Schematic representation of the (a) HSC, normal stem cell and (b) LIC, leukemia-initiating cell interactions with the microenvironment. Niches provide support for self-renewal, quiescence, homing, enfrafment, and proliferation. As shown, HSCs and LSC reside in the osteoblastic or vascular niche. HSCs and LSC interact with multiple cell types (OB, OC, EC, CAR, MSC) within the BM microenvironment. Although schematically represented separately, the endosteal, and vascular niches are physically and functionally mutually involved. Candidate niche mechanisms, which regulate HSC function are also shown, including Jagged/notch, SDF1/CXCR4, SCF/c-Kit signaling. LIC quiescence, survival, and expansion are influenced by receptor kinases, adhesive receptors and signaling via matrix mediated/bound chemokines and cytokines (IL6, G-CSF, GM-CSF, KIT L, NOTCH L). LIC may secrete substance like SCF, infiltrate the niches, and take advantage of the normal hemostatic process, which enhances self-renewal and proliferation. Growth factor and other adhesion receptors signals can be targeted to overcome chemoresistance. Oxygen level, higher in the vascular niche than the osteoblastic niche under hypoxia. LIC proliferation results in expansion of hypoxic niche. HSC: hematopoietic Stem Cell, OPN: osteopontin, LIC: leukemia-initiating Cell, N-Cad: N-Cadherin, OC: osteoclast, VLA-4: very late antigen 4, OB: osteoblast, VEGFR: vascular endothelial growth factor receptor, TB: trabecular bone, SDF1: stromal growth factor 1, SCF: stem cell factor, Ang1: angiopoietin 1, HA: hyaluronic acid, ECM: extracellular matrix.