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SETBP-1 mutations favor transformation to AML in PTPN-11 positive JMML
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  • Ravi Kumar Majhi,
  • Aditya Gupta,
  • Jagdish Meena,
  • Harshita Makkar,
  • Lata Singh,
  • Pranay Tanwar,
  • Anita Chopra,
  • Sameer Bakhshi,
  • Rachna Seth
Ravi Kumar Majhi
All India Institute of Medical Sciences Department of Pediatrics
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Aditya Gupta
All India Institute of Medical Sciences Department of Pediatrics

Corresponding Author:adivick@gmail.com

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Jagdish Meena
All India Institute of Medical Sciences Department of Pediatrics
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Harshita Makkar
All India Institute of Medical Sciences Department of Pediatrics
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Lata Singh
All India Institute of Medical Sciences Department of Pediatrics
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Pranay Tanwar
All India Institute of Medical Sciences
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Anita Chopra
All India Institute of Medical Sciences
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Sameer Bakhshi
All India Institute of Medical Sciences Department of Medical Oncology
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Rachna Seth
All India Institute of Medical Sciences Department of Pediatrics
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Abstract

Background: Juvenile Myelomonocytic leukemia(JMML) is a rare and aggressive malignancy found in children. The genomic landscape of the JMML shows that the most common mutated genes found in the RAS. The risk stratification and the management of JMML patients is determined by the precise evaluation of the underlying genetic mutations. The co-occurring mutations along with the RAS pathway mutations may affect the outcomes of the disease. PTPN11 is the most common mutation found in JMML. In this study, we describe the outcomes of JMML patients who had an underlying PTPN11 mutation along with a mutation in the SETBP1 gene. Methods: DNA was extracted from the 43 cases with JMML after confirmation of the diagnosis. Whole exome sequencing was performed to find out the underlying germline and somatic mutations. Results: We found that about 35%(n=14) of patients harboured a PTPN11 somatic mutation. A coexisting SETBP1 mutation was found in 5 patients out of 14 cases. In our cohort of patients, we found that the SETBP1 was exclusively associated with PTPN11 and all 5 patients transformed into AML. The median time to AML transformation was 12 months (13 days-35 months). PTPN11 mutation with co-existing SETBP1 mutation showed a worse outcome compared to other PTPN11 positive patients and all 5 patients died within 3 months of transformation. Conclusion: In with PTPN11 positive JMML a coexisting SETBP1 mutation confers a poorer prognosis. These patients have a high risk of AML transformation. These patients should be candidate for consideration of early hematopoietic stem cell transplantation (HSCT).