Nuclear pore complexes undergo Nup221 exchange during blood-stage asexual replication of Plasmodium parasites

James Blauwkamp; Sushma V Ambekar; Tahir Hussain; Gunnar R Mair; Josh R Beck; Sabrina Absalon

doi:10.1128/msphere.00750-24

Nuclear pore complexes undergo Nup221 exchange during blood-stage asexual replication of Plasmodium parasites

mSphere. 2024 Nov 11:e0075024. doi: 10.1128/msphere.00750-24. Online ahead of print.

Authors

James Blauwkamp^#¹, Sushma V Ambekar^#², Tahir Hussain², Gunnar R Mair^{2

3}, Josh R Beck², Sabrina Absalon¹

Affiliations

¹ Department of Pharmacology and Toxicology, Indiana University School of Medicine, Indianapolis, Indiana, USA.
² Department of Biomedical Sciences, Iowa State University, Ames, Iowa, USA.
³ School of Biological Sciences, Queen's University Belfast, Belfast, United Kingdom.

^# Contributed equally.

PMID: 39526784
DOI: 10.1128/msphere.00750-24

Abstract

Plasmodium parasites, the causative agents of malaria, undergo closed mitosis without breakdown of the nuclear envelope. Unlike closed mitosis in yeast, Plasmodium berghei parasites undergo multiple rounds of asynchronous nuclear divisions in a shared cytoplasm. This results in a multinucleated organism prior to the formation of daughter cells within an infected red blood cell. During this replication process, intact nuclear pore complexes (NPCs) and their component nucleoporins play critical roles in parasite growth, facilitating selective bi-directional nucleocytoplasmic transport and genome organization. Here, we utilize ultrastructure expansion microscopy to investigate P. berghei nucleoporins at the single nucleus level throughout the 24-hour blood-stage replication cycle. Our findings reveal that these nucleoporins are distributed around the nuclei and organized in a rosette structure previously undescribed around the centriolar plaque, responsible for intranuclear microtubule nucleation during mitosis. By adapting the recombination-induced tag exchange system to P. berghei through a single plasmid tagging system, which includes the tagging plasmid as well as the Cre recombinase, we provide evidence of NPC formation dynamics, demonstrating Nup221 turnover during parasite asexual replication. Our data shed light on the distribution of NPCs and their homeostasis during the blood-stage replication of P. berghei parasites.

Importance: Malaria, caused by Plasmodium species, remains a critical global health challenge, with an estimated 249 million cases and over 600,000 deaths in 2022, primarily affecting children under five. Understanding the nuclear dynamics of Plasmodium parasites, particularly during their unique mitotic processes, is crucial for developing novel therapeutic strategies. Our study leverages advanced microscopy techniques, such as ultrastructure expansion microscopy, to reveal the organization and turnover of nuclear pore complexes (NPCs) during the parasite's asexual replication. By elucidating these previously unknown aspects of NPC distribution and homeostasis, we provide valuable insights into the molecular mechanisms governing parasite mitosis. These findings deepen our understanding of parasite biology and may inform future research aimed at identifying new targets for anti-malarial drug development.

Keywords: Plasmodium berghei; RITE system; expansion microscopy; nuclear pore complexes.