. Here within, we discuss the risk and impact of COVID-19 in patients with mastocytosis and mast cell activation syndromes. As no published data are yet available, expert opinions are, by necessity, based on case experience and reports from patients. Whereas the overall risk to acquire the SARS-CoV-2 virus may not be elevated in mast cell disease, certain conditions may increase the risk of infected patients to develop severe COVID-19. These factors include certain co-morbidities, mast cell activation-related events affecting the cardiovascular or bronchopulmonary system and chemotherapy or immunosuppressive drugs. Therefore, such treatments should be carefully evaluated on a case-by-case basis during a COVID-19 infection. By contrast, other therapies, such as anti-mediator-type drugs, venom immunotherapy, or vitamin D, should be continued. Overall, patients with mast cell disorders should follow the general and local guidelines in the COVID-19 pandemic and advice from their medical provider.

Published

2020

11. Proposed Terminology and Classification of Pre-Malignant Neoplastic Conditions: A Consensus Proposal

Author

Valent, Peter, Akin, Cem, Arock, Michel, Bock, Christoph, George, Tracy I., Galli, Stephen J., Gotlib, Jason, Haferlach, Torsten, Hoermann, Gregor, Hermine, Olivier, Jäger, Ulrich, Kenner, Lukas, Kreipe, Hans, Majeti, Ravindra, Metcalfe, Dean D., Orfao, Alberto, Reiter, Andreas, Sperr, Wolfgang R., Staber, Philipp B., Sotlar, Karl, Schiffer, Charles, Superti-Furga, Giulio, and Horny, Hans-Peter

Subjects

lcsh:R5-920, Cell Transformation, Neoplastic, Clonal evolution, Neoplastic stem cells, lcsh:R, Disease Progression, Humans, lcsh:Medicine, Review, Pre-malignant states, lcsh:Medicine (General), Precancerous Conditions, Cancer

Abstract

Cancer evolution is a step-wise non-linear process that may start early in life or later in adulthood, and includes pre-malignant (indolent) and malignant phases. Early somatic changes may not be detectable or are found by chance in apparently healthy individuals. The same lesions may be detected in pre-malignant clonal conditions. In some patients, these lesions may never become relevant clinically whereas in others, they act together with additional pro-oncogenic hits and thereby contribute to the formation of an overt malignancy. Although some pre-malignant stages of a malignancy have been characterized, no global system to define and to classify these conditions is available. To discuss open issues related to pre-malignant phases of neoplastic disorders, a working conference was organized in Vienna in August 2015. The outcomes of this conference are summarized herein and include a basic proposal for a nomenclature and classification of pre-malignant conditions. This proposal should assist in the communication among patients, physicians and scientists, which is critical as genome-sequencing will soon be offered widely for early cancer-detection., Highlights • Premalignant neoplastic conditions are characterized by early somatic events without evidence of an overt neoplasm. • Overt neoplasms can be divided into premalignant (indolent) neoplasms and malignant (aggressive) neoplasms. • An updated nomenclature and classification of clonal conditions seems of utmost importance in the genome era of medicine.

Published

2017

12. Proposed diagnostic algorithm for patients with suspected mast cell activation syndrome

Author

Austrian Science Fund, National Institute of Allergy and Infectious Diseases (US), Valent, Peter, Akin, Cem, Bonadonna, Patrizia, Hartmann, Karin, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Siebenhaar, Frank, Sperr, Wolfgang R., Oude Elberink, Joanna N. G., Butterfield, Joseph H., Álvarez-Twose, Iván, Sotlar, Karl, Reiter, Andreas, Kluin-Nelemans, Hanneke C., Hermine, Olivier, Gotlib, Jason, Broesby-Olsen, Sigurd, Orfao, Alberto, Horny, Hans-Peter, Triggiani, Massimo, Arock, Michel, Schwartz, Lawrence B., Metcalfe, Dean D., Austrian Science Fund, National Institute of Allergy and Infectious Diseases (US), Valent, Peter, Akin, Cem, Bonadonna, Patrizia, Hartmann, Karin, Brockow, Knut, Niedoszytko, Marek, Nedoszytko, Boguslaw, Siebenhaar, Frank, Sperr, Wolfgang R., Oude Elberink, Joanna N. G., Butterfield, Joseph H., Álvarez-Twose, Iván, Sotlar, Karl, Reiter, Andreas, Kluin-Nelemans, Hanneke C., Hermine, Olivier, Gotlib, Jason, Broesby-Olsen, Sigurd, Orfao, Alberto, Horny, Hans-Peter, Triggiani, Massimo, Arock, Michel, Schwartz, Lawrence B., and Metcalfe, Dean D.

Abstract

Mast cell activation (MCA) accompanies diverse physiologic and pathologic processes and is one of the more frequently encountered conditions in medicine. MCA-related symptoms are usually mild and often transient. In such cases, histamine receptor blockers and other mediator-targeting drugs can usually control MCA. In severe cases, an MCA syndrome (MCAS) may be diagnosed. However, overt MCAS is an unusual condition, and many patients referred because of suspected MCAS are diagnosed with other diseases (autoimmune, neoplastic, or infectious) unrelated to MCA or suffer from MCA-related (eg, allergic) disorders and/or comorbidities without fulfilling criteria of an overt MCAS. These considerations are important as more and more patients are informed that they may have MCA or even MCAS without completing a thorough medical evaluation. In fact, in several instances, symptoms are misinterpreted as MCA/MCAS, and other clinically relevant conditions are not thoroughly pursued. The number of such referrals is increasing. To avoid such unnecessary referrals and to prevent misdiagnoses, we here propose a diagnostic algorithm through which a clinically relevant (systemic) MCA can be suspected and MCAS can subsequently be documented or excluded. In addition, the algorithm proposed should help guide the investigating care providers to consider the 2 principal diagnoses that may underlie MCAS, namely, severe allergy and systemic mastocytosis accompanied by severe MCA. Although validation is required, we anticipate that this algorithm will facilitate the management of patients with suspected MCAS.

Published

2019

13. International prognostic scoring system for mastocytosis (IPSM): a retrospective cohort study

Author

Austrian Science Fund, German Research Foundation, University of Cologne, Charles and Ann Johnson Foundation, Research Foundation - Flanders, University of Leuven, Instituto de Salud Carlos III, European Commission, Sperr, Wolfgang R., Kundi, Michael, Anrooij, Bjorn van, Oude Elberink, Joanna N. G., Gorska, Aleksandra, Niedoszytko, Marek, Gleixner, Karoline V., Hadzijusufovic, Emir, Zanotti, Roberta, Bonadonna, Patrizia, Bonifacio, Massimiliano, Perkins, Cecelia, Illerhaus, Anja, Elena, Chiara, Merante, Serena, Shoumariyeh, Khalid, Bubnoff, Nikolas von, Parente, Roberta, Jawhar, Mohamad, Belloni Fortina, Anna, Caroppo, Francesca, Brockow, Knut, Zink, Alexander, Fuchs, David, Kilbertus, Alex J., Selim Yavuz, Akif, Doubek, Michael, Hägglund, Hans, Panse, Jens, Sabato, Vito, Bretterklieber, Agnes, Niederwieser, Dietger, Breynaert, Christine, Hartmann, Karin, Triggiani, Massimo, Nedoszytko, Boguslaw, Reiter, Andreas, Orfao, Alberto, Hermine, Olivier, Gotlib, Jason, Arock, Michel, Kluin-Nelemans, Hanneke C., Valent, Peter, Austrian Science Fund, German Research Foundation, University of Cologne, Charles and Ann Johnson Foundation, Research Foundation - Flanders, University of Leuven, Instituto de Salud Carlos III, European Commission, Sperr, Wolfgang R., Kundi, Michael, Anrooij, Bjorn van, Oude Elberink, Joanna N. G., Gorska, Aleksandra, Niedoszytko, Marek, Gleixner, Karoline V., Hadzijusufovic, Emir, Zanotti, Roberta, Bonadonna, Patrizia, Bonifacio, Massimiliano, Perkins, Cecelia, Illerhaus, Anja, Elena, Chiara, Merante, Serena, Shoumariyeh, Khalid, Bubnoff, Nikolas von, Parente, Roberta, Jawhar, Mohamad, Belloni Fortina, Anna, Caroppo, Francesca, Brockow, Knut, Zink, Alexander, Fuchs, David, Kilbertus, Alex J., Selim Yavuz, Akif, Doubek, Michael, Hägglund, Hans, Panse, Jens, Sabato, Vito, Bretterklieber, Agnes, Niederwieser, Dietger, Breynaert, Christine, Hartmann, Karin, Triggiani, Massimo, Nedoszytko, Boguslaw, Reiter, Andreas, Orfao, Alberto, Hermine, Olivier, Gotlib, Jason, Arock, Michel, Kluin-Nelemans, Hanneke C., and Valent, Peter

Abstract

[Background]: The WHO classification separates mastocytosis into distinct variants, but prognostication remains a clinical challenge. The aim of this study was to improve prognostication for patients with mastocytosis., [Methods]: We analysed data of the registry of the European Competence Network on Mastocytosis including 1639 patients (age 17–90 years) diagnosed with mastocytosis according to WHO criteria between Jan 12, 1978, and March 16, 2017. Univariate and multivariate analyses with Cox regression were applied to identify prognostic variables predicting survival outcomes and to establish a prognostic score. We validated this International Prognostic Scoring System in Mastocytosis (IPSM) with data of 462 patients (age 17–79 years) from the Spanish network Red Española de Mastocitosis diagnosed between Jan 22, 1998, and Nov 2, 2017., [Findings]: The prognostic value of the WHO classification was confirmed in our study (p<0·0001). For patients with non-advanced mastocytosis (n=1380), we identified age 60 years or older (HR 10·75, 95% CI 5·68–20·32) and a concentration of alkaline phosphatase 100 U/L or higher (2·91, 1·60–5·30) as additional independent prognostic variables for overall survival. The resulting scoring system divided patients with non-advanced mastocytosis into three groups: low (no risk factors), intermediate 1 (one risk factor), and intermediate 2 (two risk factors). Overall survival and progression-free survival differed significantly among these groups (p<0·0001). In patients with advanced mastocytosis (n=259), age 60 years or older (HR 2·14, 95% CI 1·42–3·22), a concentration of tryptase 125 ng/mL or higher (1·81, 1·20–2·75), a leukocyte count of 16 × 109 per L or higher (1·88, 1·27–2·79), haemoglobin of 11 g/dL or lower (1·71, 1·13–2·57), a platelet count of 100 × 109 per L or lower (1·63, 1·13–2·34), and skin involvement (0·46, 0·30–0·69) were prognostic variables. Based on these variables, a separate score for advanced mastocytosis with four risk categories was established, with significantly different outcomes for overall survival and progression-free survival (p<0·0001). The prognostic value of both scores was confirmed in 413 patients with non-advanced disease and 49 with advanced mastocytosis from the validation cohort., [Interpretation]: The IPSM scores for patients with non-advanced and advanced mastocytosis can be used to predict survival outcomes and guide treatment decisions. However, the predictive value of the IPSM needs to be confirmed in forthcoming trials.

Published

2019

14. Cutaneous manifestations in patients with mastocytosis: Consensus report of the European Competence Network on Mastocytosis; The American Academy of Allergy, Asthma & Immunology; And the European Academy of Allergology and Clinical Immunology

Author

Austrian Science Fund, European Academy of Allergy and Clinical Immunology, German Research Foundation, National Institute of Allergy and Infectious Diseases (US), Hartmann, Karin, Escribano, Luis, Grattan, Clive, Brockow, Knut, Carter, Melody C., Álvarez-Twose, Iván, Matito, Almudena, Broesby-Olsen, Sigurd, Siebenhaar, Frank, Lange, Magdalena, Niedoszytko, Marek, Castells, Mariana, Oude Elberink, Joanna N. G., Bonadonna, Patrizia, Zanotti, Roberta, Hornick, Jason L., Torrelo, Antonio, Grabbe, Jürgen, Rabenhorst, Anja, Nedoszytko, Boguslaw, Butterfield, Joseph H., Gotlib, Jason, Reiter, Andreas, Radia, Deepti, Hermine, Olivier, Sotlar, Karl, George, Tracy I., Kristensen, Thomas K., Kluin-Nelemans, Hanneke C., Yavuz, Selim, Hägglund, Hans, Sperr, Wolfgang R., Schwartz, Lawrence B., Triggiani, Massimo, Maurer, Marcus, Nilsson, Gunnar, Horny, Hans-Peter, Arock, Michel, Orfao, Alberto, Metcalfe, Dean D., Akin, Cem, Valent, Peter, Austrian Science Fund, European Academy of Allergy and Clinical Immunology, German Research Foundation, National Institute of Allergy and Infectious Diseases (US), Hartmann, Karin, Escribano, Luis, Grattan, Clive, Brockow, Knut, Carter, Melody C., Álvarez-Twose, Iván, Matito, Almudena, Broesby-Olsen, Sigurd, Siebenhaar, Frank, Lange, Magdalena, Niedoszytko, Marek, Castells, Mariana, Oude Elberink, Joanna N. G., Bonadonna, Patrizia, Zanotti, Roberta, Hornick, Jason L., Torrelo, Antonio, Grabbe, Jürgen, Rabenhorst, Anja, Nedoszytko, Boguslaw, Butterfield, Joseph H., Gotlib, Jason, Reiter, Andreas, Radia, Deepti, Hermine, Olivier, Sotlar, Karl, George, Tracy I., Kristensen, Thomas K., Kluin-Nelemans, Hanneke C., Yavuz, Selim, Hägglund, Hans, Sperr, Wolfgang R., Schwartz, Lawrence B., Triggiani, Massimo, Maurer, Marcus, Nilsson, Gunnar, Horny, Hans-Peter, Arock, Michel, Orfao, Alberto, Metcalfe, Dean D., Akin, Cem, and Valent, Peter

Abstract

Cutaneous lesions in patients with mastocytosis are highly heterogeneous and encompass localized and disseminated forms. Although a classification and criteria for cutaneous mastocytosis (CM) have been proposed, there remains a need to better define subforms of cutaneous manifestations in patients with mastocytosis. To address this unmet need, an international task force involving experts from different organizations (including the European Competence Network on Mastocytosis; the American Academy of Allergy, Asthma & Immunology; and the European Academy of Allergology and Clinical Immunology) met several times between 2010 and 2014 to discuss the classification and criteria for diagnosis of cutaneous manifestations in patients with mastocytosis. This article provides the major outcomes of these meetings and a proposal for a revised definition and criteria. In particular, we recommend that the typical maculopapular cutaneous lesions (urticaria pigmentosa) should be subdivided into 2 variants, namely a monomorphic variant with small maculopapular lesions, which is typically seen in adult patients, and a polymorphic variant with larger lesions of variable size and shape, which is typically seen in pediatric patients. Clinical observations suggest that the monomorphic variant, if it develops in children, often persists into adulthood, whereas the polymorphic variant may resolve around puberty. This delineation might have important prognostic implications, and its implementation in diagnostic algorithms and future mastocytosis classifications is recommended. Refinements are also suggested for the diagnostic criteria of CM, removal of telangiectasia macularis eruptiva perstans from the current classification of CM, and removal of the adjunct solitary from the term solitary mastocytoma.

Published

2016

15. Diagnosis of mastocytosis: emerging iceberg?

Author

Rossignol J and Arock M

Subjects

Humans, Mast Cells pathology, Mast Cells metabolism, Mastocytosis diagnosis, Mastocytosis pathology

Published

2024

16. Tumor necrosis factor α promotes clonal dominance of KIT D816V+ cells in mastocytosis: role of survivin and impact on prognosis.

Author

Greiner G, Witzeneder N, Klein K, Tangermann S, Kodajova P, Jaeger E, Ratzinger F, Gerner MC, Jawhar M, Baumgartner S, Fruehwirth K, Schmetterer KG, Zuber J, Gleixner KV, Mayerhofer M, Schwarzinger I, Simonitsch-Klupp I, Esterbauer H, Baer C, Walter W, Meggendorfer M, Strassl R, Haferlach T, Hartmann K, Kenner L, Sperr WR, Reiter A, Sexl V, Arock M, Valent P, and Hoermann G

Subjects

Humans, Animals, Mice, Tumor Necrosis Factor-alpha, Survivin genetics, Prognosis, Cytokines, Mastocytosis, Mastocytosis, Systemic diagnosis, Mastocytosis, Systemic genetics

Abstract

Abstract: Systemic mastocytosis (SM) is defined by the expansion and accumulation of neoplastic mast cells (MCs) in the bone marrow (BM) and extracutaneous organs. Most patients harbor a somatic KIT D816V mutation, which leads to growth factor-independent KIT activation and accumulation of MC. Tumor necrosis factor α (TNF) is a proapoptotic and inflammatory cytokine that has been implicated in the clonal selection of neoplastic cells. We found that KIT D816V increases the expression and secretion of TNF. TNF expression in neoplastic MCs is reduced by KIT-targeting drugs. Similarly, knockdown of KIT or targeting the downstream signaling cascade of MAPK and NF-κB signaling reduced TNF expression levels. TNF reduces colony formation in human BM cells, whereas KIT D816V+ cells are less susceptible to the cytokine, potentially contributing to clonal selection. In line, knockout of TNF in neoplastic MC prolonged survival and reduced myelosuppression in a murine xenotransplantation model. Mechanistic studies revealed that the relative resistance of KIT D816V+ cells to TNF is mediated by the apoptosis-regulator BIRC5 (survivin). Expression of BIRC5 in neoplastic MC was confirmed by immunohistochemistry of samples from patients with SM. TNF serum levels are significantly elevated in patients with SM and high TNF levels were identified as a biomarker associated with inferior survival. We here characterized TNF as a KIT D816V-dependent cytokine that promotes clonal dominance. We propose TNF and apoptosis-associated proteins as potential therapeutic targets in SM., (© 2024 American Society of Hematology. Published by Elsevier Inc. All rights are reserved, including those for text and data mining, AI training, and similar technologies.)

Published

2024

17. Human C1q Tumor Necrosis Factor 8 (CTRP8) defines a novel tryptase+ mast cell subpopulation in the prostate cancer microenvironment.

Author

Krishnan SN, Thanasupawat T, Arreza L, Wong GW, Sfanos K, Trock B, Arock M, Shah GG, Glogowska A, Ghavami S, Hombach-Klonisch S, and Klonisch T

Subjects

Humans, Male, Ligands, Mast Cells, Prostate, Tryptases, Tumor Microenvironment, Tumor Necrosis Factors, Complement C1q, Prostatic Neoplasms genetics

Abstract

The adipokine C1q Tumor Necrosis Factor 8 (CTRP8) is the least known member of the 15 CTRP proteins and a ligand of the relaxin receptor RXFP1. We previously demonstrated the ability of the CTRP8-RXFP1 interaction to promote motility, matrix invasion, and drug resistance. The lack of specific tools to detect CTRP8 protein severely limits our knowledge on CTRP8 biological functions in normal and tumor tissues. Here, we have generated and characterized the first specific antiserum to human CTRP8 which identified CTRP8 as a novel marker of tryptase+ mast cells (MC T ) in normal human tissues and in the prostate cancer (PC) microenvironment. Using human PC tissue microarrays composed of neoplastic and corresponding tumor-adjacent prostate tissues, we have identified a significantly higher number of CTRP8+ MC T in the peritumor versus intratumor compartment of PC tissues of Gleason scores 6 and 7. Higher numbers of CTRP8+ MC T correlated with the clinical parameter of biochemical recurrence. We showed that the human MC line ROSA KIT WT expressed RXFP1 transcripts and responded to CTRP8 treatment with a small but significant increase in cell proliferation. Like the cognate RXFP1 ligand RLN-2 and the small molecule RXFP1 agonist ML-290, CTRP8 reduced degranulation of ROSA KIT WT MC stimulated by the Ca 2+ -ionophore A14187. In conclusion, this is the first report to identify the RXFP1 agonist CTRP8 as a novel marker of MC T and autocrine/paracrine oncogenic factor within the PC microenvironment., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

18. Activation of Siglec-7 results in inhibition of in vitro and in vivo growth of human mast cell leukemia cells.

Author

Landolina N, Zaffran I, Smiljkovic D, Serrano-Candelas E, Schmiedel D, Friedman S, Arock M, Hartmann K, Pikarsky E, Mandelboim O, Martin M, Valent P, and Levi-Schaffer F

Subjects

Adult, Aged, Aged, 80 and over, Animals, Antibodies, Monoclonal therapeutic use, Antigens, Differentiation, Myelomonocytic, Cell Line, Tumor, Cell Survival drug effects, Female, Genes, src drug effects, Humans, Leukemia, Mast-Cell pathology, Lymphoma, B-Cell drug therapy, Lymphoma, B-Cell pathology, Male, Mastocytosis drug therapy, Mice, Mice, SCID, Middle Aged, Phosphorylation, Protein Tyrosine Phosphatase, Non-Receptor Type 6 drug effects, Proto-Oncogene Proteins c-kit drug effects, Xenograft Model Antitumor Assays, Lectins agonists, Leukemia, Mast-Cell drug therapy

Abstract

Advanced systemic mastocytosis is a rare and still untreatable disease. Blocking antibodies against inhibitory receptors, also known as "immune checkpoints", have revolutionized anti-cancer treatment. Inhibitory receptors are expressed not only on normal immune cells, including mast cells but also on neoplastic cells. Whether activation of inhibitory receptors through monoclonal antibodies can lead to tumor growth inhibition remains mostly unknown. Here we show that the inhibitory receptor Siglec-7 is expressed by primary neoplastic mast cells in patients with systemic mastocytosis and by mast cell leukemia cell lines. Activation of Siglec-7 by anti-Siglec-7 monoclonal antibody caused phosphorylation of Src homology region 2 domain-containing phosphatase-1 (SHP-1), reduced phosphorylation of KIT and induced growth inhibition in mast cell lines. In SCID-beige mice injected with either the human mast cell line HMC-1.1 and HMC-1.2 or with Siglec-7 transduced B cell lymphoma cells, anti-Siglec-7 monoclonal antibody reduced tumor growth by a mechanism involving Siglec-7 cytoplasmic domains in "preventive" and "treatment" settings. These data demonstrate that activation of Siglec-7 on mast cell lines can inhibit their growth in vitro and in vivo. This might pave the way to additional treatment strategies for mastocytosis., (Copyright © 2020. Published by Elsevier Ltd.)

Published

2020

19. CD44 is a RAS/STAT5-regulated invasion receptor that triggers disease expansion in advanced mastocytosis.

Author

Mueller N, Wicklein D, Eisenwort G, Jawhar M, Berger D, Stefanzl G, Greiner G, Boehm A, Kornauth C, Muellauer L, Sehner S, Hoermann G, Sperr WR, Staber PB, Jaeger U, Zuber J, Arock M, Schumacher U, Reiter A, and Valent P

Subjects

Adult, Aged, Animals, Disease Progression, Female, Humans, Hyaluronan Receptors analysis, Male, Mast Cells metabolism, Mast Cells pathology, Mastocytosis, Systemic metabolism, Mastocytosis, Systemic pathology, Mice, Inbred BALB C, Mice, SCID, Middle Aged, Neoplasm Invasiveness pathology, Neoplasm Metastasis genetics, Neoplasm Metastasis pathology, Gene Expression Regulation, Neoplastic, Hyaluronan Receptors genetics, Mastocytosis, Systemic genetics, Neoplasm Invasiveness genetics, STAT5 Transcription Factor metabolism, Signal Transduction, ras Proteins metabolism

Abstract

The Hermes receptor CD44 is a multifunctional adhesion molecule that plays an essential role in the homing and invasion of neoplastic stem cells in various myeloid malignancies. Although mast cells (MCs) reportedly express CD44, little is known about the regulation and function of this receptor in neoplastic cells in systemic mastocytosis (SM). We found that clonal CD34 + /CD38 - stem cells, CD34 + /CD38 + progenitor cells, and CD117 ++ /CD34 - MCs invariably express CD44 in patients with indolent SM (ISM), SM with an associated hematologic neoplasm, aggressive SM, and MC leukemia (MCL). In addition, all human MCL-like cell lines examined (HMC-1, ROSA, and MCPV-1) displayed cytoplasmic and cell-surface CD44. We also found that expression of CD44 in neoplastic MCs depends on RAS-MEK and STAT5 signaling and increases with the aggressiveness of SM. Correspondingly, higher levels of soluble CD44 were measured in the sera of patients with advanced SM compared with ISM or cutaneous mastocytosis and were found to correlate with overall and progression-free survival. To investigate the functional role of CD44, a xenotransplantation model was employed using severe combined immunodeficient (SCID) mice, HMC-1.2 cells, and a short hairpin RNA (shRNA) against CD44. In this model, the shRNA-mediated knockdown of CD44 resulted in reduced MC expansion and tumor formation and prolonged survival in SCID mice compared with HMC-1.2 cells transduced with control shRNA. Together, our data show that CD44 is a RAS-MEK/STAT5-driven MC invasion receptor that correlates with the aggressiveness of SM. Whether CD44 can serve as therapeutic target in advanced SM remains to be determined in forthcoming studies., (© 2018 by The American Society of Hematology.)

Published

2018

20. A new therapeutic advance for symptomatic systemic mastocytosis?

Author

Arock M

Subjects

Humans, Mastocytosis, Mastocytosis, Systemic

Published

2017

21. Mast cell differentiation: still open questions?

Author

Arock M

Subjects

Female, Humans, Male, Antigens, CD34 analysis, Mast Cells cytology, Proto-Oncogene Proteins c-kit analysis, Receptors, IgE analysis, Stem Cells cytology

Abstract

In this issue of Blood, Dahlin et al report on a minor circulating human mast cell (MC) progenitor cell population (lineage-negative [Lin−]/CD34hi/CD117int/hi/high-affinity immunoglobulin E receptor-positive [FcεRI+]), with an immature MC-like appearance, which is present in the peripheral blood (PB) of healthy individuals and of asthma subjects well controlled by treatment or with reduced lung function.

Published

2016

22. A new human mast cell line expressing a functional IgE receptor converts to tumorigenic growth by KIT D816V transfection.

Author

Saleh R, Wedeh G, Herrmann H, Bibi S, Cerny-Reiterer S, Sadovnik I, Blatt K, Hadzijusufovic E, Jeanningros S, Blanc C, Legarff-Tavernier M, Chapiro E, Nguyen-Khac F, Subra F, Bonnemye P, Dubreuil P, Desplat V, Merle-Béral H, Willmann M, Rülicke T, Valent P, and Arock M

Subjects

Animals, Blotting, Western, Cell Separation, Flow Cytometry, Heterografts, Humans, Immunoglobulin E immunology, Immunoglobulin E metabolism, Mast Cells immunology, Mast Cells metabolism, Mice, Mice, Inbred NOD, Mice, Knockout, Mice, SCID, Transfection, Cell Line cytology, Cell Line immunology, Cell Line metabolism, Mast Cells pathology, Mastocytosis, Systemic genetics, Proto-Oncogene Proteins c-kit genetics

Abstract

In systemic mastocytosis (SM), clinical problems arise from factor-independent proliferation of mast cells (MCs) and the increased release of mediators by MCs, but no human cell line model for studying MC activation in the context of SM is available. We have created a stable stem cell factor (SCF) -dependent human MC line, ROSA(KIT WT), expressing a fully functional immunoglobulin E (IgE) receptor. Transfection with KIT D816V converted ROSA(KIT WT) cells into an SCF-independent clone, ROSA(KIT D816V), which produced a mastocytosis-like disease in NSG mice. Although several signaling pathways were activated, ROSA(KIT D816V) did not exhibit an increased, but did exhibit a decreased responsiveness to IgE-dependent stimuli. Moreover, NSG mice bearing ROSA(KIT D816V)-derived tumors did not show mediator-related symptoms, and KIT D816V-positive MCs obtained from patients with SM did not show increased IgE-dependent histamine release or CD63 upregulation. Our data show that KIT D816V is a disease-propagating oncoprotein, but it does not activate MCs to release proinflammatory mediators, which may explain why mediator-related symptoms in SM occur preferentially in the context of a coexisting allergy. ROSA(KIT D816V) may provide a valuable tool for studying the pathogenesis of mastocytosis and should facilitate the development of novel drugs for treating SM patients., (© 2014 by The American Society of Hematology.)

Published

2014

23. International Working Group-Myeloproliferative Neoplasms Research and Treatment (IWG-MRT) & European Competence Network on Mastocytosis (ECNM) consensus response criteria in advanced systemic mastocytosis.

Author

Gotlib J, Pardanani A, Akin C, Reiter A, George T, Hermine O, Kluin-Nelemans H, Hartmann K, Sperr WR, Brockow K, Schwartz LB, Orfao A, Deangelo DJ, Arock M, Sotlar K, Horny HP, Metcalfe DD, Escribano L, Verstovsek S, Tefferi A, and Valent P

Subjects

Clinical Trials as Topic, Disease Progression, Europe, Hematologic Diseases diagnosis, Hematologic Diseases etiology, Hematologic Diseases therapy, Humans, International Cooperation, Mastocytosis complications, Mastocytosis diagnosis, Mastocytosis, Systemic complications, Mastocytosis, Systemic diagnosis, Organ Dysfunction Scores, Societies, Medical legislation & jurisprudence, Societies, Medical organization & administration, Clinical Competence legislation & jurisprudence, Clinical Competence standards, Community Networks legislation & jurisprudence, Community Networks organization & administration, Consensus, Mastocytosis therapy, Mastocytosis, Systemic therapy

Abstract

Systemic mastocytosis (SM) is characterized by accumulation of neoplastic mast cells and is classified into indolent and aggressive forms. The latter include aggressive SM (ASM), mast cell leukemia (MCL), and SM associated with a myeloid neoplasm wherein 1 or both disease compartments exhibit advanced features. These variants, henceforth collectively referred to as advanced SM for the purposes of this report, are typically characterized by organ damage and shortened survival duration. In contrast to indolent SM, in which symptoms are usually managed by noncytotoxic antimediator therapy, cytoreduction is usually necessary for disease control in advanced SM. Unfortunately, current drug treatment of these patients rarely results in complete clinical and histopathologic remissions or improved survival time. Previously defined response criteria were adapted to the heterogeneous presentations of advanced SM and the limited effects of available drugs. However, recent advances in understanding the molecular pathogenesis of SM and the corresponding prospect in targeted therapy make it a priority to modify these criteria. Our current study is the product of an international group of experts and summarizes the challenges in accomplishing this task and forwards a new proposal for response criteria, which builds on prior proposals and should facilitate response evaluation in clinical trials.

Published

2013

24. Relocalization of KIT D816V to cell surface after dasatinib treatment: potential clinical implications.

Author

Bougherara H, Georgin-Lavialle S, Damaj G, Launay JM, Lhermitte L, Auclair C, Arock M, Dubreuil P, Hermine O, and Poul MA

Subjects

Adult, Aged, Aged, 80 and over, Cell Line, Tumor, Dasatinib, Female, Humans, Male, Mastocytosis, Systemic blood, Mastocytosis, Systemic enzymology, Mastocytosis, Systemic genetics, Middle Aged, Mutation, Proto-Oncogene Proteins c-kit genetics, Proto-Oncogene Proteins c-kit metabolism, Young Adult, Cell Membrane metabolism, Mastocytosis, Systemic drug therapy, Protein Kinase Inhibitors therapeutic use, Proto-Oncogene Proteins c-kit antagonists & inhibitors, Pyrimidines therapeutic use, Thiazoles therapeutic use

Abstract

Background: Systemic mastocytosis (SM) is a heterogeneous disease that displays variable aggressivity. Adults with SM frequently have a D816V mutation in the tyrosine kinase (TK) receptor gene KIT. We previously reported that, in a Chinese hamster ovarian cell model expressing exogenous KIT variants, constitutive activating KIT mutations induced intracellular mislocalization of KIT reversed by inhibition of KIT TK activity. Hence, we hypothesized that inhibition of KIT kinase activity by the TK inhibitor dasatinib could be useful to increase KIT detection sensitivity in samples from patients with SM., Patients and Methods: We tested this hypothesis on a BaF/3 cell line modified to express either KIT wild-type (WT) or KIT D816V, on the human mastocytoma cell line HMC1.2, and among 28 patients with proven SM who did (n = 24) or did not (n = 4) carry the D816V KIT mutation and displayed various SM subtypes by using a simple flow cytometry assay to quantify KIT relocalization upon dasatinib treatment., Results: We confirm KIT cell surface increase upon dasatinib treatment on BaF/3 KIT D816V and HMC1.2 cell lines but not on BaF/3 KIT WT cell line. The analysis of bone marrow and peripheral blood samples of patients with SM showed KIT surface level increase for patients with the KIT D816V mutation but not for patients who had no KIT mutation. Interestingly, the extent of KIT level relocalization correlates with SM severity, with a higher relocalization for patients with aggressive forms compared with indolent forms., Conclusions: Overall, results of this study suggests that treating the peripheral blood sample with dasatinib of a patient with SM before analysis by flow cytometry could contribute to narrowing the SM diagnosis., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

25. The classification of systemic mastocytosis should include mast cell leukemia (MCL) and systemic mastocytosis with a clonal hematologic non-mast cell lineage disease (SM-AHNMD).

Author

Valent P, Arock M, Akin C, Sperr WR, Reiter A, Sotlar K, Hartmann K, George TI, Brockow K, Kluin-Nelemans HC, Gotlib J, Metcalfe DD, and Horny HP

Subjects

Cell Lineage, Clone Cells pathology, Consensus, European Union, Hematologic Diseases classification, Humans, Leukemia, Mast-Cell genetics, Leukemia, Mast-Cell pathology, Leukemia, Myeloid, Acute classification, Leukemia, Myelomonocytic, Chronic classification, Mastocytosis, Systemic genetics, Mastocytosis, Systemic pathology, Proto-Oncogene Proteins c-kit genetics, Societies, Medical, Terminology as Topic, United States, World Health Organization, Leukemia, Mast-Cell classification, Mastocytosis, Systemic classification

Published

2010

26. Pediatric mastocytosis is a clonal disease associated with D816V and other activating c-KIT mutations.

Author

Bodemer C, Hermine O, Palmérini F, Yang Y, Grandpeix-Guyodo C, Leventhal PS, Hadj-Rabia S, Nasca L, Georgin-Lavialle S, Cohen-Akenine A, Launay JM, Barete S, Feger F, Arock M, Catteau B, Sans B, Stalder JF, Skowron F, Thomas L, Lorette G, Plantin P, Bordigoni P, Lortholary O, de Prost Y, Moussy A, Sobol H, and Dubreuil P

Subjects

Adolescent, Age of Onset, Animals, Biopsy, COS Cells, Child, Child, Preschool, Chlorocebus aethiops, Clone Cells, Exons genetics, Female, Genomics, Genotype, Humans, Infant, Infant, Newborn, Male, Mast Cells physiology, Phenotype, Mast Cells pathology, Mastocytosis, Cutaneous genetics, Mastocytosis, Cutaneous pathology, Point Mutation, Proto-Oncogene Proteins c-kit genetics

Abstract

Adult mastocytosis is an incurable clonal disease associated with c-KIT mutations, mostly in exon 17 (D816V). In contrast, pediatric mastocytosis often spontaneously regresses and is considered a reactive disease. Previous studies on childhood mastocytosis assessed only a few patients and focused primarily on codon 816 mutations, with various results. In this study, we analyzed the entire c-KIT sequence from cutaneous biopsies of 50 children with mastocytosis (ages 0-16 years). A mutation of codon 816 (exon 17) was found in 42% of cases, and mutations outside exon 17 were observed in 44%. Unexpectedly, half of the mutations were located in the fifth Ig loop of c-KIT's extracellular domain, which is encoded by exons 8 and 9. All mutations identified in this study were somatic and caused a constitutive activation of c-KIT. There was no clear phenotype-genotype correlation, no clear relationship between the mutations and familial versus spontaneous disease, and no significant change in the relative expression of the c-KIT GNNK+ and GNNK isoforms. These findings strongly support the idea that, although pediatric mastocytosis can spontaneously regress, it is a clonal disease most commonly associated with activating mutations in c-KIT.

Published

2010

27. Rapamycin inhibits growth and survival of D816V-mutated c-kit mast cells.

Author

Gabillot-Carré M, Lepelletier Y, Humbert M, de Sepuvelda P, Hamouda NB, Zappulla JP, Liblau R, Ribadeau-Dumas A, Machavoine F, Letard S, Baude C, Hermant A, Yang Y, Vargaftig J, Bodemer C, Morelon E, Lortholary O, Recher C, Laurent G, Dy M, Arock M, Dubreuil P, and Hermine O

Subjects

Animals, Apoptosis drug effects, Cell Proliferation drug effects, Cell Survival drug effects, Humans, Mast Cells drug effects, Mast Cells pathology, Mastocytosis, Systemic pathology, Mice, Mice, Transgenic, Protein Kinases metabolism, Signal Transduction, TOR Serine-Threonine Kinases, Tumor Cells, Cultured, Mastocytosis, Systemic drug therapy, Mastocytosis, Systemic genetics, Mutation, Missense, Pharmacogenetics, Proto-Oncogene Proteins c-kit genetics, Sirolimus pharmacology

Abstract

Two classes of oncogenic mutations of the c-kit tyrosine kinase have been described: the juxtamembrane domain V560G mutation, which is preferentially found in gastrointestinal stromal tumors (GISTs), and the kinase domain D816V mutation, which is highly representative of systemic mastocytosis (SM). Here we show that both mutations constitutively activate the mammalian target of rapamycin (mTOR) signaling pathway. Surprisingly, the mTOR inhibitor rapamycin induces only apoptosis in HMC-1 cells bearing the D816V but not the V560G mutation. In support of this unexpected selectivity, rapamycin inhibits the phosphorylation of 4E-BP1, a downstream substrate of the mTOR pathway, but only in D816V HMC-1 cells. Importantly, D816V mast cells isolated from SM patients or from transgenic mice are sensitive to rapamycin whereas normal human or mouse mast cells are not. Thus, rapamycin inhibition appears specific to the D816V mutation. At present there is no effective cure for SM patients with the D816V mutation. The data presented here provide a rationale to test whether rapamycin could be a possible treatment for SM and other hematologic malignancies with the D816V mutation.

Published

2006

28. Establishment and characterization of continuous hematopoietic progenitors-derived pig normal mast cell lines.

Author

Femenia F, Arock M, Leriche L, Delouis C, Millet G, Ben Hamouda N, Cote M, Alliot A, Lilin T, Pinton A, Iannucceli N, Parodi AL, and Boireau P

Subjects

Animals, Cell Culture Techniques methods, Cell Line, Genotype, Histamine metabolism, Karyotyping, Microsatellite Repeats genetics, Microscopy, Electron, Transmission, Proto-Oncogene Proteins c-kit metabolism, Receptors, IgE metabolism, Cell Lineage physiology, Hematopoietic Stem Cells cytology, Mast Cells metabolism, Mast Cells ultrastructure, Sus scrofa

Abstract

Mast cells (MCs) are tissue resident, hematopoietic stem cells-derived elements, distributed throughout the body. They are the pivotal mediating cells of allergic reactions. In addition, in mice, MCs play a critical role in the defense against several pathogens, such as bacteria, parasites and viruses. Whereas the biology of rodent and human MCs has been extensively studied using in vitro derived populations, the role of MCs in pigs has not yet been evaluated, given the very low availability of pure porcine MCs populations. In the present report, we describe an original method to obtain continuous factor-dependent normal pig MCs (PMC) lines from fetal hematopoietic progenitors. These Stem Cell Factor (SCF) and Interleukin-3- (IL-3)-dependent PMC lines retain their capacity to growth after conventional freezing methods and exhibit most of the morphological and biochemical properties of normal, although immature, MCs, including metachromatic granules containing sulfated polysaccharides, the expression of c-kit and high-affinity IgE receptors (FcepsilonRI), and the ability to store histamine that is released upon cross-linking of FcepsilonRI. In vitro derived PMC lines might thus be valuable tools to further investigate the reactivity of these elements towards several parasites frequently encountered in pig, such as, but not limited to, Ascaris suum, Trichinella spiralis or Trichuris suis, or towards antigens derived from these pathogens.

Published

2005

29. Expression of the myeloid-associated marker CD33 is not an exclusive factor for leukemic plasmacytoid dendritic cells.

Author

Garnache-Ottou F, Chaperot L, Biichle S, Ferrand C, Remy-Martin JP, Deconinck E, de Tailly PD, Bulabois B, Poulet J, Kuhlein E, Jacob MC, Salaun V, Arock M, Drenou B, Schillinger F, Seilles E, Tiberghien P, Bensa JC, Plumas J, and Saas P

Subjects

Acute Disease, Aged, Biomarkers, Tumor immunology, CD3 Complex blood, CD4 Antigens blood, CD55 Antigens blood, Flow Cytometry, Humans, Immunophenotyping, Leukemia, Plasma Cell immunology, Male, Sialic Acid Binding Ig-like Lectin 3, Antigens, CD blood, Antigens, Differentiation, Myelomonocytic blood, Dendritic Cells immunology, Plasma Cells immunology

Abstract

A new entity of acute leukemia coexpressing CD4(+)CD56(+) markers without any other lineage-specific markers has been identified recently as arising from lymphoid-related plasmacytoid dendritic cells (pDCs). In our laboratory, cells from a patient with such CD4(+)CD56(+) lineage-negative leukemia were unexpectedly found to also express the myeloid marker CD33. To confirm the diagnosis of pDC leukemia despite the CD33 expression, we demonstrated that the leukemic cells indeed exhibited pDC phenotypic and functional properties. In 7 of 8 other patients with CD4(+)CD56(+) pDC malignancies, we were able to confirm that the tumor cells expressed CD33 although with variable expression levels. CD33 expression was shown by flow cytometry, reverse transcriptase-polymerase chain reaction, and immunoblot analysis. Furthermore, CD33 monoclonal antibody stimulation of purified CD4(+)CD56(+) leukemic cells led to cytokine secretion, thus confirming the presence of a functional CD33 on these leukemic cells. Moreover, we found that circulating pDCs in healthy individuals also weakly express CD33. Overall, our results demonstrate that the expression of CD33 on CD4(+)CD56(+) lineage-negative cells should not exclude the diagnosis of pDC leukemia and underline that pDC-specific markers should be used at diagnosis for CD4(+)CD56(+) malignancies.

Published

2005