Calcium signaling in a low calcium environment

Abstract

Malaria parasites, Plasmodia, spend most of their asexual life cycle within red blood cells, where they proliferate and mature. The erythrocyte cytoplasm has very low [Ca²⁺] (2+ is usually incompatible with normal cell functions and survival. In the present work, we have tested the possibility that Plasmodia overcome the limitation posed by the erythrocyte intracellular environment through the maintenance of a high [Ca²⁺] within the parasitophorous vacuole (PV), the compartment formed during invasion and within which the parasites grow and divide. Thus, Plasmodia were allowed to invade erythrocytes in the presence of Ca²⁺ indicator dyes. This allowed selective loading of the Ca²⁺ probes within the PV. The [Ca²⁺] within this compartment was found to be ∼40 μM, i.e., high enough to be compatible with a normal loading of the Plasmodia intracellular Ca²⁺ stores, a prerequisite for the use of a Ca²⁺-based signaling mechanism. We also show that reduction of extracellular [Ca²⁺] results in a slow depletion of the [Ca²⁺] within the PV. A transient drop of [Ca²⁺] in the PV for a period as short as 2 h affects the maturation process of the parasites within the erythrocytes, with a major reduction 48 h later in the percentage of schizonts, the form that re-invades the red blood cells.