Gene expression within the apicoplast, an organelle in the malaria parasite Plasmodium falciparum, is regulated by melatonin (the circadian signaling hormone) in host blood, and intrinsic parasite cues, via a factor called ApSigma, as identified by a recent study aided by Tokyo Tech’s World Research Hub Initiative. The regulatory system highlighted in this study might be a future target for malaria treatment.
Credit: Professor Kan Tanaka, Tokyo Institute of Technology
Gene expression within the apicoplast, an organelle in the malaria parasite Plasmodium falciparum, is regulated by melatonin (the circadian signaling hormone) in host blood, and intrinsic parasite cues, via a factor called ApSigma, as identified by a recent study aided by Tokyo Tech’s World Research Hub Initiative. The regulatory system highlighted in this study might be a future target for malaria treatment.
Malaria is one of the biggest public health risks, with around 240 million people from across the globe contracting it every year. However, this life-threatening disease is not contagious. It is transmitted by the bite of a female Anopheles mosquito infected with the malaria parasite, Plasmodium falciparum. This parasite enters the human body through the mosquito bite and causes symptoms like fever, cold, fatigue, and headache, which are highly periodic. The periodicity of symptoms can be linked to the synchronization of the parasite’s life cycle with the circadian rhythm—i.e., the 24-hour internal biological clock—of the infected person or the host.
P. falciparum contains an apicoplast, a unique cellular organelle which contains its own genome and is crucial for the parasite’s life cycle. Despite its importance, however, not much is known about the mechanisms regulating gene expression in apicoplasts and their potential role in modulating the observed periodicity of malaria symptoms, or the life cycle of P. falciparum. This is why recently, a team of scientists led by Professor Kan Tanaka, of Tokyo Institute of Technology (Tokyo Tech), undertook a joint research project to take a closer look at the underlying mechanisms that mediate apicoplast gene expression. The work, published in Proceedings of National Academy of Sciences of United States of America (PNAS), was a result of collaboration with co-authors Professor Kiyoshi Kita of Nagasaki University and Professor Antony N. Dodd, a group leader at the John Innes Centre in the UK—also a visiting professor at Tokyo Tech—facilitated by the institute’s World Research Hub Initiative (WRHI), a project for interdisciplinary collaboration with leading researchers from across the world.
“Previous studies have shown that certain plant σ subunits participate in the circadian regulation of gene expression in plastids (i.e., organelles like the apicoplast). Therefore, the present study hypothesized that a nuclear-encoded σ subunit might coordinate apicoplast gene expression with the life cycle of P. falciparum or the circadian rhythm of its host,” explains Prof. Tanaka.
The team cultured P. falciparum in a lab and studied it using phylogenetic analysis and immunofluorescence microscopy techniques. As a result, they identified ApSigma, a nuclear encoded apicoplast RNA polymerase σ subunit. It, along with the α subunit, likely mediates apicoplast transcript accumulation, whose periodicity is akin to that of the parasite’s developmental control. In addition, apicoplast transcription and expression of the apicoplast subunit gene, apSig, increased in the presence of melatonin, the circadian signaling hormone present in host blood.
Based on the data collected from different tests, the scientists suggest that there is an evolutionarily preserved regulatory system in which the host’s circadian rhythm is integrated with the parasite’s intrinsic cues. Together, they coordinate genome transcription in the apicoplast of P. falciparum. This work lays solid groundwork for further studies in the field aiming to comprehensively explain the regulatory mechanisms of Plasmodium’s cell cycle.
In conclusion, Prof. Tanaka highlights the future implications of the present research. “Malaria kills hundreds of thousands of people across the world, every year. This study identifies a regulatory system that might be a future target for malaria treatment.”
Professor Dodd, adds to that, “It is amazing that a process we identified in plants has led to the discovery of an equivalent mechanism in a globally important pathogen. The new protein and mechanism identified could present a new target for the development of drugs for the treatment and or prevention of malaria, in both humans and farm animals.”
Professor Kita signs off on a positive note. “This research demonstrates the value of international and interdisciplinary collaboration, and the power of plant sciences and microbiology to drive unusual and novel discoveries that could be of considerable global benefit,” he says.
Here’s hoping for efficient treatment of malaria!
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Related Links
Circadian Control of Chloroplast Transcription by a Nuclear-Encoded Timing Signal|Science
The parasite intraerythrocytic cycle and human circadian cycle are coupled during malaria infection|
PNASTANAKA-YOSHIDA Lab, TTECH
About Tokyo Institute of Technology
Tokyo Tech stands at the forefront of research and higher education as the leading university for science and technology in Japan. Tokyo Tech researchers excel in fields ranging from materials science to biology, computer science, and physics. Founded in 1881, Tokyo Tech hosts over 10,000 undergraduate and graduate students per year, who develop into scientific leaders and some of the most sought-after engineers in industry. Embodying the Japanese philosophy of “monotsukuri,” meaning “technical ingenuity and innovation,” the Tokyo Tech community strives to contribute to society through high-impact research.
https://www.titech.ac.jp/english/
About Nagasaki University
In November 1857, a Dutch army surgeon JLC Pompe van Meerdervoort started medical lectures in Dutch to 12 students including Ryojyun Matsumoto, a Shogunate doctor. This medical school is the origin of the School of Medicine in Nagasaki University today and the university itself. Faculties of Education, Pharmaceutical Science, and Economics also celebrate 100 years of history. Experiencing the tragic event in 1945 when the atomic bomb dropped in Nagasaki city hit our students, teachers and staff members, a new Nagasaki University was created in May 1949 under the National School Establishment Law, merged with Higher School, Nagasaki Medical School, Teachers’ School and others. The university currently has ten undergraduate faculties/schools and eight graduate schools for education and research, further expanding its scope to meet demands of the time.
http://www.nagasaki-u.ac.jp/en/
About the John Innes Centre
The John Innes Centre is an independent, international centre of excellence in plant science and microbiology.
Our mission is to generate knowledge of plants and microbes through innovative research, to train scientists for the future, to apply our knowledge of nature’s diversity to benefit agriculture, the environment, human health, and wellbeing, and engage with policy makers and the public.
To achieve these goals we establish pioneering long-term research objectives in plant and microbial science, with a focus on genetics. These objectives include promoting the translation of research through partnerships to develop improved crops and to make new products from microbes and plants for human health and other applications. We also create new approaches, technologies and resources that enable research advances and help industry to make new products. The knowledge, resources and trained researchers we generate help global societies address important challenges including providing sufficient and affordable food, making new products for human health and industrial applications, and developing sustainable bio-based manufacturing.
This provides a fertile environment for training the next generation of plant and microbial scientists, many of whom go on to careers in industry and academia, around the world.
The John Innes Centre is strategically funded by the Biotechnology and Biological Sciences Research Council (BBSRC), and is supported by the John Innes Foundation through provision of research accommodation, capital funding and long-term support of the Rotation PhD programme.
For more information about the John Innes Centre visit our website www.jic.ac.uk
Journal
Proceedings of the National Academy of Sciences
DOI
10.1073/pnas.2214765120
Method of Research
Experimental study
Subject of Research
Animals
Article Title
Coordination of apicoplast transcription in a malaria parasite by internal and host cues
Article Publication Date
3-Jul-2023
COI Statement
The authors declare no competing interest.