C-type lectin-like receptor 2 specifies a functionally distinct subpopulation within phenotypically defined hematopoietic stem cell population that contribute to emergent megakaryopoiesis

C-type lectin-like receptor 2 (CLEC-2) expressed on megakaryocytes plays important roles in megakaryopoiesis. We found that CLEC-2 was expressed in about 20% of phenotypical long-term hematopoietic stem cells (LT-HSCs), which expressed lower levels of HSC-specific genes and produced larger amounts of megakaryocyte-related molecules than CLEC-2 low LT-HSCs. Although CLEC-2 high LT-HSCs had immature clonogenic activity, cultured CLEC-2 high LT-HSCs preferentially differentiated into megakaryocytes. CLEC-2 high HSCs yielded 6.8 times more megakaryocyte progenitors (MkPs) and 6.0 times more platelets 2 weeks and 1 week after transplantation compared with CLEC-2 low LT-HSCs. However, platelet yield from CLEC-2 high HSCs gradually declined with the loss of MkPs, while CLEC-2 low HSCs self-renewed long-term, indicating that CLEC-2 high LT-HSCs mainly contribute to early megakaryopoiesis. Treatment with pI:C and LPS increased the proportion of CLEC-2 high LT-HSCs within LT-HSCs. Almost all CLEC-2 low LT-HSCs were in the G0 phase and barely responded to pI:C. In contrast, 54% of CLEC-2 high LT-HSCs were in G0, and pI:C treatment obliged CLEC-2 high LT-HSCs to enter the cell cycle and differentiate into megakaryocytes, indicating that CLEC-2 high LT-HSCs are primed for cell cycle entry and rapidly yield platelets in response to inflammatory stress. In conclusion, CLEC-2 high LT-HSCs appear to act as a reserve for emergent platelet production under stress conditions.