Abstract

Tyrosine kinase inhibitors targeting the BCR-ABL oncoprotein in chronic myeloid leukemia (CML) are remarkably effective inducing deep molecular remission in most patients. However, they are less effective to eradicate the leukemic stem cells (LSC), resulting in disease persistence. Therefore, there is great need to develop novel therapeutic strategies to specifically target the LSC. In an experimental mouse CML model system, the leukotriene pathway, and specifically, the expression ALOX5, encoding 5-lipoxygenase (5-LO), has been reported as a critical regulator of the LSC. Based on these results, the 5-LO inhibitor zileuton has been introduced in clinical trials as a therapeutic option to target the LSC although its effect on primary human CML LSC has not been studied. We have here by using multiplex single cell PCR analyzed the expression of the mediators of the leukotriene pathway in bone marrow (BM) BCR-ABL+CD34+CD38− cells at diagnosis, and found low or undetectable expression of ALOX5. In line with this, zileuton did not exert significant overall growth inhibition in the long-term culture-initiating cell (LTC-IC) and colony (CFU-C) assays of BM CD34+CD38− cells from 7 CML patients. The majority of the single leukemic BCR-ABL+CD34+CD38− cells expressed cysteinyl leukotriene receptors CYSLT1 and CYSLT2. However, montelukast, an inhibitor of CYSLT1, also failed to significantly suppress CFU-C and LTC-IC growth. These findings indicate that targeting ALOX5 or CYSLT1 signaling with leukotriene antagonists, introduced into the clinical practice primarily as prophylaxis and treatment for asthma, may not be a promising pharmacological strategy to eradicate persisting LSC in CML patients.

Highlights

  • Chronic myeloid leukemia (CML) is characterized by the expression of the BCR-ABL fusion protein, a constitutively active tyrosine kinase that promotes growth of leukemic stem and progenitor cells by multiple signaling pathways involved in cell survival, proliferation and differentiation [1]

  • (LSC) in chronic phase CML reside in a phenotypically similar stem and progenitor cell population (CD34þCD38À) as normal bone marrow (BM) stem and progenitor cells [1,2] and differentiate predominantly into an expanding population of granulocytes, thrombocytes and their precursors, whereas in the terminal phase, blast crisis, immature lymphoid or myeloid progenitors accumulate as leukemic blasts

  • We found a low frequency of ALOX5-expressing CD34þCD38À cells in the CML patient samples, and no significant overall growth suppression of BM CD34þCD38À cells from CML patients by zileuton in the long-term culture-initiating cell (LTC-IC) and colony (CFU-C) assays

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Summary

Introduction

Chronic myeloid leukemia (CML) is characterized by the expression of the BCR-ABL fusion protein, a constitutively active tyrosine kinase that promotes growth of leukemic stem and progenitor cells by multiple signaling pathways involved in cell survival, proliferation and differentiation [1]. An inhibitor of 5-LO, inhibited the development of leukemia but did not inhibit the non-leukemic stem cells in this mouse model [6]. Based on these results, zileuton was proposed to be an option to eradicate the human LSC and to offer potential to improve the treatment of CML [7]. Its expression and function in the more primitive leukemic BCR-ABLþ CD34þCD38À cells of CML patients has not been explored

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