Secreted Mutant Calreticulins As Rogue Cytokines Trigger Thrombopoietin Receptor Activation Specifically in CALR Mutated Cells: Perspectives for MPN Therapy

Pecquet, Christian; Balligand, Thomas; Chachoua, Ilyas; Roy, Anita; Vertenoeil, Gaëlle; Colau, Didier; Fertig, Tudor Emanuel; Marty, Caroline; Nivarthi, Harini; Defour, Jean‐Philippe; Xu, Erica; Hug, Eva; Gisslinger, Heinz; Gisslinger, Bettina; Schalling, Martin; Casetti, Ilaria Carola; Rumi, Elisa; Pietra, Daniela; Cavalloni, Chiara; Arcaini, Luca; Cazzola, Mario; Komatsu, Norio; Kihara, Yoshihiko; Sunami, Yoshitaka; Edahiro, Yoko; Araki, Marito; Plo, Isabelle; Vainchenker, William; Královics, Róbert; Constantinescu, Stefan N.

doi:10.1182/blood-2018-99-118348

Cited by 29 publications

(26 citation statements)

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“…Data from independent laboratories have shown that mutant CALR protein requires MPL for signaling and factor-independent cell growth, and that the normal lectin domain of CALR is essential to bind glycosylated sites on MPL. [32][33][34] More recently, it was reported that both mutant and wild-type CALR proteins are present at higher levels in the plasma of myelofibrosis patients (compared to normal individuals), 35,36 and may function in a paracrine fashion by binding the extracellular domains of MPL to facilitate receptor dimerization. 34,36 However, the relative contribution of autocrine versus paracrine versus endosomal signaling of mutant CALR protein to aberrant activation of the JAK-STAT pathway in MPN has not been fully elucidated (Figure 1).…”

Section: Molecular Aspects Of Calr and Ruxolitinibmentioning

confidence: 99%

Persistence of myelofibrosis treated with ruxolitinib: biology and clinical implications

et al. 2021

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Activation of JAK-STAT signaling is one of the hallmarks of myelofibrosis, a myeloproliferative neoplasm that leads to inflammation, progressive bone marrow failure, and a risk of leukemic transformation. Around 90% of patients with myelofibrosis have a mutation in JAK2, MPL, or CALR: so-called ‘driver’ mutations that lead to activation of JAK2. Ruxolitinib, and other JAK2 inhibitors in clinical use, provide clinical benefit but do not have a major impact on the abnormal hematopoietic clone. This phenomenon is termed ‘persistence’, in contrast to usual patterns of resistance. Multiple groups have shown that type 1 inhibitors of JAK2, which bind the active conformation of the enzyme, lead to JAK2 becoming resistant to degradation with consequent accumulation of phospho-JAK2. In turn, this can lead to exacerbation of inflammatory manifestations when the JAK inhibitor is discontinued, and it may also contribute to disease persistence. The ways in which JAK2 V617F and CALR mutations lead to activation of JAK-STAT signaling are incompletely understood. We summarize what is known about pathological JAK-STAT activation in myelofibrosis and how this might lead to future novel therapies for myelofibrosis with greater disease-modifying potential.

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Section: Molecular Aspects Of Calr and Ruxolitinibmentioning

confidence: 99%

Persistence of myelofibrosis treated with ruxolitinib: biology and clinical implications

et al. 2021

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“…Interestingly, although CALR m has been shown to accumulate at the cell surface and be secreted, co-cultured and conditioned experiments did not detect MPL activation through secreted CALR m (39,41). However, a recent study using Nano-BRET and Nano-luciferase found that CALR m can act as a rogue cytokine and activate JAK-STAT signaling by binding in trans to surface MPL (50). Accordingly, CALR m is likely involved in MPL glycosylation and interacts with a specific form MPL during receptor maturation in the ER and in the Golgi apparatus, but not with the mature form.…”

Section: Calr Mutants' Role On Mpl Binding and Maturationmentioning

confidence: 99%

Unfolding the Role of Calreticulin in Myeloproliferative Neoplasm Pathogenesis

Merlinsky

Levine

Pronier

2019

Clinical Cancer Research

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In 2013, two seminal studies identified gain-of-function mutations in the Calreticulin (CALR) gene in a subset of JAK2/MPL-negative myeloproliferative neoplasm (MPN) patients. CALR is an endoplasmic reticulum (ER) chaperone protein that normally binds misfolded proteins in the ER and prevents their export to the Golgi and had never previously been reported mutated in cancer or to be asso-ciated with hematologic disorders. Further investigation determined that mutated CALR is able to achieve oncogenic transformation primarily through constitutive activation of the MPL-JAK-STAT signaling axis. Here we review our current understanding of the role of CALR mutations in MPN pathogenesis and how these insights can lead to innovative therapeutics approaches.

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“…This new C-terminal sequence is rich in positively charged amino acids and, unlike unmutated CALR (which is located in the cytoplasm), these unique CALR -mutated peptides are transported to the cellular membrane and activate thrombopoietin receptor. They are even secreted and activate non-mutated cells, thus acting as the roque cytokines [43,44].…”

Section: Mutational Landscape Of Mpnmentioning

confidence: 99%

Experimental Modeling of Myeloproliferative Neoplasms

Lanikova

Babošová

Prchal

2019

Genes

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Myeloproliferative neoplasms (MPN) are genetically very complex and heterogeneous diseases in which the acquisition of a somatic driver mutation triggers three main myeloid cytokine receptors, and phenotypically expresses as polycythemia vera (PV), essential thrombocytosis (ET), and primary myelofibrosis (PMF). The course of the diseases may be influenced by germline predispositions, modifying mutations, their order of acquisition and environmental factors such as aging and inflammation. Deciphering these contributory elements, their mutual interrelationships, and their contribution to MPN pathogenesis brings important insights into the diseases. Animal models (mainly mouse and zebrafish) have already significantly contributed to understanding the role of several acquired and germline mutations in MPN oncogenic signaling. Novel technologies such as induced pluripotent stem cells (iPSCs) and precise genome editing (using CRISPR/Cas9) contribute to the emerging understanding of MPN pathogenesis and clonal architecture, and form a convenient platform for evaluating drug efficacy. In this overview, the genetic landscape of MPN is briefly described, with an attempt to cover the main discoveries of the last 15 years. Mouse and zebrafish models of the driver mutations are discussed and followed by a review of recent progress in modeling MPN with patient-derived iPSCs and CRISPR/Cas9 gene editing.

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Secreted Mutant Calreticulins As Rogue Cytokines Trigger Thrombopoietin Receptor Activation Specifically in CALR Mutated Cells: Perspectives for MPN Therapy

Cited by 29 publications

References 0 publications

Persistence of myelofibrosis treated with ruxolitinib: biology and clinical implications

Persistence of myelofibrosis treated with ruxolitinib: biology and clinical implications

Unfolding the Role of Calreticulin in Myeloproliferative Neoplasm Pathogenesis

Experimental Modeling of Myeloproliferative Neoplasms

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