Publications by authors named "Jason W Reeves"

In combination with cell-intrinsic properties, interactions in the tumor microenvironment modulate therapeutic response. We leveraged single-cell spatial transcriptomics to dissect the remodeling of multicellular neighborhoods and cell-cell interactions in human pancreatic cancer associated with neoadjuvant chemotherapy and radiotherapy. We developed spatially constrained optimal transport interaction analysis (SCOTIA), an optimal transport model with a cost function that includes both spatial distance and ligand-receptor gene expression.

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Article Synopsis
  • Scientists are trying to understand how immune cells are organized in human tumors, especially in lung cancer.
  • They found special areas called 'immunity hubs' in tumors that help attract T cells and can improve responses to a type of treatment called PD-1 blockade.
  • One important type of hub they discovered is called the 'stem-immunity hub,' which has a mix of special immune cells that work together in a way that can help fight the cancer better when patients get immunotherapy.
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In combination with cell intrinsic properties, interactions in the tumor microenvironment modulate therapeutic response. We leveraged high-plex single-cell spatial transcriptomics to dissect the remodeling of multicellular neighborhoods and cell-cell interactions in human pancreatic cancer associated with specific malignant subtypes and neoadjuvant chemotherapy/radiotherapy. We developed Spatially Constrained Optimal Transport Interaction Analysis (SCOTIA), an optimal transport model with a cost function that includes both spatial distance and ligand-receptor gene expression.

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The organization of immune cells in human tumors is not well understood. Immunogenic tumors harbor spatially-localized multicellular 'immunity hubs' defined by expression of the T cell-attracting chemokines and abundant T cells. Here, we examined immunity hubs in human pre-immunotherapy lung cancer specimens, and found that they were associated with beneficial responses to PD-1-blockade.

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  • Pancreatic ductal adenocarcinoma (PDAC) is a deadly cancer with limited treatment options, and current methods for understanding its molecular characteristics are inadequate.
  • Researchers used advanced techniques, including single-nucleus RNA sequencing and digital spatial profiling, to analyze 43 PDAC tumors, revealing key cellular subtypes and their interactions.
  • They identified new malignant cell programs linked to poor outcomes and established three distinct multicellular communities, providing insights that could improve patient stratification in clinical trials and guide targeted therapies.
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Anosmia, the loss of smell, is a common and often the sole symptom of COVID-19. The onset of the sequence of pathobiological events leading to olfactory dysfunction remains obscure. Here, we have developed a postmortem bedside surgical procedure to harvest endoscopically samples of respiratory and olfactory mucosae and whole olfactory bulbs.

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Breast cancer is a heterogenous disease with variability in tumor cells and in the surrounding tumor microenvironment (TME). Understanding the molecular diversity in breast cancer is critical for improving prediction of therapeutic response and prognostication. High-plex spatial profiling of tumors enables characterization of heterogeneity in the breast TME, which can holistically illuminate the biology of tumor growth, dissemination and, ultimately, response to therapy.

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Immune responses to cancer are highly variable, with mismatch repair-deficient (MMRd) tumors exhibiting more anti-tumor immunity than mismatch repair-proficient (MMRp) tumors. To understand the rules governing these varied responses, we transcriptionally profiled 371,223 cells from colorectal tumors and adjacent normal tissues of 28 MMRp and 34 MMRd individuals. Analysis of 88 cell subsets and their 204 associated gene expression programs revealed extensive transcriptional and spatial remodeling across tumors.

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Article Synopsis
  • The CD155/TIGIT axis plays a significant role in how tumors evade the immune system, specifically in conditions like pancreatic cancer, which is notoriously difficult to treat.
  • Research confirms that many pancreatic tumors have strong neoepitopes that could trigger an immune response, but T cells in these tumors show dysfunction similar to patients.
  • By modifying the CD155/TIGIT interaction, the study identifies a promising immunotherapy approach combining TIGIT/PD-1 co-blockade with CD40 agonism, which has shown strong anti-tumor effects and is ready for clinical trials.
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In less than nine months, the Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) killed over a million people, including >25,000 in New York City (NYC) alone. The COVID-19 pandemic caused by SARS-CoV-2 highlights clinical needs to detect infection, track strain evolution, and identify biomarkers of disease course. To address these challenges, we designed a fast (30-minute) colorimetric test (LAMP) for SARS-CoV-2 infection from naso/oropharyngeal swabs and a large-scale shotgun metatranscriptomics platform (total-RNA-seq) for host, viral, and microbial profiling.

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  • The study investigates how SARS-CoV-2 affects the lungs at different severity levels by analyzing autopsy samples from 24 patients who died from the virus.
  • It identifies two categories of patients: those with high viral loads showing strong immune responses and specific macrophage types, and those with low viral loads exhibiting varied responses and signs of lung recovery.
  • The research also highlights that the spatial distribution of the virus and immune responses within the lungs is heterogeneous, with different patterns of interferon response genes linked to virus presence.
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  • The study investigates the differences in immune response to immune checkpoint blockade (ICB) between cutaneous melanoma (CM) and uveal melanoma (UM) patients, focusing on metastases in the liver.
  • Researchers analyzed liver samples from both CM and UM patients, using various genomic, transcriptional, and protein-level techniques.
  • Findings revealed that while CM and UM share a melanoma lineage, they significantly differ in mutation profiles and immune markers, with CM showing higher PD-L1 expression and UM demonstrating a higher ratio of exhausted CD8 T cells, suggesting distinct mechanisms behind their responses to ICB.
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The relationship of SARS-CoV-2 lung infection and severity of pulmonary disease is not fully understood. We analyzed autopsy specimens from 24 patients who succumbed to SARS-CoV-2 infection using a combination of different RNA and protein analytical platforms to characterize inter- and intra- patient heterogeneity of pulmonary virus infection. There was a spectrum of high and low virus cases that was associated with duration of disease and activation of interferon pathway genes.

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Objective: Prior reports demonstrate that personalized medicine implementation in clinical care is lacking. Given the program focus at Duke University on personalized medicine, we assessed health care providers' perspectives on their preparation and educational needs to effectively integrate personalized medicine tools and applications into their clinical practices.

Methods: Data from 78 health care providers who participated in a larger study of personalized and precision medicine at Duke University were analyzed using Qualtrics (descriptive statistics).

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Unlabelled: In this age of personalized medicine, genetic and genomic testing is expected to become instrumental in health care delivery, but little is known about its actual implementation in clinical practice.

Methods: We surveyed Duke faculty and healthcare providers to examine the extent of genetic and genomic testing adoption. We assessed providers' use of genetic and genomic testing options and indications in clinical practice, providers' awareness of pharmacogenetic applications, and providers' opinions on returning research-generated genetic test results to participants.

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Human centromeres are multi-megabase regions of highly ordered arrays of alpha satellite DNA that are separated from chromosome arms by unordered alpha satellite monomers and other repetitive elements. Complexities in assembling such large repetitive regions have limited detailed studies of centromeric chromatin organization. However, a genomic map of the human X centromere has provided new opportunities to explore genomic architecture of a complex locus.

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Transformation of both prokaryotes and eukaryotes with single-stranded oligonucleotides can transfer sequence information from the oligonucleotide to the chromosome. We have studied this process using oligonucleotides that correct a -1 frameshift mutation in the LYS2 gene of Saccharomyces cerevisiae. We demonstrate that transformation by oligonucleotides occurs preferentially on the lagging strand of replication and is strongly inhibited by the mismatch-repair system.

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We have previously shown that recombination between 400-bp substrates containing only 4-bp differences, when present in an inverted repeat orientation, is suppressed by >20-fold in wild-type strains of S. cerevisiae. Among the genes involved in this suppression were three genes involved in mismatch repair--MSH2, MSH3, and MSH6--and one in nucleotide excision repair, RAD1.

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A TRP5-based reversion system that allows the rates of all possible base pair substitutions to be measured when the TRP5 locus is in both orientations relative to a defined origin of replication has been developed. This system should be useful for a wide variety of mutation and repair studies in yeast.

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