(A) After malaria sporozoite entry into a hepatocyte, the parasite begins to grow inside a PV to a size larger than its original host cell. Schizogonic division results in the formation of thousands of erythrocyte-infective merozoites. During the final stage of differentiation, the PVM dissolves and allows the parasites to mix with the remaining host cell organelles. Eventually, the plasma membrane of the infected hepatocyte bulges out and forms merosomes; thus releasing merozoites, remnant bodies, and host cell mitochondria into the sinusoidal lumen. Camouflaged by host cell membrane, merosomes are not recognized by Kupffer cells and are shuttled out of the liver. Infiltration of the remains of the infected host cell by mononuclear phagocytes and neutrophil granulocytes gives rise to the formation of a small granuloma. Me, merosomes; RB, remnant bodies; Mi, host cell mitochondria; KC, Kupffer cells; M∅, mononuclear phagocytes; S, sporozoite.
(B) Shear forces inside the hepatic and other larger veins cause the merosomes to break down into smaller units. After passing through the right heart, these small merosomes are arrested inside lung capillaries where (1) they eventually release infectious merozoites into the pulmonary microvasculature; (2) local stagnation of the blood flow due to capillary occlusion by merosomes may result in dense erythrocyte packing; and thus (3) facilitate merozoite infection. ∗, alveolar space; H, hepatocyte; N, nucleus; E, endothelium; P-I, type I pneumocyte; P-II, type II pneumocyte; F, fibroblast; aM∅, alveolar macrophage; PMN, polymorphnuclear macrophage.