Phenotypic expression of pyruvate kinase deficiency and protection against malaria in a mouse model

Min‐Oo, Gundula; Fortin, Anny; Mf, Tam; Gros, Philippe; Mm, Stevenson

doi:10.1038/sj.gene.6364069

Cited by 33 publications

(34 citation statements)

References 35 publications

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“…42 The various cell populations were determined by singlecolor staining of the cells with fluorescein isothiocyanateor phytoerythrin-conjugated monoclonal antibodies against Mac-1 (CD11b, clone M1/70, rat IgG2b), Gr-1 (Ly-6G and Ly-6C, clone RB6-8C5, rat IgG2b), CD3e (clone 145-2C11, hamster IgG1), CD11c (clone HL3, hamster IgG1), CD49b/Pan-NK (clone DX5, rat IgM), I-A b (clone AF6-120.1, mouse (BALB/c) IgG2a) and IgM (clone R6-60.2, rat IgG2a). CD16/CD32 (clone 2.4G2, rat IgG2b) was used before staining to block the nonspecific binding by Fc receptors.…”

Section: Flow Cytometrymentioning

confidence: 99%

Incremental expression of Tlr4 correlates with mouse resistance to Salmonella infection and fine regulation of relevant immune genes

Larivière

Wilkinson

et al. 2006

Genes Immun

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Section: Flow Cytometrymentioning

confidence: 99%

Incremental expression of Tlr4 correlates with mouse resistance to Salmonella infection and fine regulation of relevant immune genes

Larivière

Wilkinson

et al. 2006

Genes Immun

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“…in (Hernandez-Valladares et al, 2005)]. Using positional cloning, we have shown that the protective effect of the Char4 locus is caused by a loss-of-function mutation in the erythrocyte form of pyruvate kinase ( Pklr I90N ) (Min-Oo et al, 2003; Min-Oo et al, 2004). Likewise, we observed that homozygosity and heterozygosity for mutant alleles at the human PKLR gene also protect against Plasmodium falciparum malaria in erythrocytes ex vivo (Ayi et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Cysteamine, the natural metabolite of pantetheinase, shows specific activity against Plasmodium

Min‐Oo

Ayi

Bongfen

et al. 2010

Experimental Parasitology

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In mice, loss of pantetheinase activity causes susceptibility to infection with Plasmodium chabaudi AS. Treatment of mice with the pantetheinase metabolite cysteamine reduces blood-stage replication of P. chabaudi and significantly increases survival. Similarly, a short exposure of Plasmodium to cysteamine ex vivo is sufficient to suppress parasite infectivity in vivo. This effect of cysteamine is specific and not observed with a related thiol (dimercaptosuccinic acid) or with the pantethine precursor of cysteamine. Also, cysteamine does not protect against infection with the parasite Trypanosoma cruzi or the fungal pathogen Candida albicans, suggesting cysteamine acts directly against the parasite and does not modulate host inflammatory response. Cysteamine exposure also blocks replication of P. falciparum in vitro; moreover, these treated parasites show higher levels of intact hemoglobin. This study highlights the in vivo action of cysteamine against Plasmodium and provides further evidence for the involvement of pantetheinase in host response to this infection.

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“…Splenomegaly was apparent and histological analysis revealed breakdown of normal splenic architecture and massive expansion of the red pulp in AcB62 (Figure 2a), all known consequences of PK deficiency. 11 Compared with A/J, AcB62 and AcB55 showed elevated spleen cell counts (twofold to fourfold increase; Figure 2b), and a higher fraction of CD71 þ /TER119 þ doubly positive erythroid precursors (Figure 2c). Owing to an RBC lysis step of spleen cell suspensions performed before labeling, the percentage of erythroid precursor cells is likely under-represented, but nevertheless indicates higher levels of erythroid progenitors in the PK mutant strains compared with A/J mice.…”

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confidence: 99%

“…These parameters suggest the presence of a slightly more severe anemia in AcB62 compared to that which we have reported earlier for AcB55 and AcB61. 11 Like AcB55, and as opposed to A/J controls, AcB62 mice show signs of compensatory erythropoietic activity in the spleen ( Figure 2) and liver (not shown). Splenomegaly was apparent and histological analysis revealed breakdown of normal splenic architecture and massive expansion of the red pulp in AcB62 (Figure 2a), all known consequences of PK deficiency.…”

mentioning

confidence: 99%

“…AcB55/AcB61 show signs of anemia even in the absence of P. chabaudi infection, manifested by splenomegaly, extramedullary erythropoiesis, and high levels of reticulocytes in the peripheral blood. 11 Using parasitemia and reticulocyte levels as quantitative traits in informative F2 populations derived from AcB55/ AcB61, a major locus (Char4) was identified that controlled both traits and mapped to the same segment of Chr. 3.…”

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confidence: 99%

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Mapping of Char10, a novel malaria susceptibility locus on mouse chromosome 9

Min‐Oo¹,

Willemetz²,

Tam³

et al. 2009

Genes Immun

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Resistance to blood-stage malaria in AcB55 and AcB61 is caused by a loss of function mutation in pyruvate kinase (Pklr I90N ). Likewise, pyruvate kinase (PK) deficiency in humans is protective against Plasmodium replication in vitro. We identified a third AcB strain, AcB62 that also carries the Pklr I90N mutation. However, AcB62 mice were susceptible to P.chabaudi infection and showed high levels of parasite replication (54-62% peak parasitemia). AcB62 mice showed the hallmarks of PK deficiencyassociated anemia similar to AcB55/61 with reticulocytosis, splenic red pulp expansion, tissue iron overload, and increased expression of iron metabolism proteins. This suggests that malaria susceptibility in AcB62 is not because of absence of PK deficiency-associated pathophysiology. To map novel genetic factors affecting malaria susceptibility in AcB62, we generated an informative F2 population using AcB62 (Pklr I90N ) and CBA-Pk slc (Pklr G338D ) as progenitors and identified a novel locus on chromosome 9 (Char10; LOD ¼ 7.24) that controls peak parasitemia. A weaker linkage to the Pklr region of chromosome 3 (LOD ¼ 3.7) was also detected, a finding that may reflect the segregation of the two defective Pklr alleles. AcB62 alleles at both loci are associated with higher peak parasitemia. These results identify Char10 as a novel locus modulating severity of malaria in the context of PK deficiency.

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Phenotypic expression of pyruvate kinase deficiency and protection against malaria in a mouse model

Cited by 33 publications

References 35 publications

Incremental expression of Tlr4 correlates with mouse resistance to Salmonella infection and fine regulation of relevant immune genes

Incremental expression of Tlr4 correlates with mouse resistance to Salmonella infection and fine regulation of relevant immune genes

Cysteamine, the natural metabolite of pantetheinase, shows specific activity against Plasmodium

Mapping of Char10, a novel malaria susceptibility locus on mouse chromosome 9

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