Ryan Corces, PhD

Assistant Professor

Neurology

Research Description

The Corces Lab studies the gene-regulatory underpinnings of neurodegenerative disease. We utilize broad epigenomic and transcriptomic profiling of primary human disease tissue to generate hypotheses about the cell types and molecular mechanisms driving neurodegeneration. We then test these hypotheses using in vitro and murine model systems through large-scale screens (CRISPR / MPRA) and targeted molecular perturbation.

Current Projects

Pathologic Resilience in AD
AD is associated with the accumulation of beta-amyloid into plaques and hyperphosphorylated tau into neurofibrillary tangles. Though the precise mechanisms are still debated, these two pathologic changes are widely regarded as drivers of neuronal dysfunction and subsequent cognitive decline. In most cases, the burden of AD-related pathology correlates with the degree of cognitive decline. However, some individuals appear to be resilient to increased AD-related pathology, maintaining unperturbed cognitive function for years. We are interested in understanding (i) if this resilient state truly exists or if these individuals would eventually develop AD-related cognitive impairment, and (ii) if resilience truly exists, how is this resilience genetically and epigenetically encoded. Ultimately, we hope to identify how certain individuals of advanced age avoid cognitive decline and use this understanding to increase resilience across more vulnerable patients.

Selective Vulnerability in AD
In addition to the cognitive resilience to pathology mentioned above, AD is also characterized by “selective vulnerability” – the disease only affects particular neurons and exhibits consistent differential effects on different brain regions. Moreover, this selective vulnerability exists across multiple diverse neurodegenerative diseases, though the neuronal types affected by the pathology differ across diseases. In most cases, the cells that accumulate the pathology-associated proteins are the cells that are most affected. However, many examples exist of neuronal cell types that accumulate pathology but remain relatively unaffected. Some studies indicate that this is a cell-autonomous property of the cells, implicated specific gene expression patterns in the selectivity of pathologic vulnerability. We are using single-cell approaches to characterize cell type- and brain region-specific differences to identify putative mechanisms underlying this selective vulnerability.

The role of inherited genetic variation in AD
Through decades of research, genome-wide association studies have identified heritable mutations that lead to an increased risk of developing AD. The vast majority (>95%) of these mutations occur in noncoding regions of the genome, making their functions difficult to predict. As such, many of these mutations remain under-characterized and their contribution to AD pathogenesis remains unclear. Moreover, it has become increasingly clear that an individual’s lifetime risk of developing AD is not merely governed by genetics. In addition, the epigenome, the complement of all of the chemical and physical modifications imposed on DNA that do not change the underlying sequence, is also thought to play a crucial role. We aim to define the epigenetic and genetic components of AD through profiling of the open chromatin landscapes and three-dimensional chromatin interactions in brain regions and primary cell types of patients with and without AD. We have integrated machine learning and single-cell epigenomics to predict functionality of many of these polymorphisms. Layering on single-cell transcriptomics, massively parallel reporter assays, and CRISPR-based perturbation of regulatory elements, we hope to uncover the mechanisms behind AD-associated genetic variation with the ultimate goal of identifying novel aspects of AD pathogenesis and nominating putative avenues for therapeutic intervention.

Parkinson’s Disease
The Corces Lab is also broadly interested in other neurodegenerative diseases including Parkinson’s disease (PD). PD is a progressive long-term neurodegenerative disorder that is classically associated with effects on the motor system (tremors, muscle rigidity, bradykinesia etc.). The primary cellular cause of these symptoms is the loss of dopamine-secreting neurons in the substantia nigra. Similar to the pathologic accumulations in AD, PD is characterized by the accumulation of alpha-synuclein protein in Lewy bodies. Many of the same questions and techniques that we apply to AD are also being applied to PD. We are particularly interested in the inherited genetic contributions to PD as our understanding of this remains much less mature.

Lab Members

Fiorella Grandi - Postdoctoral fellow

Hailey Modi - Research Associate

Superenhancer Analysis Defines Novel Epigenomic Subtypes of Non-APL AML, Including an RARa Dependency Targetable by SY-1425, a Potent and Selective RARa Agonist.

Ryan Corces, PhD

Lab Website

Single-cell mutational profiling enhances the clinical evaluation of AML MRD.

Single-cell multiomic analysis identifies regulatory programs in mixed-phenotype acute leukemia.

Circular ecDNA promotes accessible chromatin and high oncogene expression.

Massively parallel single-cell chromatin landscapes of human immune cell development and intratumoral T cell exhaustion.

HiChIRP reveals RNA-associated chromosome conformation.

Single-cell lineage tracing by endogenous mutations enriched in transposase accessible mitochondrial DNA.

The chromatin accessibility landscape of primary human cancers.

Integrated Single-Cell Analysis Maps the Continuous Regulatory Landscape of Human Hematopoietic Differentiation.

Transcript-indexed ATAC-seq for precision immune profiling.

Preleukemic Hematopoietic Stem Cells in Human Acute Myeloid Leukemia.

Rapid Chromatin Switch in the Direct Reprogramming of Fibroblasts to Neurons.

Enhancer connectome in primary human cells identifies target genes of disease-associated DNA elements.

An improved ATAC-seq protocol reduces background and enables interrogation of frozen tissues.

Superenhancer Analysis Defines Novel Epigenomic Subtypes of Non-APL AML, Including an RARa Dependency Targetable by SY-1425, a Potent and Selective RARa Agonist.

Human AML-iPSCs Reacquire Leukemic Properties after Differentiation and Model Clonal Variation of Disease.

Lineage-specific and single-cell chromatin accessibility charts human hematopoiesis and leukemia evolution.

A humanized bone marrow ossicle xenotransplantation model enables improved engraftment of healthy and leukemic human hematopoietic cells.

The three-dimensional cancer genome.

Leukemia-Associated Cohesin Mutants Dominantly Enforce Stem Cell Programs and Impair Human Hematopoietic Progenitor Differentiation.

Isocitrate dehydrogenase 1 and 2 mutations induce BCL-2 dependence in acute myeloid leukemia.

Mutant WT1 is associated with DNA hypermethylation of PRC2 targets in AML and responds to EZH2 inhibition.

Pre-leukemic evolution of hematopoietic stem cells: the importance of early mutations in leukemogenesis.

Preleukemic mutations in human acute myeloid leukemia affect epigenetic regulators and persist in remission.

Clonal evolution of preleukemic hematopoietic stem cells precedes human acute myeloid leukemia.

A long noncoding RNA maintains active chromatin to coordinate homeotic gene expression.

Insulin signaling and dietary restriction differentially influence the decline of learning and memory with age.

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Ryan Corces, PhD

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