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Chromatin structure determines the sites of chromosome breakages in Plasmodium falciparum.

机译:染色质结构决定了恶性疟原虫中染色体断裂的位置。

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摘要

Spontaneous chromosome breakages are frequently observed in the human malaria parasite Plasmodium falciparum and are responsible for the generation of novel phenotypes, which may contribute to the pathogenicity and virulence of this protozoan parasite. The identification of a hot spot of chromosome breakage within the coding region of the KAHRP gene revealed that these events do not occur randomly but follow a regular pattern with a periodicity of 155 bp. This phasing corresponds to the average repeat unit of P. falciparum nucleosomes. Furthermore, breakage events preferentially occur within the linker regions of nucleosomes, as demonstrated by mapping endonuclease hypersensitive sites of chromatin. These data suggest that, in P. falciparum, the chromatin structure is involved in the molecular process of chromosome breakage, a mechanism that may be common in other eukaryotes.
机译:在人类疟原虫的恶性疟原虫中经常观察到自发染色体断裂,并导致新表型的产生,这可能导致这种原生动物寄生虫的致病性和致病性。在KAHRP基因的编码区域内的染色体断裂热点的鉴定表明,这些事件不是随机发生的,而是遵循规则模式,周期为155bp。该阶段对应于恶性疟原虫核小体的平均重复单元。此外,如定位染色质的核酸内切酶超敏位点所证明的,断裂事件优先发生在核小体的接头区域内。这些数据表明,在恶性疟原虫中,染色质结构参与了染色体断裂的分子过程,这是其他真核生物可能共有的机制。

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