Fine Mapping of
 Leishmania major
 Susceptibility Locus
 lmr2
 and Evidence of a Role for
 Fli1
 in Disease and Wound Healing

Sakthianandeswaren, Anuratha; Curtis, Joan M.; Elso, Colleen M.; Kumar, Beena; Baldwin, Tracey M.; Lopaticki, Sash; Kędzierski, Łukasz; Smyth, Gordon K.; Foote, Simon J.; Handman, Emanuela

doi:10.1128/iai.00126-10

Cited by 33 publications

(40 citation statements)

References 37 publications

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“…Polymorphisms in this factor's gene govern susceptibility to cutaneous leishmaniasis (6,51), and Abl facilitates FLI-1 activation (4). However, decreased FLI-1 activity and subsequent effects on wound healing should not lower parasite burdens (51). Thus, it seems unlikely that differences in FLI-1 activation are solely responsible for the differences we see in lesion size in Abl family kinase-deficient mice.…”

Section: Discussionmentioning

confidence: 99%

The Abl and Arg Kinases Mediate Distinct Modes of Phagocytosis and Are Required for Maximal Leishmania Infection

Wetzel

McMahon-Pratt

Koleske

2012

Molecular and Cellular Biology

130

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Leishmania, an obligate intracellular parasite, binds several receptors to trigger engulfment by phagocytes, leading to cutaneous or visceral disease. These receptors include complement receptor 3 (CR3), used by promastigotes, and the Fc receptor (FcR), used by amastigotes. The mechanisms mediating uptake are not well understood. Here we show that Abl family kinases mediate both phagocytosis and the uptake of Leishmania amazonensis by macrophages (Ms). Imatinib, an Abl/Arg kinase inhibitor, decreases opsonized polystyrene bead phagocytosis and Leishmania uptake. Interestingly, phagocytosis of IgG-coated beads is decreased in Arg-deficient Ms, while that of C3bi-coated beads is unaffected. Conversely, uptake of C3bi-coated beads is decreased in Abl-deficient Ms, but that of IgG-coated beads is unaffected. Consistent with these results, Abl-deficient Ms are inefficient at C3bi-opsonized promastigote uptake, and Arg-deficient Ms are defective in IgG1-opsonized amastigote uptake. Finally, genetic loss of Abl or Arg reduces infection severity in murine cutaneous leishmaniasis, and imatinib treatment results in smaller lesions with fewer parasites than in controls. Our studies are the first to demonstrate that efficient phagocytosis and maximal Leishmania infection require Abl family kinases. These results highlight Abl family kinase-mediated signaling pathways as potential therapeutic targets for leishmaniasis. L eishmania parasites cause cutaneous or visceral disease in 1 to 2 million people a year in the developing world (17). Leishmania undergoes two life cycle stages: (i) the promastigote, found in the sand fly, and (ii) the amastigote, found in mammalian hosts. When an infected sand fly bites a host, the injected promastigotes must be engulfed by phagocytes to establish infection. The promastigotes then differentiate into amastigotes within the phagolysosome. If the amastigote finds itself outside a cell, it must be reengulfed for continued infection (23).Several M surface proteins permit Leishmania uptake. Promastigote internalization is mediated by the fibronectin receptor (integrin ␣5␤1) (2), the mannose-fucose receptor (63, 64), and complement receptors CR1 (10) and CR3 (38). Promastigotes may interact directly with CR3 (49), but binding is facilitated by opsonization with C3bi, a complement component (22,37,40,45). Both CR3 and the Fc receptor (FcR) mediate amastigote uptake (16); interactions with the latter are facilitated by IgG opsonization (35). The FcR subclass Fc␥R, which mediates IgG-mediated phagocytosis (33), is most likely responsible for amastigote uptake by Ms. Indeed, internalization of IgG-opsonized amastigotes via FcR␥I and -III sustains infection in murine cutaneous leishmaniasis (8,24,65). Adhesion of Leishmania to any of these receptors causes an actin-rich phagocytic cup to form and engulf the parasite (30). Our study explores the requirement for actin regulatory proteins in efficient Leishmania internalization.The Abl family kinases Abl and Arg translate signals from adhesion and growth...

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Section: Discussionmentioning

confidence: 99%

The Abl and Arg Kinases Mediate Distinct Modes of Phagocytosis and Are Required for Maximal Leishmania Infection

Wetzel

McMahon-Pratt

Koleske

2012

Molecular and Cellular Biology

130

View full text Add to dashboard Cite

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“…In the last few years we have shown that polymorphisms at genes associated with wound healing and tissue repair are important risk factors for cutaneous leishmaniasis (CL) caused by Leishmania braziliensis (Castellucci et al, 2012; Castellucci et al, 2011). Thus, the FLI1 gene, initially identified and mapped as a gene controlling susceptibility to CL caused by L. major infection in mice (Sakthianandeswaren et al, 2010; Sakthianandeswaren et al, 2005), was also associated with development of CL in humans exposed to L. braziliensis in Brazil. In addition, our data showed that polymorphisms in other wound healing genes related to FLI1 function, in particular genes ( TGFB1, TGFBR2, CTGF, SMAD2/3/7 ) encoding proteins in the transforming growth factor β (TGF-β) signaling pathway, were risk factors for CL.…”

Section: Introductionmentioning

confidence: 99%

Wound healing genes and susceptibility to cutaneous leishmaniasis in Brazil: Role of COL1A1

Almeida

Oliveira

Guimarães

et al. 2015

Infection, Genetics and Evolution

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Previous studies have demonstrated a role for wound healing genes in resolution of cutaneous lesions caused by Leishmania spp. in both mice and humans, including the gene FLI1 encoding Friend leukaemia virus integration 1. Reduction of Fli1 expression in mice has been shown to result in up-regulation of collagen type I alpha 1 (Col1a1) and alpha 2 (Col1a2) genes and, conversely, in down-regulation of the matrix metalloproteinase 1 (Mmp1) gene, suggesting that Fli1 suppression is involved in activation of the profibrotic gene program. Here we examined single nucleotide polymorphisms (SNPs) in these genes as risk factors for cutaneous (CL) and mucosal leishmaniasis (ML), and leishmaniasis per se, caused by L. braziliensis in humans. SNPs were genotyped in 168 nuclear families (250 CL; 87 ML cases) and replicated in 157 families (402 CL; 39 ML cases). Family-based association tests (FBAT) showed the strongest association between SNPs rs1061237 (combined P=0.002) and rs2586488 (combined P=0.027) at COL1A1 and CL disease. This contributes to our further understanding of the role of wound healing in the resolution of CL disease, providing potential for therapies modulating COL1A1 via drugs acting on FLI1.

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“…A locus regulating differential susceptibility of BALB/c (susceptible) and B6 (resistant) mice to cutaneous leishmaniasis induced by infection with Leishmania major, and designated Lmr2, has been mapped to a ~10 Mb interval on chromosome 9 that overlaps the genetic interval defined herein for the Ccs4 locus [31]. The genetic difference at Lmr2 is expressed as a vigorous wound healing response required for lesion resolution following cutaneous infection with L. major.…”

Section: Discussionmentioning

confidence: 99%

“…A number of candidate genes have been proposed for Lmr2 including Tirap, Fli1, Il10ra, as well as members of the Mmp family, and Aplp2. Recently, a functional promotor polymorphism in the Fli1 gene has been proposed as a strong candidate for Lmr2 [31]. The possibility that the Ccs4-controlled differential susceptibility to CA-CRC may involve differential response to, and recovery from acute inflammationinduced tissue injury requires further investigation.…”

Section: Discussionmentioning

confidence: 99%

A Two-Locus System Controls Susceptibility to Colitis-Associated Colon Cancer in Mice

et al. 2010

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AbstrAct:We have previously shown that the differential susceptibility of A/J (susceptible) and C57BL/6J (B6, resistant) mouse strains to azoxymethane (AOM)-induced colorectal cancer (CRC) is controlled by the chromosome 3 locus, Ccs3. We report that A/J and B6 mice also show differential susceptibility to colitis-associated colorectal cancer (CA-CRC) induced by combined administration of AOM and dextran sulfate. This differential susceptibility is not controlled by Ccs3, but is under distinct genetic control. Linkage analyses in (A/J x B6)F2 mice detected a major CA-CRC susceptibility locus on chromosome 9 (Ccs4) which controls tumor multiplicity and tumor surface area. Susceptibility alleles at Ccs4 are inherited in a recessive fashion, with A/J alleles being associated with susceptibility. We also detected a second locus on chromosome 14 that acts in an additive fashion with Ccs4. Strikingly, F2 mice homozygous for A/J alleles at both loci (Ccs4 and chromosome 14) are as susceptible to CA-CRC as the A/J controls while mice homozygous for B6 alleles are as resistant as the B6 controls, thus supporting the role of two interacting loci in this CA-CRC model. This indicates that susceptibility to chemically-induced CRC and susceptibility to CA-CRC are under distinct genetic control in mice, and probably involve distinct cellular pathways.

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Fine Mapping of Leishmania major Susceptibility Locus lmr2 and Evidence of a Role for Fli1 in Disease and Wound Healing

Cited by 33 publications

References 37 publications

The Abl and Arg Kinases Mediate Distinct Modes of Phagocytosis and Are Required for Maximal Leishmania Infection

The Abl and Arg Kinases Mediate Distinct Modes of Phagocytosis and Are Required for Maximal Leishmania Infection

Wound healing genes and susceptibility to cutaneous leishmaniasis in Brazil: Role of COL1A1

A Two-Locus System Controls Susceptibility to Colitis-Associated Colon Cancer in Mice

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