Nanofocused Scanning X-ray Fluorescence Microscopy Revealing an Effect of Heterozygous Hemoglobin S and C on Biochemical Activities in Plasmodium falciparum-Infected Erythrocytes.
Benjamin FröhlichYang YangJudith ThomaJulian CzajorChristine LanscheCecilia SanchezMichael LanzerPeter CloetensMotomu TanakaPublished in: Analytical chemistry (2020)
While there is ample evidence suggesting that carriers of heterozygous hemoglobin S and C are protected from life-threatening malaria, little is known about the underlying biochemical mechanisms at the single cell level. Using nanofocused scanning X-ray fluorescence microscopy, we quantify the spatial distribution of individual elements in subcellular compartments, including Fe, S, P, Zn, and Cu, in Plasmodium falciparum-infected (P. falciparum-infected) erythrocytes carrying the wild type or variant hemoglobins. Our data indicate that heterozygous hemoglobin S and C significantly modulate biochemical reactions in parasitized erythrocytes, such as aberrant hemozoin mineralization and a delay in hemoglobin degradation. The label-free scanning X-ray fluorescence imaging has great potential to quantify the spatial distribution of elements in subcellular compartments of P. falciparum-infected erythrocytes and unravel the biochemical mechanisms underpinning disease and protective traits.
Keyphrases
- plasmodium falciparum
- high resolution
- electron microscopy
- label free
- single molecule
- fluorescence imaging
- early onset
- wild type
- single cell
- red blood cell
- mass spectrometry
- dual energy
- high speed
- high throughput
- optical coherence tomography
- photodynamic therapy
- rna seq
- computed tomography
- electronic health record
- genome wide
- magnetic resonance imaging
- risk assessment
- dna methylation
- energy transfer
- quantum dots