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表面面积损失和球形度增加导致疟原虫环状感染红细胞亚群的脾脏捕获。

Surface area loss and increased sphericity account for the splenic entrapment of subpopulations of Plasmodium falciparum ring-infected erythrocytes.

机构信息

Institut Pasteur, Immunologie Moléculaire des Parasites, Département de Parasitologie Mycologie, Paris, France.

出版信息

PLoS One. 2013;8(3):e60150. doi: 10.1371/journal.pone.0060150. Epub 2013 Mar 28.

Abstract

Ex vivo perfusion of human spleens revealed innate retention of numerous cultured Plasmodium falciparum ring-infected red blood cells (ring-iRBCs). Ring-iRBC retention was confirmed by a microsphiltration device, a microbead-based technology that mimics the mechanical filtering function of the human spleen. However, the cellular alterations underpinning this retention remain unclear. Here, we use ImageStream technology to analyze infected RBCs' morphology and cell dimensions before and after fractionation with microsphiltration. Compared to fresh normal RBCs, the mean cell membrane surface area loss of trophozoite-iRBCs, ring-iRBCs and uninfected co-cultured RBCs (uRBCs) was 14.2% (range: 8.3-21.9%), 9.6% (7.3-12.2%) and 3.7% (0-8.4), respectively. Microsphilters retained 100%, ∼50% and 4% of trophozoite-iRBCs, ring-iRBCs and uRBCs, respectively. Retained ring-iRBCs display reduced surface area values (estimated mean, range: 17%, 15-18%), similar to the previously shown threshold of surface-deficient RBCs retention in the human spleen (surface area loss: >18%). By contrast, ring-iRBCs that successfully traversed microsphilters had minimal surface area loss and normal sphericity, suggesting that these parameters are determinants of their retention. To confirm this hypothesis, fresh normal RBCs were exposed to lysophosphatidylcholine to induce a controlled loss of surface area. This resulted in a dose-dependent retention in microsphilters, with complete retention occurring for RBCs displaying >14% surface area loss. Taken together, these data demonstrate that surface area loss and resultant increased sphericity drive ring-iRBC retention in microsphilters, and contribute to splenic entrapment of a subpopulation of ring-iRBCs. These findings trigger more interest in malaria research fields, including modeling of infection kinetics, estimation of parasite load, and analysis of risk factors for severe clinical forms. The determination of the threshold of splenic retention of ring-iRBCs has significant implications for diagnosis (spleen functionality) and drug treatment (screening of adjuvant therapy targeting ring-iRBCs).

摘要

对人类脾脏进行的离体灌注实验显示,大量培养的恶性疟原虫环状感染红细胞(环状 iRBC)会被先天保留。环状 iRBC 的保留通过微孔过滤装置得到了确认,该装置使用基于微珠的技术模拟了人体脾脏的机械过滤功能。然而,支持这种保留的细胞变化仍然不清楚。在这里,我们使用 ImageStream 技术在与微孔过滤分离之前和之后分析感染 RBC 的形态和细胞尺寸。与新鲜正常 RBC 相比,滋养体-iRBC、环状 iRBC 和未感染共培养 RBC(uRBC)的平均细胞膜表面积损失分别为 14.2%(范围:8.3-21.9%)、9.6%(7.3-12.2%)和 3.7%(0-8.4%)。微孔过滤器分别保留了 100%、约 50%和 4%的滋养体-iRBC、环状 iRBC 和 uRBC。保留的环状 iRBC 显示出降低的表面积值(估计平均值,范围:17%,15-18%),类似于先前在人体脾脏中观察到的表面缺陷 RBC 保留的阈值(表面积损失:>18%)。相比之下,成功穿过微孔过滤器的环状 iRBC 的表面积损失极小,且形态为球形,这表明这些参数是它们被保留的决定因素。为了证实这一假设,我们用溶血磷脂酰胆碱处理新鲜正常 RBC 以诱导可控的表面积损失。这导致了在微孔过滤器中的剂量依赖性保留,对于显示 >14%表面积损失的 RBC 完全保留。综上所述,这些数据表明表面积损失和由此产生的球形度增加导致了环状 iRBC 在微孔过滤器中的保留,并有助于微球体对环状 iRBC 亚群的捕获。这些发现引发了人们对疟疾研究领域的更多兴趣,包括感染动力学模型的建立、寄生虫负荷的估计以及严重临床形式的风险因素分析。确定环状 iRBC 在脾脏中的保留阈值对诊断(脾脏功能)和药物治疗(针对环状 iRBC 的辅助治疗筛选)具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5ff9/3610737/5f70675355cd/pone.0060150.g001.jpg

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