UASOM Faculty Profiles


Name	DANIEL J TYRRELL
Campus Address	PBMR 504 Zip 0000
Phone	(205) 975-0088
E-mail	dtyrrell@uab.edu
Other websites	Tyrrell Lab Scholars

Appointment Type

Department

Division

Rank

Primary

Joint Pathology

Molecular & Cellular Pathology

Assistant Professor

Center

Comprehensive Neuroscience Center

Assistant Professor

Center

Ctr for Clinical & Translational Sci

Assistant Professor

Center

Evelyn F. McKnight Brain Institute

Assistant Professor

Center

UAB Immunology Institute

Assistant Professor

My laboratory is interested in understanding how the blood-brain barrier changes during aging. Breakdown of the blood-brain-barrier impairs leads to a poor neurovascular microenvironment and ultimately impairs cognitive function and can contribute to neurodegeneration. We aim to uncover mechanisms of vascular aging that may contribute to blood-brain barrier breakdown. Much of our previous findings have been related to alteration in mitochondrial function and inflammation within cerebrovascular vessels. We are also interested in exploring how CD8 T cells may take advantage of the leakier blood-brain-barrier with aging to infiltrate the brain and contribute to neurodegeneration. T cell populations change dramatically during aging with a significant reduction in naive T cell output due to age-associated thymic involution. Some populations of effector and memory T cells also increase with aging. Many of these populations also demonstrate greater levels of exhaustion and senescence with aging. Taken together, the age-associated changes in CD8 T cells appear to contribute to a variety of diseases. We are interested in exploring their role in neurodegenerative diseases. We primarily use murine models along with genetic and surgical manipulations. The major experiments we perform in the laboratory are immunohistochemistry, histology, flow cytometry, immunoblot, and single-cell RNA sequencing approaches.

Title

Description
My laboratory is interested in understanding how the blood-brain barrier changes during aging. Breakdown of the blood-brain-barrier impairs leads to a poor neurovascular microenvironment and ultimately impairs cognitive function and can contribute to neurodegeneration. We aim to uncover mechanisms of vascular aging that may contribute to blood-brain barrier breakdown. Much of our previous findings have been related to alteration in mitochondrial function and inflammation within cerebrovascular vessels. We are also interested in exploring how CD8 T cells may take advantage of the leakier blood-brain-barrier with aging to infiltrate the brain and contribute to neurodegeneration. T cell populations change dramatically during aging with a significant reduction in naive T cell output due to age-associated thymic involution. Some populations of effector and memory T cells also increase with aging. Many of these populations also demonstrate greater levels of exhaustion and senescence with aging. Taken together, the age-associated changes in CD8 T cells appear to contribute to a variety of diseases. We are interested in exploring their role in neurodegenerative diseases. We primarily use murine models along with genetic and surgical manipulations. The major experiments we perform in the laboratory are immunohistochemistry, histology, flow cytometry, immunoblot, and single-cell RNA sequencing approaches.