Publications by authors named "Kay Chung"
The metabolic landscape of cancer greatly influences antitumor immunity, yet it remains unclear how organ-specific metabolites in the tumor microenvironment influence immunosurveillance. We found that accumulation of primary conjugated and secondary bile acids (BAs) are metabolic features of human hepatocellular carcinoma and experimental liver cancer models. Inhibiting conjugated BA synthesis in hepatocytes through deletion of the BA-conjugating enzyme bile acid-CoA:amino acid -acyltransferase (BAAT) enhanced tumor-specific T cell responses, reduced tumor growth, and sensitized tumors to anti-programmed cell death protein 1 (anti-PD-1) immunotherapy.
View Article and Find Full Text PDFExhausted T cells (TEX) in cancer and chronic viral infections undergo metabolic and epigenetic remodeling, impairing their protective capabilities. However, the impact of nutrient metabolism on epigenetic modifications that control TEX differentiation remains unclear. We showed that TEX cells shifted from acetate to citrate metabolism by downregulating acetyl-CoA synthetase 2 (ACSS2) while maintaining ATP-citrate lyase (ACLY) activity.
View Article and Find Full Text PDFArticle Synopsis
- * Treatment with αCTLA-4 enhanced survival in a mouse model of glioblastoma, with this effect relying on the presence of CD4 T cells and their interaction with microglia.
- * CD4 T cells were found to activate microglia through IFNγ, leading to increased tumor suppression, indicating a critical CD4 T cell-microglia interaction for effective anti-tumor immunity.
Article Synopsis
- Transcription factors (TFs) play a crucial role in determining different T cell states, particularly in contexts like viral infections and cancer, leading to the creation of a detailed atlas of nine CD8 T cell differentiation states for predicting TF activity.
- The study highlights the functional contrast between terminally exhausted T cells (TEX), which are dysfunctional, and tissue-resident memory T cells (T), which provide protection, while emphasizing the challenges in selectively promoting the beneficial state without allowing TEX differentiation.
- Using techniques like CRISPR screening and single-cell RNA sequencing, researchers identified specific TFs linked to TEX state differentiation, discovered new TEX-specific TFs, and established potential targets for enhancing tumor control by improving T cell functionalities.
Although recent evidence demonstrates heterogeneity among CD8+ T cells during chronic infection, developmental relationships and mechanisms underlying their fate decisions remain incompletely understood. Using single-cell RNA and TCR sequencing, we traced the clonal expansion and differentiation of CD8+ T cells during chronic LCMV infection. We identified immense clonal and phenotypic diversity, including a subset termed intermediate cells.
View Article and Find Full Text PDFIn response to infection, T cells adopt a range of differentiation states, creating numerous heterogeneous subsets that exhibit different phenotypes, functions, and migration patterns. This T cell heterogeneity is a universal feature of T cell immunity, needed to effectively control pathogens in a context-dependent manner and generate long-lived immunity to those pathogens. Here, we review new insights into differentiation state dynamics and population heterogeneity of CD8+ T cells in acute and chronic viral infections and cancer and highlight the parallels and distinctions between acute and chronic antigen stimulation settings.
View Article and Find Full Text PDFCraniofacial asymmetry, mandibular condylar modeling and temporomandibular joint disorders are common comorbidities of skeletally disproportionate malocclusions, but etiology of occurrence together is poorly understood. We compared asymmetry, condyle modeling stability and temporomandibular health in a cohort of 128 patients having orthodontics and orthognathic surgery to correct dentofacial deformity malocclusions. We also compared ACTN3 and ENPP1 genotypes for association to clinical conditions.
View Article and Find Full Text PDFOn the cutting edge: protease-based methods for sensing and controlling cell biology.
Nat Methods
September 2020
Sequence-specific proteases have proven to be versatile building blocks for tools that report or control cellular function. Reporting methods link protease activity to biochemical signals, whereas control methods rely on engineering proteases to respond to exogenous inputs such as light or chemicals. In turn, proteases have inherent control abilities, as their native functions are to release, activate or destroy proteins by cleavage, with the irreversibility of proteolysis allowing sustained downstream effects.
View Article and Find Full Text PDFIntroduction: We investigated whether ACTN3, ENPP1, ESR1, PITX1, and PITX2 genes which contribute to sagittal and vertical malocclusions also contribute to facial asymmetries and temporomandibular disorders (TMD) before and after orthodontic and orthognathic surgery treatment.
Methods: One hundred seventy-four patients with a dentofacial deformity were diagnosed as symmetric or subdivided into 4 asymmetric groups according to posteroanterior cephalometric measurements. TMD examination diagnosis and jaw pain and function (JPF) questionnaires assessed the presence and severity of TMD.