Dynamins 2 and 3 control the migration of human megakaryocytes by regulating CXCR4 surface expression and ITGB1 activity

Suraneni, Praveen; Corey, Seth J.; Hession, Michael; Ishaq, Rameez; Awomolo, Arinola; Hasan, Shirin; Shah, Chirag; Liu, Hui; Wickrema, Amittha; Debili, Najet; Crispino, John D.; Eklund, Elizabeth A.; Chen, Yolande

doi:10.1182/bloodadvances.2018021923

Cited by 13 publications

(23 citation statements)

References 95 publications

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“…Furthermore, CXCR4 high MDICs egressed into circulation and infiltrated into peripheral organs, such as the liver, spleen, and lung. This is consistent with previous reports that MKs egress and migrate to the pulmonary capillary 12,37,93 , and CXCR4 navigates cell migration upon chemotactic stimuli 8,70 . HSCs like MK progenitors induce emergency megakaryopoiesis to generate mature MKs for platelet production 87 .…”

Section: Discussionsupporting

confidence: 93%

“…Moreover, we seldom observed CD41 + hematopoietic stem and progenitor cells (HSPCs) with a tighter gating strategy because of lower CD41 levels in HSCs, consistent with single-cell analysis showing rarely expressed HSC marker genes in MKs 65-68 (Supplemental Figure 1P, 2C). To assign the immune response and modulatory functionality to potential clusters, we identified surface protein and cytokinin encoded marker genes: Cdh1 (encoding CD324/E-cadherin) and Il6 enriched in MDICs (MK5), Ccr2 enriched in MK4 and MDICs (MK5), and high Cxcr4 expression in MDICs, compared to low Cxcr4 level in classic MKs 69,70 (Figure 1G and I). Single cells expressed a high level of Cxcr4 also enriched cell migration, immune-modulatory, and inflammatory response pathways (Supplemental Figure 1Q).…”

Section: Resultsmentioning

confidence: 99%

“…No reuse allowed without permission. Cxcr4 expression in MDICs, compared to low Cxcr4 level in classic MKs 69,70 (Figure 1G and I). Single cells expressed a high level of Cxcr4 also enriched cell migration, immunemodulatory, and inflammatory response pathways (Supplemental Figure 1Q).…”

Section: Mdics Migrate To Peripheral Organs Upon L Monocytogenes Infectionmentioning

confidence: 93%

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Megakaryocyte derived immune-stimulating cells regulate host-defense immunity against bacterial pathogens

Wang

Xie

Han

et al. 2021

Preprint

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Megakaryocytes (MKs) continuously produce platelets in bone marrow to support hemostasis. However, MKs also play roles beyond thrombopoiesis as they regulate hematopoietic stem cell quiescence and erythropoiesis, which suggests the functional heterogeneity of MKs. Here, using single-cell sequencing we identified an MK-derived immune-stimulating cell (MDIC) population, which plays an important role in host-protective response against bacteria. In contrast to platelet-generating MKs, MDICs highly express cell migration, immune-modulatory, and response genes. Upon Listeria (L.) monocytogenes infection, MDICs egress to circulation and infiltrate into the spleen, liver and lung. MDICs interact with myeloid cells to promote their migration and tissue infiltration. More importantly, MDICs stimulate phagocytosis of macrophages and neutrophils by producing TNFα and IL-6 and facilitating antigen-specific T cell activation via IL-6 to enhance anti-bacterial response. Ablation of MKs reduced innate immune response and compromised T cell activation in spleen and liver, impairs the anti-bacterial effects in mice under L. monocytogenes challenge. Finally, infection-induced emergency megakaryopoiesis efficiently stimulated MDICs generation upon bacterial infection. Overall, we identify MDICs as a novel MK subpopulation, which regulates host-defense immune response against bacterial infection.

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Section: Discussionsupporting

confidence: 93%

Section: Resultsmentioning

confidence: 99%

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Megakaryocyte derived immune-stimulating cells regulate host-defense immunity against bacterial pathogens

Wang

Xie

Han

et al. 2021

Preprint

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“…6c, d). Importantly, the efficacy of Dynole 34-2 irrespective of activating mutations of growth factor-induced signalling could be explained by the importance of Dynamin for the CXCR4/CXCL12-mediated response to the microenvironment, which promotes survival of LSCs through the activation of the MAPK and AKT signalling pathways in acute leukemia 15,19,70 . Our data support previous reports confirming the efficacy of Dynole 34-2 to inhibit internalization of signalling receptors and downstream signal transduction in different malignancies 35,71 .…”

Section: Discussionmentioning

confidence: 99%

Small molecule inhibition of Dynamin-dependent endocytosis targets multiple niche signals and impairs leukemia stem cells

et al. 2020

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Intensive chemotherapy for acute leukemia can usually induce complete remission, but fails in many patients to eradicate the leukemia stem cells responsible for relapse. There is accumulating evidence that these relapse-inducing cells are maintained and protected by signals provided by the microenvironment. Thus, inhibition of niche signals is a proposed strategy to target leukemia stem cells but this requires knowledge of the critical signals and may be subject to compensatory mechanisms. Signals from the niche require receptor-mediated endocytosis, a generic process dependent on the Dynamin family of large GTPases. Here, we show that Dynole 34-2, a potent inhibitor of Dynamin GTPase activity, can block transduction of key signalling pathways and overcome chemoresistance of leukemia stem cells. Our results provide a significant conceptual advance in therapeutic strategies for acute leukemia that may be applicable to other malignancies in which signals from the niche are involved in disease progression and chemoresistance.

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“…These genes may regulate cell adhesion and migration (Deem and Cook‐Mills ; Suraneni et al . ), but the consequences of their expression changes in hypertension remain to be determined.…”

Section: Hypertension‐induced Cerebral Damage Mediated By Cns Pericytesmentioning

confidence: 99%

The role of pericytes in brain disorders: from the periphery to the brain

Hirunpattarasilp

Attwell

Freitas

2019

Journal of Neurochemistry

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It is becoming increasingly apparent that disorders of the brain microvasculature contribute to many neurological disorders. In recent years it has become clear that a major player in these events is the capillary pericyte which, in the brain, is now known to control the blood–brain barrier, regulate blood flow, influence immune cell entry and be crucial for angiogenesis. In this review we consider the under‐explored possibility that peripheral diseases which affect the microvasculature, such as hypertension, kidney disease and diabetes, produce central nervous system (CNS) dysfunction by mechanisms affecting capillary pericytes within the CNS. We highlight how cellular messengers produced peripherally can act via signalling pathways within CNS pericytes to reshape blood vessels, restrict blood flow or compromise blood–brain barrier function, thus causing neuronal dysfunction. Increased understanding of how renin–angiotensin, Rho‐kinase and PDGFRβ signalling affect CNS pericytes may suggest novel therapeutic approaches to reducing the CNS effects of peripheral disorders.

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Dynamins 2 and 3 control the migration of human megakaryocytes by regulating CXCR4 surface expression and ITGB1 activity

Cited by 13 publications

References 95 publications

Megakaryocyte derived immune-stimulating cells regulate host-defense immunity against bacterial pathogens

Megakaryocyte derived immune-stimulating cells regulate host-defense immunity against bacterial pathogens

Small molecule inhibition of Dynamin-dependent endocytosis targets multiple niche signals and impairs leukemia stem cells

The role of pericytes in brain disorders: from the periphery to the brain

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