Fig. 6.
Fig. 6. Defective erythropoiesis in MM. / Hypothetical model of the pathogenic defective maturation of erythroid cells by malignant cytotoxic plasma cells in active MM. GpA+dim erythroblasts progress to the GpA+bright form by GATA-1. At their prebasophilic/basophilic stage (GpA+dim), erythroblasts are highly susceptible to Fas stimulation because they can be negatively regulated by Fas-L from mature (GpA+bright) erythroblasts just as GpA+interm erythroblasts are restrained by TRAIL. Fas and the TRAIL receptors, namely, DR4/DR5 molecules, are expressed during erythroid differentiation, though they are not functional in specific stages (empty symbols). Highly malignant myeloma cells express large amounts of both Fas-L and TRAIL and exert a direct erythroblast cytotoxicity by inducing apoptosis. The cytotoxic mechanism operates during either the immature or the semimature stage of differentiation by both Fas and DR4/DR5. The cytoplasmic caspases activated by these apoptogen receptors induce the cleavage of GATA-1, whose intracellular defect promotes an arrest in the maturative progression. This results in a relative increase of immature erythroblasts and systematic impairment of the erythroid matrix.

Defective erythropoiesis in MM.

Hypothetical model of the pathogenic defective maturation of erythroid cells by malignant cytotoxic plasma cells in active MM. GpA+dim erythroblasts progress to the GpA+bright form by GATA-1. At their prebasophilic/basophilic stage (GpA+dim), erythroblasts are highly susceptible to Fas stimulation because they can be negatively regulated by Fas-L from mature (GpA+bright) erythroblasts just as GpA+interm erythroblasts are restrained by TRAIL. Fas and the TRAIL receptors, namely, DR4/DR5 molecules, are expressed during erythroid differentiation, though they are not functional in specific stages (empty symbols). Highly malignant myeloma cells express large amounts of both Fas-L and TRAIL and exert a direct erythroblast cytotoxicity by inducing apoptosis. The cytotoxic mechanism operates during either the immature or the semimature stage of differentiation by both Fas and DR4/DR5. The cytoplasmic caspases activated by these apoptogen receptors induce the cleavage of GATA-1, whose intracellular defect promotes an arrest in the maturative progression. This results in a relative increase of immature erythroblasts and systematic impairment of the erythroid matrix.

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