Targeting circulating labile heme as a defense strategy against malaria

Susana Ramos; Viktoria Jeney; Ana Figueiredo; Tiago Paixão; Maria Rosário Sambo; Vatúsia Quinhentos; Rui Martins; Zélia Gouveia; Ana Rita Carlos; Ana Ferreira; Teresa F. Pais; Hugo Lainé; Pedro Faísca; Sofia Rebelo; Silvia Cardoso; Emanuela Tolosano; Carlos Penha-Gonçalves; Miguel P. Soares

doi:10.26508/lsa.202302276

Targeting circulating labile heme as a defense strategy against malaria

Susana Ramos
, Viktoria Jeney
, Ana Figueiredo
, Tiago Paixão
, Maria Rosário Sambo
, Vatúsia Quinhentos
, Rui Martins
, Zélia Gouveia
, Ana Rita Carlos
, Ana Ferreira
, Teresa F. Pais
, Hugo Lainé
, Pedro Faísca
, Sofia Rebelo
, Silvia Cardoso
, Emanuela Tolosano
, Carlos Penha-Gonçalves
, Miguel P. Soares

Resultado de pesquisa: ???type-name??? › ???researchoutput.researchoutputtypes.contributiontojournal.article??? › revisão de pares

11 Citações (Scopus)

Resumo

Severe presentations of malaria emerge as Plasmodium (P.) spp. parasites invade and lyse red blood cells (RBC), producing extracellular hemoglobin (HB), from which labile heme is re-leased. Here, we tested whether scavenging of extracellular HB and/or labile heme, by haptoglobin (HP) and/or hemopexin (HPX), respectively, counter the pathogenesis of severe presentations of malaria. We found that circulating labile heme is an independent risk factor for cerebral and non-cerebral presentations of severe P. falciparum malaria in children. Labile heme was negatively correlated with circulating HP and HPX, which were, however, not risk factors for severe P. fal-ciparum malaria. Genetic Hp and/or Hpx deletion in mice led to labile heme accumulation in plasma and kidneys, upon Plas-modium infection. This was associated with higher incidence of mortality and acute kidney injury (AKI) in ageing but not adult Plasmodium-infected mice, and was corroborated by an in-verse correlation between heme and HPX with serological markers of AKI in P. falciparum malaria. In conclusion, HP and HPX act in an age-dependent manner to prevent the patho-genesis of severe presentation of malaria in mice and pre-sumably in humans.

Idioma original	???core.languages.en_GB???
Número do artigo	e202302276
Número de páginas	20
Revista	Life Science Alliance
Volume	7
Número de emissão	4
DOIs	https://doi.org/10.26508/lsa.202302276
Estado da publicação	???researchoutput.status.published??? - abr. 2024
Publicado externamente	Sim

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Ramos, S., Jeney, V., Figueiredo, A., Paixão, T., Sambo, M. R., Quinhentos, V., Martins, R., Gouveia, Z., Carlos, A. R., Ferreira, A., Pais, T. F., Lainé, H., Faísca, P., Rebelo, S., Cardoso, S., Tolosano, E., Penha-Gonçalves, C., & Soares, M. P. (2024). Targeting circulating labile heme as a defense strategy against malaria. Life Science Alliance, 7(4), Artigo e202302276. https://doi.org/10.26508/lsa.202302276

@article{2c74a34408414921af620f9873acc632,

title = "Targeting circulating labile heme as a defense strategy against malaria",

abstract = "Severe presentations of malaria emerge as Plasmodium (P.) spp. parasites invade and lyse red blood cells (RBC), producing extracellular hemoglobin (HB), from which labile heme is re-leased. Here, we tested whether scavenging of extracellular HB and/or labile heme, by haptoglobin (HP) and/or hemopexin (HPX), respectively, counter the pathogenesis of severe presentations of malaria. We found that circulating labile heme is an independent risk factor for cerebral and non-cerebral presentations of severe P. falciparum malaria in children. Labile heme was negatively correlated with circulating HP and HPX, which were, however, not risk factors for severe P. fal-ciparum malaria. Genetic Hp and/or Hpx deletion in mice led to labile heme accumulation in plasma and kidneys, upon Plas-modium infection. This was associated with higher incidence of mortality and acute kidney injury (AKI) in ageing but not adult Plasmodium-infected mice, and was corroborated by an in-verse correlation between heme and HPX with serological markers of AKI in P. falciparum malaria. In conclusion, HP and HPX act in an age-dependent manner to prevent the patho-genesis of severe presentation of malaria in mice and pre-sumably in humans.",

keywords = "Acute Kidney Injury, Animals, Child, Haptoglobins, Heme, Hemoglobins, Humans, Malaria, Mice, Susceptibility, Hemopexin, Confers tolerance, Haptoglobin, Human-serum-albumin, Rna-seq, Hemoglobin, Disease tolerance, Falciparum-malaria, Oxygenase-1",

author = "Susana Ramos and Viktoria Jeney and Ana Figueiredo and Tiago Paix{\~a}o and Sambo, \{Maria Ros{\'a}rio\} and Vat{\'u}sia Quinhentos and Rui Martins and Z{\'e}lia Gouveia and Carlos, \{Ana Rita\} and Ana Ferreira and Pais, \{Teresa F.\} and Hugo Lain{\'e} and Pedro Fa{\'i}sca and Sofia Rebelo and Silvia Cardoso and Emanuela Tolosano and Carlos Penha-Gon{\c c}alves and Soares, \{Miguel P.\}",

note = "{\textcopyright} 2024 Ramos et al.",

year = "2024",

month = apr,

doi = "10.26508/lsa.202302276",

language = "English",

volume = "7",

journal = "Life Science Alliance",

issn = "2575-1077",

publisher = "Life Science Alliance, LLC",

number = "4",

}

Ramos, S, Jeney, V, Figueiredo, A, Paixão, T, Sambo, MR, Quinhentos, V, Martins, R, Gouveia, Z, Carlos, AR, Ferreira, A, Pais, TF, Lainé, H, Faísca, P, Rebelo, S, Cardoso, S, Tolosano, E, Penha-Gonçalves, C & Soares, MP 2024, 'Targeting circulating labile heme as a defense strategy against malaria', Life Science Alliance, vol. 7, n.º 4, e202302276. https://doi.org/10.26508/lsa.202302276

TY - JOUR

T1 - Targeting circulating labile heme as a defense strategy against malaria

AU - Ramos, Susana

AU - Jeney, Viktoria

AU - Figueiredo, Ana

AU - Paixão, Tiago

AU - Sambo, Maria Rosário

AU - Quinhentos, Vatúsia

AU - Martins, Rui

AU - Gouveia, Zélia

AU - Carlos, Ana Rita

AU - Ferreira, Ana

AU - Pais, Teresa F.

AU - Lainé, Hugo

AU - Faísca, Pedro

AU - Rebelo, Sofia

AU - Cardoso, Silvia

AU - Tolosano, Emanuela

AU - Penha-Gonçalves, Carlos

AU - Soares, Miguel P.

PY - 2024/4

Y1 - 2024/4

N2 - Severe presentations of malaria emerge as Plasmodium (P.) spp. parasites invade and lyse red blood cells (RBC), producing extracellular hemoglobin (HB), from which labile heme is re-leased. Here, we tested whether scavenging of extracellular HB and/or labile heme, by haptoglobin (HP) and/or hemopexin (HPX), respectively, counter the pathogenesis of severe presentations of malaria. We found that circulating labile heme is an independent risk factor for cerebral and non-cerebral presentations of severe P. falciparum malaria in children. Labile heme was negatively correlated with circulating HP and HPX, which were, however, not risk factors for severe P. fal-ciparum malaria. Genetic Hp and/or Hpx deletion in mice led to labile heme accumulation in plasma and kidneys, upon Plas-modium infection. This was associated with higher incidence of mortality and acute kidney injury (AKI) in ageing but not adult Plasmodium-infected mice, and was corroborated by an in-verse correlation between heme and HPX with serological markers of AKI in P. falciparum malaria. In conclusion, HP and HPX act in an age-dependent manner to prevent the patho-genesis of severe presentation of malaria in mice and pre-sumably in humans.

AB - Severe presentations of malaria emerge as Plasmodium (P.) spp. parasites invade and lyse red blood cells (RBC), producing extracellular hemoglobin (HB), from which labile heme is re-leased. Here, we tested whether scavenging of extracellular HB and/or labile heme, by haptoglobin (HP) and/or hemopexin (HPX), respectively, counter the pathogenesis of severe presentations of malaria. We found that circulating labile heme is an independent risk factor for cerebral and non-cerebral presentations of severe P. falciparum malaria in children. Labile heme was negatively correlated with circulating HP and HPX, which were, however, not risk factors for severe P. fal-ciparum malaria. Genetic Hp and/or Hpx deletion in mice led to labile heme accumulation in plasma and kidneys, upon Plas-modium infection. This was associated with higher incidence of mortality and acute kidney injury (AKI) in ageing but not adult Plasmodium-infected mice, and was corroborated by an in-verse correlation between heme and HPX with serological markers of AKI in P. falciparum malaria. In conclusion, HP and HPX act in an age-dependent manner to prevent the patho-genesis of severe presentation of malaria in mice and pre-sumably in humans.

KW - Acute Kidney Injury

KW - Animals

KW - Child

KW - Haptoglobins

KW - Heme

KW - Hemoglobins

KW - Humans

KW - Malaria

KW - Mice

KW - Susceptibility

KW - Hemopexin

KW - Confers tolerance

KW - Haptoglobin

KW - Human-serum-albumin

KW - Rna-seq

KW - Hemoglobin

KW - Disease tolerance

KW - Falciparum-malaria

KW - Oxygenase-1

UR - https://www.scopus.com/pages/publications/85183790814

U2 - 10.26508/lsa.202302276

DO - 10.26508/lsa.202302276

M3 - Article

C2 - 38307624

AN - SCOPUS:85183790814

SN - 2575-1077

VL - 7

JO - Life Science Alliance

JF - Life Science Alliance

IS - 4

M1 - e202302276

ER -

Targeting circulating labile heme as a defense strategy against malaria

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