Haem-responsive gene transporter enables mobilization of host haem in ticks
Author(s) -
Jan Perner,
Tereza Hatalová,
María CabelloDonayre,
Veronika Urbanová,
Daniel Sojka,
Helena Frantová,
David J. Hartmann,
Dagmar Jírsová,
José M. PérezVictoria,
Petr Kopáček
Publication year - 2021
Publication title -
open biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.078
H-Index - 53
ISSN - 2046-2441
DOI - 10.1098/rsob.210048
Subject(s) - biology , gene , biochemistry , transcriptome , transporter , heme , genetics , gene expression , enzyme
Ticks, notorious blood-feeders and disease-vectors, have lost a part of their genetic complement encoding haem biosynthetic enzymes and are, therefore, dependent on the acquisition and distribution of host haem. Solute carrier protein SLC48A1, aka haem-responsive gene 1 protein (HRG1), has been implicated in haem transport, regulating the availability of intracellular haem. HRG1 transporter has been identified in both free-living and parasitic organisms ranging from unicellular kinetoplastids, nematodes, up to vertebrates. However, an HRG1 homologue in the arthropod lineage has not yet been identified. We have identified a single HRG1 homologue in the midgut transcriptome of the tickIxodes ricinus, denoted asIr HRG, and have elucidated its role as a haem transporter. Data from haem biosynthesis-deficient yeast growth assays, systemic RNA interference and the evaluation of gallium protoporphyrin IX-mediated toxicity through tick membrane feeding clearly show thatIr HRG is thebona fide tetrapyrrole transporter. We argue that during evolution, ticks profited from retaining a functionalhrg1 gene in the genome because its protein product facilitates host haem escort from intracellularly digested haemoglobin, rendering haem bioavailable for a haem-dependent network of enzymes.
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