![Schematic representation of SOCE activation in physiologic and pathologic megakaryopoiesis. In physiologic conditions (A), upon binding with TPO, c-Mpl promotes phosphorylation of downstream signaling molecules (STAT, AKT, ERK) together with IP3 formation and consequent mobilization of the IP3-sensitive Ca2+ pool. In Mks with repleted ER, STIM is localized in an inactive configuration in the ER membrane, and forms a complex with CALR and ERp57. Depletion of Ca2+ stores triggers Ca2+ release from the ER through IP3 receptors (IP3Rs) and consequent Ca2+ dissociation from STIM-CALR-ERp57 complex. Consequently, STIMs oligomerize and translocate next to the plasma membrane. Then, STIM binding to Orai and TRPC results in the opening of these channels and extracellular Ca2+ entry. The increased cytosolic Ca2+ concentration ([Ca2+]i) in turn sustains the long-lasting phosphorylation of c-Mpl downstream pathways. In pathologic conditions (B), the TPO-independent activation of c-Mpl by mutant CALR, which leaves the ER and consequently loses its binding to STIM and ERp57, leads to a constitutive activation of SOCE, which results in increased Mk proliferation.](https://ash.silverchair-cdn.com/ash/content_public/journal/blood/135/2/10.1182_blood.2019001103/2/bloodbld2019001103f7.png?Expires=1724855511&Signature=k6Y39Zx38-WW47std~srlfM5P-gfo2RS5IHlykgsgcD5WonjJau49yPCbHfIDjHIv6jUkQPvVpoisR-PK43w7OS0iY7-rSn4uQUNGjzgz~WteBZSfEdQtpncTBCxK-8xADh4JOWU9TUm7~2joS5BO0bOp~XIDHVqmxlVngJnGPlQQ9JZmooPmjmn~MmnEFaLuNuTYWoYPqIG~BqXBfGAd3m~sMAL8sBfFOBWyKiZgynjWEdjXDUo1uniHD7GbrRYHTKAOHsQGnRrtJdqYiM7eks~CDl5CM938m3-50vffKHWfYuuGV1dv3nSY3-ltMUPdnk56KnsgZe5i~X8VszFcw__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
Schematic representation of SOCE activation in physiologic and pathologic megakaryopoiesis. In physiologic conditions (A), upon binding with TPO, c-Mpl promotes phosphorylation of downstream signaling molecules (STAT, AKT, ERK) together with IP3 formation and consequent mobilization of the IP3-sensitive Ca2+ pool. In Mks with repleted ER, STIM is localized in an inactive configuration in the ER membrane, and forms a complex with CALR and ERp57. Depletion of Ca2+ stores triggers Ca2+ release from the ER through IP3 receptors (IP3Rs) and consequent Ca2+ dissociation from STIM-CALR-ERp57 complex. Consequently, STIMs oligomerize and translocate next to the plasma membrane. Then, STIM binding to Orai and TRPC results in the opening of these channels and extracellular Ca2+ entry. The increased cytosolic Ca2+ concentration ([Ca2+]i) in turn sustains the long-lasting phosphorylation of c-Mpl downstream pathways. In pathologic conditions (B), the TPO-independent activation of c-Mpl by mutant CALR, which leaves the ER and consequently loses its binding to STIM and ERp57, leads to a constitutive activation of SOCE, which results in increased Mk proliferation.