Abstract
Malaria parasites must undergo a round of sexual reproduction in the blood meal of a mosquito vector to be transmitted between hosts. Developing a transmission-blocking intervention to prevent parasites from mating is a major goal of biomedicine, but its effectiveness could be compromised if parasites can compensate by simply adjusting their sex allocation strategies. Recently, the application of evolutionary theory for sex allocation has been supported by experiments demonstrating that malaria parasites adjust their sex ratios in response to infection genetic diversity, precisely as predicted. Theory also predicts that parasites should adjust sex allocation in response to host immunity. Whilst data are supportive, the assumptions underlying this prediction – that host immune responses have differential effects on the mating ability of males and females – have not yet been tested. Here, we combine experimental work with theoretical models in order to investigate whether the development and fertility of male and female parasites is affected by innate immune factors and develop new theory to predict how parasites' sex allocation strategies should evolve in response to the observed effects. Specifically, we demonstrate that reactive nitrogen species impair gametogenesis of males only, but reduce the fertility of both male and female gametes. In contrast, tumour necrosis factor-α does not influence gametogenesis in either sex but impairs zygote development. Therefore, our experiments demonstrate that immune factors have complex effects on each sex, ranging from reducing the ability of gametocytes to develop into gametes, to affecting the viability of offspring. We incorporate these results into theory to predict how the evolutionary trajectories of parasite sex ratio strategies are shaped by sex differences in gamete production, fertility and offspring development. We show that medical interventions targeting offspring development are more likely to be ‘evolution-proof’ than interventions directed at killing males or females. Given the drive to develop medical interventions that interfere with parasite mating, our data and theoretical models have important implications.
Highlights
Malaria parasites are obliged to undertake a single round of sexual reproduction in the mosquito vector before they can transmit to new hosts, making this stage of their life-cycle a potential target for medical interventions [1,2]
Experiment 2: Effects of reactive nitrogen species (RNS) and tumour necrosis factor-a (TNF-a) on gametogenesis and ookinete production Having found significant negative effects of RNS and TNF-a on exflagellation and ookinete production we investigated whether these factors interacted with each other to further reduce parasite mating success and if these effects depended on the developmental stage at which parasites were exposed
We observed that RNS exposure significantly reduced fertility of both males and females regardless of whether parasites were exposed as gametocytes or during gametogenesis (F(1,131) = 15.87, P = 0.0001; mean ‘RNS2’ 0.3060.02; ‘RNS+’ 0.2060.02)
Summary
Malaria parasites are obliged to undertake a single round of sexual reproduction in the mosquito vector before they can transmit to new hosts, making this stage of their life-cycle a potential target for medical interventions [1,2]. Current candidates for transmission-blocking vaccines (TBV) involve targeting proteins, expressed on the surface of sexual stages, that are essential for the fertility of males (e.g. P48/45 and P230) [4,5,6,7,8]. Theory predicts that the efficacy of a vaccine that reduces the fertility of one sex may be eroded if parasites respond by adjusting their sex ratios in favour of the targeted sex. The study of sex allocation has been one of the most successful areas of evolutionary biology, with empirical data matching clear theoretical predictions across a variety of taxa [9]. Before describing evolutionary theory for sex allocation strategies we outline the relevant aspects of Plasmodium mating biology
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
