Your search keyword '"Lucas T Jennelle"' showing total 14 results

1. Modeling the effect of prolonged ethanol exposure on global gene expression and chromatin accessibility in normal 3D colon organoids.

Author

Matthew Devall, Lucas T Jennelle, Jennifer Bryant, Stephanie Bien, Ulrike Peters, Steven Powell, and Graham Casey

Subjects

Medicine, Science

Abstract

In this study we aimed to explore the potential biological effect of ethanol exposure on healthy colon epithelial cells using normal human colon 3D organoid "mini-gut" cultures. In numerous published studies ethanol use has been shown to be an environmental risk factor for colorectal cancer (CRC) development; however, the influence of ethanol exposure on normal colon epithelial cell biology remains poorly understood. We investigated the potential molecular effects of ethanol exposure in normal colon 3D organoids in a small pilot study (n = 3) using RNA-seq and ATAC-seq. We identify 1965 differentially expressed genes and 2217 differentially accessible regions of chromatin in response to ethanol treatment. Further, by cross-referencing our results with previously published analysis in colorectal cancer cell lines, we have not only validated a number of reported differentially expressed genes, but also identified several novel candidates for future investigation. In summary, our data highlights the potential importance for the use of normal colon 3D organoid models as a novel tool for the investigation of the relationship between the effects of environmental risk factors associated with colorectal cancer and the molecular mechanisms through which they confer this risk.

Published

2020

2. Ethanol exposure drives colon location specific cell composition changes in a normal colon crypt 3D organoid model

Author

Matthew Devall, Sarah J. Plummer, Jennifer Bryant, Lucas T. Jennelle, Stephen Eaton, Christopher H. Dampier, Jeroen R. Huyghe, Ulrike Peters, Steven M. Powell, and Graham Casey

Subjects

Medicine, Science

Abstract

Abstract Alcohol is a consistently identified risk factor for colon cancer. However, the molecular mechanism underlying its effect on normal colon crypt cells remains poorly understood. We employed RNA-sequencing to asses transcriptomic response to ethanol exposure (0.2% vol:vol) in 3D organoid lines derived from healthy colon (n = 34). Paired regression analysis identified 2,162 differentially expressed genes in response to ethanol. When stratified by colon location, a far greater number of differentially expressed genes were identified in organoids derived from the left versus right colon, many of which corresponded to cell-type specific markers. To test the hypothesis that the effects of ethanol treatment on colon organoid populations were in part due to differential cell composition, we incorporated external single cell RNA-sequencing data from normal colon biopsies to estimate cellular proportions following single cell deconvolution. We inferred cell-type-specific changes, and observed an increase in transit amplifying cells following ethanol exposure that was greater in organoids from the left than right colon, with a concomitant decrease in more differentiated cells. If this occurs in the colon following alcohol consumption, this would lead to an increased zone of cells in the lower crypt where conditions are optimal for cell division and the potential to develop mutations.

Published

2021

3. Supplementary Figure from Transcriptome-wide In Vitro Effects of Aspirin on Patient-derived Normal Colon Organoids

Author

Graham Casey, Ulrike Peters, Andrew T. Chan, Steven M. Powell, Victor Moreno, Ömer H. Yilmaz, Mourad W. Ali, Lucas T. Jennelle, Oliver Takacsi-Nagy, Dylan C. Zerjav, Dmitriy Kedrin, Jiancheng Mo, Virginia Díez-Obrero, Jennifer Bryant, Stephen Eaton, Sarah J. Plummer, Christopher H. Dampier, David A. Drew, and Matthew A.M. Devall

Abstract

Supplementary Figure from Transcriptome-wide In Vitro Effects of Aspirin on Patient-derived Normal Colon Organoids

Published

2023

4. Supplementary Data from Transcriptome-wide In Vitro Effects of Aspirin on Patient-derived Normal Colon Organoids

Author

Graham Casey, Ulrike Peters, Andrew T. Chan, Steven M. Powell, Victor Moreno, Ömer H. Yilmaz, Mourad W. Ali, Lucas T. Jennelle, Oliver Takacsi-Nagy, Dylan C. Zerjav, Dmitriy Kedrin, Jiancheng Mo, Virginia Díez-Obrero, Jennifer Bryant, Stephen Eaton, Sarah J. Plummer, Christopher H. Dampier, David A. Drew, and Matthew A.M. Devall

Abstract

Supplementary Data from Transcriptome-wide In Vitro Effects of Aspirin on Patient-derived Normal Colon Organoids

Published

2023

5. Transcriptome-wide In Vitro Effects of Aspirin on Patient-derived Normal Colon Organoids

Author

Christopher H. Dampier, Matthew Devall, Sarah J. Plummer, Mourad Wagdy Ali, David A. Drew, Dylan C Zerjav, Steven M. Powell, Jiancheng Mo, Victor Moreno, Ulrike Peters, Oliver Takacsi-Nagy, Graham Casey, Andrew T. Chan, Ömer H. Yilmaz, Stephen Eaton, Virginia Díez-Obrero, Lucas T. Jennelle, Jennifer Bryant, and Dmitriy Kedrin

Subjects

Cancer Research, education.field_of_study, Aspirin, business.industry, Colorectal cancer, Population, Wnt signaling pathway, medicine.disease, In vitro, Epithelium, Transcriptome, medicine.anatomical_structure, Oncology, medicine, Cancer research, Organoid, education, business, medicine.drug

Abstract

Mechanisms underlying aspirin chemoprevention of colorectal cancer remain unclear. Prior studies have been limited because of the inability of preclinical models to recapitulate human normal colon epithelium or cellular heterogeneity present in mucosal biopsies. To overcome some of these obstacles, we performed in vitro aspirin treatment of colon organoids derived from normal mucosal biopsies to reveal transcriptional networks relevant to aspirin chemoprevention. Colon organoids derived from 38 healthy individuals undergoing endoscopy were treated with 50 μmol/L aspirin or vehicle control for 72 hours and subjected to bulk RNA sequencing. Paired regression analysis using DESeq2 identified differentially expressed genes (DEG) associated with aspirin treatment. Cellular composition was determined using CIBERSORTx. Aspirin treatment was associated with 1,154 significant (q < 0.10) DEGs prior to deconvolution. We provide replication of these findings in an independent population-based RNA-sequencing dataset of mucosal biopsies (BarcUVa-Seq), where a significant enrichment for overlap of DEGs was observed (P < 2.2E−16). Single-cell deconvolution revealed changes in cell composition, including a decrease in transit-amplifying cells following aspirin treatment (P = 0.01). Following deconvolution, DEGs included novel putative targets for aspirin such as TRABD2A (q = 0.055), a negative regulator of Wnt signaling. Weighted gene co-expression network analysis identified 12 significant modules, including two that contained hubs for EGFR and PTGES2, the latter being previously implicated in aspirin chemoprevention. In summary, aspirin treatment of patient-derived colon organoids using physiologically relevant doses resulted in transcriptome-wide changes that reveal altered cell composition and improved understanding of transcriptional pathways, providing novel insight into its chemopreventive properties. Prevention Relevance: Numerous studies have highlighted a role for aspirin in colorectal cancer chemoprevention, though the mechanisms driving this association remain unclear. We addressed this by showing that aspirin treatment of normal colon organoids diminished the transit-amplifying cell population, inhibited prostaglandin synthesis, and dysregulated expression of novel genes implicated in colon tumorigenesis.

Published

2021

6. Hepatitis C Virus Alters Macrophage Cholesterol Metabolism Through Interaction with Scavenger Receptors

Author

Lucas T. Jennelle, Tshifhiwa Magoro, Angelina R. Angelucci, Aditya Dandekar, and Young S. Hahn

Subjects

Inflammation, Receptors, Scavenger, Macrophages, Immunology, Original Articles, Hepacivirus, Hepatitis C, Chronic, Lipid Metabolism, Hepatitis C, Fatty Liver, Cholesterol, Virology, Molecular Medicine, Humans, RNA, Inflammation Mediators

Abstract

Lipid accumulation and inflammation act together to induce, sustain, and further development of chronic liver disease. Hepatitis C virus (HCV) infection induces metabolic and immune changes in liver macrophages, promoting lipid accumulation and inflammation that synergize and culminate in the development of steatohepatitis and fibrogenesis. Chronic HCV patients have increased liver macrophages with disruptions in cholesterol metabolism and alterations in inflammatory mediators. While HCV-induced changes in inflammatory mediators are well documented, how HCV triggers metabolic change in macrophages is unknown. In this report, we examined the mechanism of macrophage sensing of HCV to cause metabolic impairment and subsequent immune dysfunction. We demonstrate that HCV protein and RNA kinetics in macrophages are distinct from hepatocytes. In macrophages, HCV RNAs and protein accumulate rapidly after exposure but internalized RNAs quickly decline to a low-level set point. Notably, exposure of macrophages to HCV resulted in increased lipids and cholesterol and activation of cholesterol-sensing, immunomodulatory liver X receptors (LXRs). Furthermore, we provide evidence that HCV RNA accumulation in macrophages occurs through scavenging receptors. These results suggest that HCV released from infected hepatocytes stimulates accumulation of lipids and activation of LXR in macrophages contributing to metabolic changes involved in HCV-induced chronic liver disease. Our results provide novel insight into mechanisms through which impaired lipid metabolism in macrophages associated with HCV infection promotes development of liver steatohepatitis and fibrosis.

Published

2022

7. IL-1β/TNF-α/IL-6 inflammatory cytokines promote STAT1-dependent induction of CH25H in Zika virus–infected human macrophages

Author

Aditya Dandekar, Tshifhiwa Magoro, Angelina R. Angelucci, Young S. Hahn, Gabriel Lipkowitz, Lucas T. Jennelle, Rohan Bajaj, and Pascal O. Bessong

Subjects

0301 basic medicine, Interleukin-1beta, Immunology, Virus Replication, Antiviral Agents, Biochemistry, Gene Expression Regulation, Enzymologic, Virus, Proinflammatory cytokine, Zika virus, 03 medical and health sciences, Interferon, medicine, Humans, STAT1, Molecular Biology, Transcription factor, Inflammation, Activating Transcription Factor 3, 030102 biochemistry & molecular biology, biology, Interleukin-6, Tumor Necrosis Factor-alpha, Zika Virus Infection, Macrophages, Toll-Like Receptors, Zika Virus, Cell Biology, biology.organism_classification, Virology, DNA-Binding Proteins, Flavivirus, STAT1 Transcription Factor, 030104 developmental biology, Interferon Type I, Steroid Hydroxylases, biology.protein, Cytokines, Tumor necrosis factor alpha, medicine.drug

Abstract

Zika virus (ZIKV)(3) is an enveloped, single-stranded, positive-sense RNA virus of the Flaviviridae family that has emerged as a public health threat because of its global transmission and link to microcephaly. Currently there is no vaccine for this virus. Conversion of cholesterol to 25-hydroxycholesterol by cholesterol 25-hydroxylase (CH25H) has been shown to have broad antiviral properties. However, the molecular basis of induction of CH25H in humans is not known. Elucidation of signaling and transcriptional events for induction of CH25H expression is critical for designing therapeutic antiviral agents. In this study, we show that CH25H is induced by ZIKV infection or Toll-like receptor stimulation. Interestingly, CH25H is induced by pro-inflammatory cytokines, including IL-1β, tumor necrosis factor α, and IL-6, and this induction depends on the STAT1 transcription factor. Additionally, we observed that cAMP-dependent transcription factor (ATF3) weakly binds to the CH25H promoter, suggesting cooperation with STAT1. However, ZIKV-induced CH25H was independent of type I interferon. These findings provide important information for understanding how the Zika virus induces innate inflammatory responses and promotes the expression of anti-viral CH25H protein.

Published

2019

8. Transcriptome-wide

Author

Matthew A M, Devall, David A, Drew, Christopher H, Dampier, Sarah J, Plummer, Stephen, Eaton, Jennifer, Bryant, Virginia, Díez-Obrero, Jiancheng, Mo, Dmitriy, Kedrin, Dylan C, Zerjav, Oliver, Takacsi-Nagy, Lucas T, Jennelle, Mourad W, Ali, Ömer H, Yilmaz, Victor, Moreno, Steven M, Powell, Andrew T, Chan, Ulrike, Peters, and Graham, Casey

Subjects

Organoids, Aspirin, Colon, Sequence Analysis, RNA, Humans, Transcriptome, Article

Abstract

Mechanisms underlying aspirin chemoprevention of colorectal cancer remain unclear. Prior studies have been limited due to the inability of preclinical models to recapitulate human normal colon epithelium or cellular heterogeneity present in mucosal biopsies. To overcome some of these obstacles we performed in vitro aspirin treatment of colon organoids derived from normal mucosal biopsies to reveal transcriptional networks relevant to aspirin chemoprevention. Colon organoids derived from 38 healthy individuals undergoing endoscopy were treated with 50μM aspirin or vehicle control for 72 hours and subjected to bulk RNA-sequencing. Paired regression analysis using DESeq2 identified differentially expressed genes (DEGs) associated with aspirin treatment. Cellular composition was determined using CIBERSORTx. Aspirin treatment was associated with 1,154 significant (q

Published

2021

9. Novel insights into the molecular mechanisms underlying risk of colorectal cancer from smoking and red/processed meat carcinogens by modeling exposure in normal colon organoids

Author

Virginia Díez-Obrero, Lucas T. Jennelle, Christopher H. Dampier, Graham Casey, Mourad Wagdy Ali, Ulrike Peters, Ferran Moratalla-Navarro, Stephen Eaton, Victor Moreno, Jennifer Bryant, Matthew Devall, and Steven M. Powell

Subjects

Carcinògens, colon organoids, Etiology, weighted gene co-expression network analysis, Colorectal cancer, Biology, smoking, Tobacco smoke, Hàbit de fumar, Càncer colorectal, medicine, Organoid, Gene, Carcinogen, Genetic association, single-cell deconvolution, Smoking, Microsatellite instability, medicine.disease, digestive system diseases, In vitro, Oncology, Etiologia, Cancer research, Carcinogens, microsatellite instability, Research Paper

Abstract

Tobacco smoke and red/processed meats are well-known risk factors for colorectal cancer (CRC). Most research has focused on studies of normal colon biopsies in epidemiologic studies or treatment of CRC cell lines in vitro. These studies are often constrained by challenges with accuracy of self-report data or, in the case of CRC cell lines, small sample sizes and lack of relationship to normal tissue at risk. In an attempt to address some of these limitations, we performed a 24-hour treatment of a representative carcinogens cocktail in 37 independent organoid lines derived from normal colon biopsies. Machine learning algorithms were applied to bulk RNA-sequencing and revealed cellular composition changes in colon organoids. We identified 738 differentially expressed genes in response to carcinogens exposure. Network analysis identified significantly different modules of co-expression, that included genes related to MSI-H tumor biology, and genes previously implicated in CRC through genome-wide association studies. Our study helps to better define the molecular effects of representative carcinogens from smoking and red/processed meat in normal colon epithelial cells and in the etiology of the MSI-H subtype of CRC, and suggests an overlap between molecular mechanisms involved in inherited and environmental CRC risk. Keywords: colon organoids; microsatellite instability; single-cell deconvolution; smoking; weighted gene co-expression network analysis.

Published

2021

10. Colon Crypts of Subjects With Familial Adenomatous Polyposis Show an Increased Number of LGR5+ Ectopic Stem Cells

Author

Christopher H. Dampier, Lucas T. Jennelle, Stephanie Tring, Graham Casey, and Steven M. Powell

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Adenoma, Colorectal cancer, Colon, Biopsy, Fluorescent Antibody Technique, Article, Familial adenomatous polyposis, DNA Glycosylases, Receptors, G-Protein-Coupled, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Medicine, Humans, neoplasms, Aged, Cell Proliferation, Microscopy, Confocal, business.industry, Stem Cells, Gastroenterology, LGR5, Wnt signaling pathway, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Immunohistochemistry, Lynch syndrome, digestive system diseases, Adenomatous Polyposis Coli, 030220 oncology & carcinogenesis, Case-Control Studies, Cancer research, 030211 gastroenterology & hepatology, Female, Stem cell, business

Abstract

Introduction Familial adenomatous polyposis (FAP) is a hereditary colorectal cancer (CRC) syndrome characterized by accelerated adenoma development due to inherited (or de novo) mutations in the APC regulator of WNT signaling pathway (APC) gene. The mechanism underlying this accelerated polyp development in subjects with FAP has not been defined. Given that LGR5+ stem cells drive crypt cell proliferation, we hypothesized that FAP crypts would demonstrate aberrant leucine-rich repeat-containing G-protein-coupled receptor 5 (LGR5) staining patterns. Methods Biopsies were taken from 11 healthy subjects, 7 subjects with Lynch syndrome, 4 subjects with FAP, and 1 subject with MUTYH-associated polyposis syndrome during routine screening or surveillance colonoscopy. Crypt staining was evaluated by immunohistochemistry of paraffin-embedded tissue sections. Stem cell numbers were estimated by immunofluorescence staining of isolated crypts using antibodies against LGR5 and other proteins. Results Subjects with FAP exhibited a greater number of LGR5+ stem cells in their crypts than healthy subjects and subjects with Lynch syndrome and MUTYH-associated polyposis syndrome. Most crypts of subjects with FAP harbored LGR5+ cells located above the lower third of the crypts. Discussion These findings support a model in which inactivation of one copy of APC leads to increased numbers of LGR5+ stem cells, many of which are ectopic, in colon crypts of subjects with FAP. Overabundant and ectopic LGR5+ stem cells could lead to an expanded proliferative zone of dividing cells more likely to develop mutations that would contribute to the accelerated adenoma development observed in FAP.

Published

2020

11. Immunometabolic Signaling Pathways Contribute to Macrophage and Dendritic Cell Function

Author

Aditya Dandekar, Young S. Hahn, Tshifhiwa Magoro, and Lucas T. Jennelle

Subjects

0301 basic medicine, T-Lymphocytes, Systems biology, Immunology, Disease, Article, 03 medical and health sciences, Immune system, Animals, Humans, Immunology and Allergy, Integrated stress response, Medicine, business.industry, Macrophages, Dendritic Cells, Dendritic cell, Crosstalk (biology), 030104 developmental biology, Unfolded protein response, Interferons, Signal transduction, business, Neuroscience, Signal Transduction

Abstract

Understanding of antigen-presenting cell (APC) participation in tissue inflammation and metabolism has advanced through numerous studies using systems biology approaches. Previously unrecognized connections between these research areas have been elucidated in the context of inflammatory disease involving innate and adaptive immune responses. A new conceptual framework bridges APC biology, metabolism, and cytokines in the generation of effective T-cell responses. Exploring these connections is paramount to addressing the rising tide of multi-organ system diseases, particularly chronic diseases associated with metabolic syndrome, infection, and cancer. Focused research in these areas will aid the development of strategies to harness and manipulate innate immunology to improve vaccine development, anti-viral, anti-inflammatory, and anti-tumor therapies. This review highlights recent advances in APC "immunometabolism" specifically related to chronic viral and metabolic disease in humans. The goal of this review is to develop an abridged and consolidated outlook on recent thematic updates to APC immunometabolism in the areas of regulation and crosstalk between metabolic and inflammatory signaling and the integrated stress response and how these signals dictate APC function in providing T-cell activation Signal 3.

Published

2016

12. Oncogenic Features in Histologically Normal Mucosa: Novel Insights Into Field Effect From a Mega-Analysis of Colorectal Transcriptomes

Author

Sarah J. Plummer, Graham Casey, Virginia Díez-Obrero, Lucas T. Jennelle, Christopher H. Dampier, Matthew Devall, and Victor Moreno

Subjects

Oncology, medicine.medical_specialty, Carcinogenesis, Colon, Colorectal cancer, Biopsy, Datasets as Topic, Malignancy, Article, Cohort Studies, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Càncer colorectal, Internal medicine, Biomarkers, Tumor, medicine, Humans, Mass Screening, RNA-Seq, Intestinal Mucosa, Independent data, Gene, business.industry, Gastroenterology, Computational Biology, Cancer, Colonoscopy, medicine.disease, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, Cohort, RNA, 030211 gastroenterology & hepatology, Mega analysis, Colorectal Neoplasms, business

Abstract

Introduction Colorectal cancer is a common malignancy that can be cured when detected early, but recurrence among survivors is a persistent risk. A field effect of cancer in the colon has been reported and could have implications for surveillance, but studies to date have been limited. A joint analysis of pooled transcriptomic data from all available bulk RNA-sequencing data sets of healthy, histologically normal tumor-adjacent, and tumor tissues was performed to provide an unbiased assessment of field effect. Methods A novel bulk RNA-sequencing data set from biopsies of nondiseased colon from screening colonoscopy along with published data sets from the Genomic Data Commons and Sequence Read Archive were considered for inclusion. Analyses were limited to samples with a quantified read depth of at least 10 million reads. Transcript abundance was estimated with Salmon, and downstream analysis was performed in R. Results A total of 1,139 samples were analyzed in 3 cohorts. The primary cohort consisted of 834 independent samples from 8 independent data sets, including 462 healthy, 61 tumor-adjacent, and 311 tumor samples. Tumor-adjacent gene expression was found to represent an intermediate state between healthy and tumor expression. Among differentially expressed genes in tumor-adjacent samples, 1,143 were expressed in patterns similar to tumor samples, and these genes were enriched for cancer-associated pathways. Discussion Novel insights into the field effect in colorectal cancer were generated in this mega-analysis of the colorectal transcriptome. Oncogenic features that might help explain metachronous lesions in cancer survivors and could be used for surveillance and risk stratification were identified.

Published

2020

13. Expression of scavenger receptor-AI promotes alternative activation of murine macrophages to limit hepatic inflammation and fibrosis

Author

Lucas T. Jennelle, Adam C. Labonte, Aditya Dandekar, Young S. Hahn, and Sun‐Sang J. Sung

Subjects

0301 basic medicine, Liver Cirrhosis, Adoptive cell transfer, Viral Hepatitis, Immunology, Biology, Hepatitis, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Fibrosis, medicine, Animals, Scavenger receptor, Cells, Cultured, Gene knockdown, Hepatology, Scavenger Receptors, Class A, MERTK, Macrophage Activation, medicine.disease, 3. Good health, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Experimental Models of Liver Disease, Cell culture, 030220 oncology & carcinogenesis, Regulatory Pathways, Female, Hepatic fibrosis

Abstract

The liver maintains an immunologically tolerant environment as a result of continuous exposure to food and bacterial constituents from the digestive tract. Hepatotropic pathogens can take advantage of this niche and establish lifelong chronic infections causing hepatic fibrosis and hepatocellular carcinoma. Macrophages (Mϕ) play a critical role in regulation of immune responses to hepatic infection and regeneration of tissue. However, the factors crucial for Mϕ in limiting hepatic inflammation or resolving liver damage have not been fully understood. In this report, we demonstrate that expression of C‐type lectin receptor scavenger receptor‐AI (SR‐AI) is crucial for promoting M2‐like Mϕ activation and polarization during hepatic inflammation. Liver Mϕ uniquely up‐regulated SR‐AI during hepatotropic viral infection and displayed increased expression of alternative Mϕ activation markers, such as YM‐1, arginase‐1, and interleukin‐10 by activation of mer receptor tyrosine kinase associated with inhibition of mammalian target of rapamycin. Expression of these molecules was reduced on Mϕ obtained from livers of infected mice deficient for the gene encoding SR‐AI (msr1). Furthermore, in vitro studies using an SR‐AI‐deficient Mϕ cell line revealed impeded M2 polarization and decreased phagocytic capacity. Direct stimulation with virus was sufficient to activate M2 gene expression in the wild‐type (WT) cell line, but not in the knockdown cell line. Importantly, tissue damage and fibrosis were exacerbated in SR‐AI–/– mice following hepatic infection and adoptive transfer of WT bone‐marrow–derived Mϕ conferred protection against fibrosis in these mice. Conclusion: SR‐AI expression on liver Mϕ promotes recovery from infection‐induced tissue damage by mediating a switch to a proresolving Mϕ polarization state. (Hepatology 2017;65:32‐43).

Published

2016

14. HIV-1 Nef targets calnexin: a novel mechanism behind Nef effects on host cell and viral proteins

Author

Ruth Hunegnaw, Lucas T. Jennelle, Michael Bukrinsky, and Dmitri Sviridov

Subjects

Cell signaling, Glycosylation, biology, viruses, Endoplasmic reticulum, virus diseases, Virology, Cell biology, chemistry.chemical_compound, Infectious Diseases, chemistry, Chaperone (protein), Calnexin, ABCA1, Poster Presentation, MHC class I, biology.protein, lipids (amino acids, peptides, and proteins), Target protein

Abstract

HIV-1 Nef is a pleiotropic modulator of various cellular signaling proteins and cell surface receptors. It conditions cells for viral replication by aiding in immune evasion and priming T-cell activation, and also enhances HIV-1 infectivity by a poorly defined mechanism. Most of described effects of Nef, such as downregulation of CD4 and MHC I, involve Nef binding to the target protein and directing it to a degradation pathway. We have demonstrated previously that Nef causes degradation and functional impairment of ABCA1, the major cellular cholesterol transporter, an effect that likely contributes to low HDL levels and high risk of atherosclerosis in HIV-infected patients. Surprisingly, direct interaction between Nef and ABCA1 was not required for ABCA1 inactivation. Here we investigated the mechanism of this Nef activity using proteomics, co-immunoprecipitation, mutagenesis, confocal microscopy, and subcellular fractionation approaches. These studies identified calnexin, an endoplasmic reticulum (ER) resident lectin-like chaperone, as an essential partner of ABCA1 and a target of Nef, and characterized Nef- calnexin interaction and its effects on interactions between calnexin and its other partners, such as gp160. We demonstrated that Nef binds to calnexin and increases affinity and enhances interaction of calnexin with HIV-1 gp160, but disrupts calnexin interaction with ABCA1. Interaction with calnexin is essential for functionality of both these proteins, as knock-down of calnexin led to reduced infectivity of HIV-1, as well as to defective cholesterol efflux. However, gp160 and ABCA1 interacted with calnexin differently: while gp160 binding to calnexin was dependent on glycosylation, glycosylation was of little importance for interaction between ABCA1 and calnexin. Thus, Nef binding appears to induce a conformational change in calnexin that stimulates glycosylation-dependent interaction of calnexin with gp160 at the expense of glycosylation-independent interaction with ABCA1. This study identifies a novel mechanism for Nef-dependent inactivation of ABCA1, provides an additional explanation for the effect of Nef on HIV-1 infectivity, and suggests a number of other potential targets of this new Nef activity.

Published

2013