Literature DB >> 11071651

Differentiation-independent retinoid induction of folate receptor type beta, a potential tumor target in myeloid leukemia.

H Wang1, X Zheng, F G Behm, M Ratnam.   

Abstract

Folate receptor (FR) type beta is expressed in the myelomonocytic lineage, predominantly during neutrophil maturation and in myeloid leukemias. FR-beta expression was elevated up to 20-fold by all-trans retinoic acid (ATRA) in KG-1 myeloid leukemia cells in a dose-dependent and reversible manner in the absence of terminal differentiation or cell growth inhibition. ATRA also increased FR-beta expression in vitro in myeloid leukemia cells from patient marrow. FR-beta was not up-regulated in KG-1 cells treated with phorbol ester, dexamethasone, 1,25-dihydroxy vitamin D(3), or transforming growth factor beta. ATRA did not induce FR-beta expression in receptor negative cells of diverse origin. The ATRA-induced increase in FR-beta expression in KG-1 cells occurred at the level of messenger RNA synthesis, and in 293 cells containing a stably integrated FR-beta promoter-luciferase reporter construct, ATRA induced expression of the reporter. From experiments using retinoid agonists and antagonists and from cotransfection studies using the FR-beta promoter and expression plasmids for the nuclear receptors retinoic acid receptor (RAR)alpha, RARbeta, or RARgamma, it appears that the retinoid effect on FR-beta expression could be mediated by ligand binding to RARs alpha, beta, or gamma, but not to retinoid X receptors. Furthermore, there was apparent cross-talk between RARalpha and RARgamma selective agonists or antagonists, suggesting a common downstream target for RAR isoforms in inducing FR-beta expression. Thus, blocks in the RARalpha-specific pathway of retinoid-induced differentiation may be bypassed during retinoid induction of FR-beta expression. The results suggest that to facilitate FR-targeted therapies, retinoids may be used to modulate FR-beta expression in myeloid leukemia cells refractory to retinoid differentiation therapy.

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Year:  2000        PMID: 11071651

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  24 in total

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Journal:  Annu Rev Nutr       Date:  2011-08-21       Impact factor: 11.848

3.  Targeting human clonogenic acute myelogenous leukemia cells via folate conjugated liposomes combined with receptor modulation by all-trans retinoic acid.

Authors:  Hong Li; Yanhui Lu; Longzhu Piao; Jun Wu; Shujun Liu; Guido Marcucci; Manohar Ratnam; Robert J Lee
Journal:  Int J Pharm       Date:  2010-09-29       Impact factor: 5.875

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5.  Targeting of folate receptor β on acute myeloid leukemia blasts with chimeric antigen receptor-expressing T cells.

Authors:  Rachel C Lynn; Mathilde Poussin; Anna Kalota; Yang Feng; Philip S Low; Dimiter S Dimitrov; Daniel J Powell
Journal:  Blood       Date:  2015-04-17       Impact factor: 22.113

Review 6.  Membrane transporters and folate homeostasis: intestinal absorption and transport into systemic compartments and tissues.

Authors:  Rongbao Zhao; Larry H Matherly; I David Goldman
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Review 8.  Finding new lanes: Chimeric antigen receptor (CAR) T-cells for myeloid leukemia.

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Journal:  Cancer Rep (Hoboken)       Date:  2020-01-08

Review 9.  Folate and thiamine transporters mediated by facilitative carriers (SLC19A1-3 and SLC46A1) and folate receptors.

Authors:  Rongbao Zhao; I David Goldman
Journal:  Mol Aspects Med       Date:  2013 Apr-Jun

10.  Grapefruit-derived Nanovectors Delivering Therapeutic miR17 Through an Intranasal Route Inhibit Brain Tumor Progression.

Authors:  Xiaoying Zhuang; Yun Teng; Abhilash Samykutty; Jingyao Mu; Zhongbin Deng; Lifeng Zhang; Pengxiao Cao; Yuan Rong; Jun Yan; Donald Miller; Huang-Ge Zhang
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