Identification of an AP2-family Protein That Is Critical for Malaria Liver Stage Development

Shiroh Iwanaga,Izumi Kaneko,Tomomi Kato,Masao Yuda,Anne Charlotte Gruner

doi:10.1371/journal.pone.0047557

Shiroh Iwanaga, Izumi Kaneko + Show 3 more

Open Access

https://doi.org/10.1371/journal.pone.0047557

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Journal: PloS one	Publication Date: Nov 7, 2012
Citations: 115	License type: CC BY 4.0

Affiliation: Mie University

Abstract

Liver-stage malaria parasites are a promising target for drugs and vaccines against malaria infection. However, little is currently known about gene regulation in this stage. In this study, we used the rodent malaria parasite Plasmodium berghei and showed that an AP2-family transcription factor, designated AP2-L, plays a critical role in the liver-stage development of the parasite. AP2-L-depleted parasites proliferated normally in blood and in mosquitoes. However, the ability of these parasites to infect the liver was approximately 10,000 times lower than that of wild-type parasites. In vitro assays showed that the sporozoites of these parasites invaded hepatocytes normally but that their development stopped in the middle of the liver schizont stage. Expression profiling using transgenic P. berghei showed that fluorescent protein-tagged AP2-L increased rapidly during the liver schizont stage but suddenly disappeared with the formation of the mature liver schizont. DNA microarray analysis showed that the expression of several genes, including those of parasitophorous vacuole membrane proteins, was significantly decreased in the early liver stage of AP2-L-depleted parasites. Investigation of the targets of this transcription factor should greatly promote the exploration of liver-stage antigens and the elucidation of the mechanisms of hepatocyte infection by malaria parasites.

Highlights

The transmission of malaria to humans is initiated by the bite of an Anopheles mosquito, which deposits malaria sporozoites from the mosquito salivary glands into the skin of the host
We report that an Apetala 2 (AP2)-family transcription factor of the rodent malaria parasite P. berghei (PlasmoDB ID, PBANKA_021440, designated AP2-L) is expressed in LS parasites
To investigate the involvement of AP2-family transcription factors in liver infection by P. berghei, we searched for expressed sequence tags (ESTs) encoding AP2 transcription factors in our P. berghei sporozoite EST database

Summary

Introduction

The transmission of malaria to humans is initiated by the bite of an Anopheles mosquito, which deposits malaria sporozoites from the mosquito salivary glands into the skin of the host. All mosquito stages (oocysts, oocyst sporozoites and salivary gland sporozoites) formed in numbers similar to those of wild-type parasites (Table S1). From the replication rate of the asexual blood stage (,6–10 fold per day) and the delay in parasitemia, the liver infection ability of AP2-L(2) parasites was estimated to be approximately 10,000 times lower than that of wild-type parasites.

Results

Conclusion