Tyler Parsons scite author profile

Tyler Parsons

4Publications

32Citation Statements Received

49Citation Statements Given

How they've been cited

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191

Affiliations

Washington University in St. Louis, Oakland University, Beaumont Health

Publications

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Integrin α6 (CD49f), The Microenvironment and Cancer Stem Cells

Bigoni-Ordóñez

Czarnowski

Parsons

et al. 2019

CSCR

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Cancer is a highly prevalent and potentially terminal disease that affects millions of individuals worldwide. Here, we review the literature exploring the intricacies of stem cells bearing tumorigenic characteristics and collect evidence demonstrating the importance of integrin α6 (ITGA6, also known as CD49f) in cancer stem cell (CSC) activity. ITGA6 is commonly used to identify CSC populations in various tissues and plays an important role sustaining the self-renewal of CSCs by interconnecting them with the tumorigenic microenvironment.

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Effect of Clonal Hematopoiesis on Cardiovascular Disease in People Living with HIV

Wiley¹,

Parsons²,

Burkart³

et al. 2022

Experimental Hematology

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Intratumoural haematopoietic stem and progenitor cell differentiation into M2 macrophages facilitates the regrowth of solid tumours after radiation therapy

et al. 2021

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KDM6B protects T-ALL cells from NOTCH1-induced oncogenic stress

et al. 2023

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T-cell acute lymphoblastic leukemia (T-ALL) is an aggressive hematopoietic neoplasm resulting from the malignant transformation of T-cell progenitors. While activating NOTCH1 mutations are the dominant genetic drivers of T-ALL, epigenetic dysfunction plays a central role in the pathology of T-ALL and can provide alternative mechanisms to oncogenesis in lieu of or in combination with genetic mutations. The histone demethylase enzyme KDM6A (UTX) is also recurrently mutated in T-ALL patients and functions as a tumor suppressor. However, its gene paralog, KDM6B (JMJD3), is never mutated and can be significantly overexpressed, suggesting it may be necessary for sustaining the disease. Here, we used mouse and human T-ALL models to show that KDM6B is required for T-ALL development and maintenance. Using NOTCH1 gain-offunction retroviral models, mouse cells genetically deficient for Kdm6b were unable to propagate T-ALL. Inactivating KDM6B in human T-ALL patient cells by CRISPR/Cas9 showed KDM6Btargeted cells were significantly outcompeted over time. The dependence of T-ALL cells on KDM6B was proportional to the oncogenic strength of NOTCH1 mutation, with KDM6B required to prevent stress-induced apoptosis from strong NOTCH1 signaling. These studies identify a crucial role for KDM6B in sustaining NOTCH1-driven T-ALL and implicate KDM6B as a novel therapeutic target in these patients.

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Tyler Parsons

Integrin α6 (CD49f), The Microenvironment and Cancer Stem Cells

Effect of Clonal Hematopoiesis on Cardiovascular Disease in People Living with HIV

Intratumoural haematopoietic stem and progenitor cell differentiation into M2 macrophages facilitates the regrowth of solid tumours after radiation therapy

KDM6B protects T-ALL cells from NOTCH1-induced oncogenic stress

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