4.2 Article

Diffraction contrast in cryo-scanning transmission electron tomography reveals the boundary of hemozoin crystals in situ

Journal

FARADAY DISCUSSIONS
Volume 240, Issue -, Pages 127-141

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d2fd00088a

Keywords

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Funding

  1. Minerva Research Foundation
  2. Israel Science Foundation [1523/18, 1696/18]
  3. Estate of David Levinson
  4. Ministry of Science and Technology [103240]
  5. United States-Israel Binational Science Foundation (BSF) [2019236]
  6. Dr Louis M. Leland and Ruth M. Leland Chair in Infectious Diseases
  7. Irving and Cherna Moskowitz Center for Nano

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Malaria, a potentially fatal infectious disease caused by parasites, can be treated by interfering with the crystallization process of parasites within human red blood cells. This study used cryo-scanning transmission electron tomography to investigate the chemical environment of crystallization and found no intermediate medium surrounding the crystals. These findings have important implications for evaluating new drug candidates.
Malaria is a potentially fatal infectious disease caused by the obligate intracellular parasite Plasmodium falciparum. The parasite infects human red blood cells (RBC) and derives nutrition by catabolism of hemoglobin. As amino acids are assimilated from the protein component, the toxic heme is released. Molecular heme is detoxified by rapid sequestration to physiologically insoluble hemozoin crystals within the parasite's digestive vacuole (DV). Common antimalarial drugs interfere with this crystallization process, leaving the parasites vulnerable to the by-product of their own metabolism. A fundamental debate with important implications on drug mechanism regards the chemical environment of crystallization in situ, whether aqueous or lipid. This issue had been addressed previously by cryogenic soft X-ray tomography. We employ cryo-scanning transmission electron tomography (CSTET) to probe parasite cells throughout the life cycle in a fully hydrated, vitrified state at higher resolution. During the acquisition of CSTET data, Bragg diffraction from the hemozoin provides a uniquely clear view of the crystal boundary at nanometer resolution. No intermediate medium, such as a lipid coating or shroud, could be detected surrounding the crystals. The present study describes a unique application of CSTET in the study of malaria. The findings can be extended to evaluate new drug candidates affecting hemozoin crystal growth.

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