Figure 1.
Stem cell model of normal and malignant hematopoiesis. Hematopoietic stem cells (HSCs) are capable of self-renewal (semicircular arrow) and reside at the apex of healthy polyclonal hematopoiesis (black). The acquisition of mutations in HSCs (m1) can create preleukemic HSCs (pHSCs; purple) that can drive clonal hematopoiesis (shaded purple). Clonal evolution through additional mutation acquisition (m2, 3, …x) or other molecular processes can further transform pHSCs into LSCs (red). These LSCs reside at the apex of the AML cellular hierarchy and are capable of (re)generating frank leukemia (brown).

Stem cell model of normal and malignant hematopoiesis. Hematopoietic stem cells (HSCs) are capable of self-renewal (semicircular arrow) and reside at the apex of healthy polyclonal hematopoiesis (black). The acquisition of mutations in HSCs (m1) can create preleukemic HSCs (pHSCs; purple) that can drive clonal hematopoiesis (shaded purple). Clonal evolution through additional mutation acquisition (m2, 3, …x) or other molecular processes can further transform pHSCs into LSCs (red). These LSCs reside at the apex of the AML cellular hierarchy and are capable of (re)generating frank leukemia (brown).

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