Your search keyword '"MEMBRANE glycoproteins"' showing total 83,462 results

1. Lipid-associated macrophages’ promotion of fibrosis resolution during MASH regression requires TREM2

Author

Ganguly, Souradipta, Rosenthal, Sara Brin, Ishizuka, Kei, Troutman, Ty D, Rohm, Theresa V, Khader, Naser, Aleman-Muench, German, Sano, Yasuyo, Archilei, Sebastiano, Soroosh, Pejman, Olefsky, Jerrold M, Feldstein, Ariel E, Kisseleva, Tatiana, Loomba, Rohit, Glass, Christopher K, Brenner, David A, and Dhar, Debanjan

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Digestive Diseases, Liver Disease, Chronic Liver Disease and Cirrhosis, 2.1 Biological and endogenous factors, Good Health and Well Being, Receptors, Immunologic, Membrane Glycoproteins, Animals, Mice, Macrophages, Liver Cirrhosis, Kupffer Cells, Liver, Lipid Metabolism, Mice, Inbred C57BL, Male, Lipids, Fatty Liver, Mice, Knockout, Trem2, fibrosis, lipid associated macrophages, macrophage, steatohepatitis

Abstract

While macrophage heterogeneity during metabolic dysfunction-associated steatohepatitis (MASH) has been described, the fate of these macrophages during MASH regression is poorly understood. Comparing macrophage heterogeneity during MASH progression vs regression, we identified specific macrophage subpopulations that are critical for MASH/fibrosis resolution. We elucidated the restorative pathways and gene signatures that define regression-associated macrophages and establish the importance of TREM2+ macrophages during MASH regression. Liver-resident Kupffer cells are lost during MASH and are replaced by four distinct monocyte-derived macrophage subpopulations. Trem2 is expressed in two macrophage subpopulations: i) monocyte-derived macrophages occupying the Kupffer cell niche (MoKC) and ii) lipid-associated macrophages (LAM). In regression livers, no new transcriptionally distinct macrophage subpopulation emerged. However, the relative macrophage composition changed during regression compared to MASH. While MoKC was the major macrophage subpopulation during MASH, they decreased during regression. LAM was the dominant macrophage subtype during MASH regression and maintained Trem2 expression. Both MoKC and LAM were enriched in disease-resolving pathways. Absence of TREM2 restricted the emergence of LAMs and formation of hepatic crown-like structures. TREM2+ macrophages are functionally important not only for restricting MASH-fibrosis progression but also for effective regression of inflammation and fibrosis. TREM2+ macrophages are superior collagen degraders. Lack of TREM2+ macrophages also prevented elimination of hepatic steatosis and inactivation of HSC during regression, indicating their significance in metabolic coordination with other cell types in the liver. TREM2 imparts this protective effect through multifactorial mechanisms, including improved phagocytosis, lipid handling, and collagen degradation.

Published

2024

2. Plexin D1 emerges as a novel target in the development of neural lineage plasticity in treatment-resistant prostate cancer

Author

Chen, Bo, Xu, Pengfei, Yang, Joy C, Nip, Christopher, Wang, Leyi, Shen, Yuqiu, Ning, Shu, Shang, Yufeng, Corey, Eva, Gao, Allen C, Gestwicki, Jason E, Wei, Qiang, Liu, Liangren, and Liu, Chengfei

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Prostate Cancer, Genetics, Urologic Diseases, Biotechnology, Cancer, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Humans, Male, Animals, Mice, Drug Resistance, Neoplasm, Cell Line, Tumor, Prostatic Neoplasms, Cell Proliferation, Gene Expression Regulation, Neoplastic, Cell Lineage, Nerve Tissue Proteins, Xenograft Model Antitumor Assays, Cell Plasticity, Receptors, Cell Surface, Prognosis, Membrane Glycoproteins, Intracellular Signaling Peptides and Proteins, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Treatment-induced neuroendocrine prostate cancer (t-NEPC) often arises from adenocarcinoma via lineage plasticity in response to androgen receptor signaling inhibitors, such as enzalutamide. However, the specific regulators and targets involved in the transition to NEPC are not well understood. Plexin D1 (PLXND1) is a cellular receptor of the semaphorin (SEMA) family that plays important roles in modulating the cytoskeleton and cell adhesion. Here, we found that PLXND1 was highly expressed and positively correlated with neuroendocrine markers in patients with NEPC. High PLXND1 expression was associated with poorer prognosis in prostate cancer patients. Additionally, PLXND1 was upregulated and negatively regulated by androgen receptor signaling in enzalutamide-resistant cells. Knockdown or knockout of PLXND1 inhibited neural lineage pathways, thereby suppressing NEPC cell proliferation, patient derived xenograft (PDX) tumor organoid viability, and xenograft tumor growth. Mechanistically, the heat shock protein 70 (HSP70) regulated PLXND1 protein stability through degradation, and inhibition of HSP70 decreased PLXND1 expression and NEPC organoid growth. In summary, our findings indicate that PLXND1 could serve as a promising therapeutic target and molecular marker for NEPC.

Published

2024

3. Clinical characteristics and treatment patterns of patients with NTRK fusion-positive solid tumors: A multisite cohort study at US academic cancer centers.

Author

Willis, Connor, Au, Trang, Hejazi, Andre, Griswold, Cassia, Schabath, Matthew, Thompson, Jonathan, Malhotra, Jyoti, Federman, Noah, Ko, Gilbert, Appukkuttan, Sreevalsa, Warnock, Neil, Kong, Sheldon, Hocum, Brian, Brixner, Diana, and Stenehjem, David

Subjects

Humans, Female, Male, Retrospective Studies, Middle Aged, United States, Neoplasms, Receptor, trkC, Aged, Receptor, trkA, Adult, Protein Kinase Inhibitors, Receptor, trkB, Academic Medical Centers, Membrane Glycoproteins, Oncogene Proteins, Fusion, Cohort Studies, Pyrimidines, Pyrazoles, Benzamides, Young Adult, Indazoles

Abstract

BACKGROUND: Neurotrophic tyrosine receptor kinase (NTRK) gene fusions are rare oncogenic drivers prevalent in 0.3% of solid tumors. They are most common in salivary gland cancer (2.6%), thyroid cancer (1.6%), and soft-tissue sarcoma (1.5%). Currently, there are 2 US Food and Drug Administration-approved targeted therapies for NTRK gene fusions: larotrectinib, approved in 2018, and entrectinib, approved in 2019. To date, the real-world uptake of tyrosine receptor kinase inhibitor (TRKi) use for NTRK-positive solid tumors in academic cancer centers remains largely unknown. OBJECTIVE: To describe the demographics, clinical and genomic characteristics, and testing and treatment patterns of patients with NTRK-positive solid tumors treated at US academic cancer centers. METHODS: This was a retrospective chart review study conducted in academic cancer centers in the United States. All patients diagnosed with an NTRK fusion-positive (NTRK1, NTRK2, NTRK3) solid tumor (any stage) and who received cancer treatment at participating sites between January 1, 2012, and July 1, 2023, were included in this study. Patient demographics, clinical characteristics, genomic characteristics, NTRK testing data, and treatment patterns were collected from electronic medical records and analyzed using descriptive statistics as appropriate. RESULTS: In total, 6 centers contributed data for 55 patients with NTRK-positive tumors. The mean age was 49.3 (SD = 20.5) years, 51% patients were female, and the majority were White (78%). The median duration of time from cancer diagnosis to NTRK testing was 85 days (IQR = 44-978). At the time of NTRK testing, 64% of patients had stage IV disease, compared with 33% at cancer diagnosis. Prevalent cancer types in the overall cohort included head and neck (15%), thyroid (15%), brain (13%), lung (13%), and colorectal (11%). NTRK1 fusions were most common (45%), followed by NTRK3 (40%) and NTRK2 (15%). Across all lines of therapy, 51% of patients (n = 28) received a TRKi. Among TRKi-treated patients, 71% had stage IV disease at TRKi initiation. The median time from positive NTRK test to initiation of TRKi was 48 days (IQR = 9-207). TRKis were commonly given as first-line (30%) or second-line (48%) therapies. Median duration of therapy was 610 (IQR = 182-764) days for TRKi use and 207.5 (IQR = 42-539) days for all other first-line therapies. CONCLUSIONS: This study reports on contemporary real-world NTRK testing patterns and use of TRKis in solid tumors, including time between NTRK testing and initiation of TRKi therapy and duration of TRKi therapy.

Published

2024

4. UCHL1 is a potential molecular indicator and therapeutic target for neuroendocrine carcinomas.

Author

Liu, Shiqin, Chai, Timothy, Garcia-Marques, Fernando, Yin, Qingqing, Hsu, En-Chi, Shen, Michelle, Shaw Toland, Angus, Bermudez, Abel, Hartono, Alifiani, Massey, Christopher, Lee, Chung, Zheng, Liwei, Baron, Maya, Denning, Caden, Aslan, Merve, Nguyen, Holly, Zoubeidi, Amina, Das, Millie, Kunder, Christian, Howitt, Brooke, Soh, H, Weissman, Irving, Liss, Michael, Chin, Arnold, Brooks, James, Corey, Eva, Pitteri, Sharon, Huang, Jiaoti, Nolley, Rosie, and Stoyanova, Tanya

Subjects

UCHL1, neuroblastoma, neuroendocrine carcinomas, neuroendocrine prostate cancer, nuclear pore complex, small cell lung cancer, Male, Humans, Ubiquitin Thiolesterase, Carcinoma, Neuroendocrine, Small Cell Lung Carcinoma, Lung Neoplasms, Membrane Glycoproteins

Abstract

Neuroendocrine carcinomas, such as neuroendocrine prostate cancer and small-cell lung cancer, commonly have a poor prognosis and limited therapeutic options. We report that ubiquitin carboxy-terminal hydrolase L1 (UCHL1), a deubiquitinating enzyme, is elevated in tissues and plasma from patients with neuroendocrine carcinomas. Loss of UCHL1 decreases tumor growth and inhibits metastasis of these malignancies. UCHL1 maintains neuroendocrine differentiation and promotes cancer progression by regulating nucleoporin, POM121, and p53. UCHL1 binds, deubiquitinates, and stabilizes POM121 to regulate POM121-associated nuclear transport of E2F1 and c-MYC. Treatment with the UCHL1 inhibitor LDN-57444 slows tumor growth and metastasis across neuroendocrine carcinomas. The combination of UCHL1 inhibitors with cisplatin, the standard of care used for neuroendocrine carcinomas, significantly delays tumor growth in pre-clinical settings. Our study reveals mechanisms of UCHL1 function in regulating the progression of neuroendocrine carcinomas and identifies UCHL1 as a therapeutic target and potential molecular indicator for diagnosing and monitoring treatment responses in these malignancies.

Published

2024

5. Critical domains for NACC2-NTRK2 fusion protein activation.

Author

Yang, Wei, Meyer, April, Jiang, Zian, Jiang, Xuan, and Donoghue, Daniel

Subjects

Humans, Oncogene Proteins, Fusion, Receptor, trkB, Protein Domains, Mutation, Membrane Glycoproteins, Glioblastoma, Signal Transduction, Protein Multimerization

Abstract

Neurotrophic receptor tyrosine kinases (NTRKs) belong to the receptor tyrosine kinase (RTK) family. NTRKs are responsible for the activation of multiple downstream signaling pathways that regulate cell growth, proliferation, differentiation, and apoptosis. NTRK-associated mutations often result in oncogenesis and lead to aberrant activation of downstream signaling pathways including MAPK, JAK/STAT, and PLCγ1. This study characterizes the NACC2-NTRK2 oncogenic fusion protein that leads to pilocytic astrocytoma and pediatric glioblastoma. This fusion joins the BTB domain (Broad-complex, Tramtrack, and Bric-a-brac) domain of NACC2 (Nucleus Accumbens-associated protein 2) with the transmembrane helix and tyrosine kinase domain of NTRK2. We focus on identifying critical domains for the biological activity of the fusion protein. Mutations were introduced in the charged pocket of the BTB domain or in the monomer core, based on a structural comparison of the NACC2 BTB domain with that of PLZF, another BTB-containing protein. Mutations were also introduced into the NTRK2-derived portion to allow comparison of two different breakpoints that have been clinically reported. We show that activation of the NTRK2 kinase domain relies on multimerization of the BTB domain in NACC2-NTRK2. Mutations which disrupt BTB-mediated multimerization significantly reduce kinase activity and downstream signaling. The ability of these mutations to abrogate biological activity suggests that BTB domain inhibition could be a potential treatment for NACC2-NTRK2-induced cancers. Removal of the transmembrane helix leads to enhanced stability of the fusion protein and increased activity of the NACC2-NTRK2 fusion, suggesting a mechanism for the oncogenicity of a distinct NACC2-NTRK2 isoform observed in pediatric glioblastoma.

Published

2024

6. CAR-T cell therapy targeting surface expression of TYRP1 to treat cutaneous and rare melanoma subtypes

Author

Jilani, Sameeha, Saco, Justin D, Mugarza, Edurne, Pujol-Morcillo, Aleida, Chokry, Jeffrey, Ng, Clement, Abril-Rodriguez, Gabriel, Berger-Manerio, David, Pant, Ami, Hu, Jane, Gupta, Rubi, Vega-Crespo, Agustin, Baselga-Carretero, Ignacio, Chen, Jia M, Shin, Daniel Sanghoon, Scumpia, Philip, Radu, Roxana A, Chen, Yvonne, Ribas, Antoni, and Puig-Saus, Cristina

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Genetics, Gene Therapy, Cancer, Rare Diseases, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Humans, Mice, Animals, Melanoma, Receptors, Chimeric Antigen, Immunotherapy, Adoptive, Uveal Neoplasms, Cell- and Tissue-Based Therapy, Membrane Glycoproteins, Oxidoreductases

Abstract

A major limitation to developing chimeric antigen receptor (CAR)-T cell therapies for solid tumors is identifying surface proteins highly expressed in tumors but not in normal tissues. Here, we identify Tyrosinase Related Protein 1 (TYRP1) as a CAR-T cell therapy target to treat patients with cutaneous and rare melanoma subtypes unresponsive to immune checkpoint blockade. TYRP1 is primarily located intracellularly in the melanosomes, with a small fraction being trafficked to the cell surface via vesicular transport. We develop a highly sensitive CAR-T cell therapy that detects surface TYRP1 in tumor cells with high TYRP1 overexpression and presents antitumor activity in vitro and in vivo in murine and patient-derived cutaneous, acral and uveal melanoma models. Furthermore, no systemic or off-tumor severe toxicities are observed in an immunocompetent murine model. The efficacy and safety profile of the TYRP1 CAR-T cell therapy supports the ongoing preparation of a phase I clinical trial.

Published

2024

7. Safety and immunogenicity of the live-attenuated hRVFV-4s vaccine against Rift Valley fever in healthy adults: a dose-escalation, placebo-controlled, first-in-human, phase 1 randomised clinical trial.

Author

Leroux-Roels, Isabel, Prajeeth, Chittappen Kandiyil, Aregay, Amare, Nair, Niranjana, Rimmelzwaan, Guus F, Osterhaus, Albert D M E, Kardinahl, Simone, Pelz, Sabrina, Bauer, Stephan, D'Onofrio, Valentino, Alhatemi, Azhar, Jacobs, Bart, De Boever, Fien, Porrez, Sharon, Waerlop, Gwenn, Punt, Carine, Hendriks, Bart, von Mauw, Ellemieke, van de Water, Sandra, and Harders-Westerveen, Jose

Subjects

*RIFT Valley fever, *PANDEMIC preparedness, *VACCINE effectiveness, *MEMBRANE glycoproteins, *TISSUE culture, *ALPHAVIRUSES

Abstract

Rift Valley fever virus, a pathogen to ruminants, camelids, and humans, is an emerging mosquito-borne bunyavirus currently endemic to Africa and the Arabian Peninsula. Although animals are primarily infected via mosquito bites, humans mainly become infected following contact with infected tissues or fluids of infected animals. There is an urgent need for adequate countermeasures, especially for humans, because effective therapeutics or vaccines are not yet available. Here we assessed the safety, tolerability, and immunogenicity of a next-generation, four-segmented, live-attenuated vaccine candidate, referred to as hRVFV-4s, in humans. A first-in-human, single-centre, randomised, double-blind, placebo-controlled trial was done in Belgium in which a single dose of hRVFV-4s was administered to healthy volunteers aged 18–45 years. Participants were randomly assigned using an interactive web response system. The study population encompassed 75 participants naive to Rift Valley fever virus infection, divided over three dosage groups (cohorts) of 25 participants each. All participants were followed up until 6 months. Using a staggered dose escalating approach, 20 individuals of each cohort were injected in the deltoid muscle of the non-dominant arm with either 104 (low dose), 105 (medium dose), or 106 (high dose) of 50% tissue culture infectious dose of hRVFV-4s as based on animal data, and five individuals per cohort received formulation buffer as a placebo. Primary outcome measures in the intention-to-treat population were adverse events and tolerability. Secondary outcome measures were vaccine-induced viraemia, vaccine virus shedding, Rift Valley fever virus nucleocapsid antibody responses (with ELISA), and neutralising antibody titres. Furthermore, exploratory objectives included the assessment of cellular immune responses by ELISpot. The trial was registered with the EU Clinical Trials Register, 2022-501460-17-00. Between August and December, 2022, all 75 participants were vaccinated. No serious adverse events or vaccine-related severe adverse events were reported. Pain at the injection site (51 [85%] of 60 participants) was most frequently reported as solicited local adverse event, and headache (28 [47%] of 60) and fatigue (28 [47%] of 60) as solicited systemic adverse events in the active group. No vaccine virus RNA was detected in any of the blood, saliva, urine, or semen samples. Rift Valley fever virus nucleocapsid antibody responses were detected in most participants who were vaccinated with hRVFV-4s (43 [72%] of 60 on day 14) irrespective of the administered dose. In contrast, a clear dose–response relationship was observed for neutralising antibodies on day 28 with four (20%) of 20 participants responding in the low-dose group, 13 (65%) of 20 responding in the medium-dose group, and all participants (20 [100%] of 20) responding in the high-dose group. Consistent with the antibody responses, cellular immune responses against the nucleocapsid protein were detected in all dose groups, whereas a more dose-dependent response was observed for the Gn and Gc surface glycoproteins. Neutralising antibody titres declined over time, whereas nucleocapsid antibody responses remained relatively stable for at least 6 months. The hRVFV-4s vaccine showed a high safety profile and excellent tolerability across all tested dose regimens, eliciting robust immune responses, particularly with the high-dose administration. The findings strongly support further clinical development of this candidate vaccine for human use. The Coalition for Epidemic Preparedness Innovations with support from the EU Horizon 2020 programme. [ABSTRACT FROM AUTHOR]

Published

2024

8. Platelet Physiology *.

Author

Gremmel, Thomas, Frelinger III, Andrew L., and Michelson, Alan D.

Subjects

*MEMBRANE glycoproteins, *BLOOD platelet activation, *BLOOD cells, *BLOOD platelets, *TUMOR growth

Abstract

Platelets are the smallest blood cells, numbering 150 to 350 × 10 9 /L in healthy individuals. The ability of activated platelets to adhere to an injured vessel wall and form aggregates was first described in the 19th century. Besides their long-established roles in thrombosis and hemostasis, platelets are increasingly recognized as pivotal players in numerous other pathophysiological processes including inflammation and atherogenesis, antimicrobial host defense, and tumor growth and metastasis. Consequently, profound knowledge of platelet structure and function is becoming more important in research and in many fields of modern medicine. This review provides an overview of platelet physiology focusing particularly on the structure, granules, surface glycoproteins, and activation pathways of platelets. [ABSTRACT FROM AUTHOR]

Published

2024

9. Unravelling CD24‐Siglec‐10 pathway: Cancer immunotherapy from basic science to clinical studies.

Author

Hazra, Rudradeep, Chattopadhyay, Soumyadeep, Mallick, Arijit, Gayen, Sakuntala, and Roy, Souvik

Subjects

*MEMBRANE glycoproteins, *TUMOR microenvironment, *IMMUNOLOGICAL tolerance, *IMMUNE response, *IMMUNE system

Abstract

Cancer immunotherapy has revolutionized the treatment landscape by harnessing the power of the immune system to combat malignancies. Two of the most promising players in this field are cluster of differentiation 24 (CD24) and sialic acid‐binding Ig‐like lectin 10 (Siglec‐10), and both of them play pivotal roles in modulating immune responses. CD24, a cell surface glycoprotein, emerges as a convincing fundamental signal transducer for therapeutic intervention, given its significant implication in the processes related to tumour progression and immunogenic evasion. Additionally, the immunomodulatory functions of Siglec‐10, a prominent member within the Siglec family of immune receptors, have recently become a crucial point of interest, particularly in the context of the tumour microenvironment. Hence, the intricate interplay of both CD24 and Siglec‐10 assumes a critical role in fostering tumour growth, facilitating metastasis and also orchestrating immune evasion. Recent studies have found multiple evidences supporting the therapeutic potential of targeting CD24 in cancer treatment. Siglec‐10, on the other hand, exhibits immunosuppressive properties that contribute to immune tolerance within the tumour microenvironment. Therefore, we delve into the complex mechanisms through which Siglec‐10 modulates immune responses and facilitates immune escape in cancer. Siglec‐10 also acts as a viable target for cancer immunotherapy and presents novel avenues for the development of therapeutic interventions. Furthermore, we examine the synergy between CD24 and Siglec‐10 in shaping the immunosuppressive tumour microenvironment and discuss the implications for combination therapies. Therefore, understanding the roles of CD24 and Siglec‐10 in cancer immunotherapy opens exciting possibilities for the development of novel therapeutics. [ABSTRACT FROM AUTHOR]

Published

2024

10. Dendritic Cells Loaded With Heat Shock Inactivated Glioma Stem Cells Enhance Antitumor Response of Mouse Glioma When Combining With CD47 Blockade.

Author

Tan, Qijia, Li, Feng, Wang, Jun, Liu, Yi, Cai, Yingqian, Zou, Yuxi, and Jiang, Xiaodan

Subjects

*BIOLOGICAL models, *FLOW cytometry, *IMMUNIZATION, *IN vitro studies, *T-cell lymphoma, *GLIOMAS, *MONOCYTES, *RESEARCH funding, *PHYSIOLOGICAL effects of heat, *IMMUNOTHERAPY, *TREATMENT effectiveness, *CANCER vaccines, *IN vivo studies, *DESCRIPTIVE statistics, *MICE, *MEMBRANE glycoproteins, *ANIMAL experimentation, *CELL death, *STEM cells, *TUMOR antigens, *DENDRITIC cells

Abstract

Background: For glioma patients, the long-term advantages of dendritic cells (DCs) immunization remain unknown. It is extremely important to develop new treatment strategies that enhance the immunotherapy effect of DC-based vaccines. DCs exposed to glioma stem cells (GSCs) are considered promising vaccines against glioma. Methods: Glioma stem cells were isolated from mouse glioma GL261 cells (GCs). Both were subjected to severe (47°C) and mild (42°C) heat shock to induce immunogenic cell death (ICD). Membrane mobilization of calreticulin (CRT) and release of heat shock proteins (HSPs) were detected by flow cytometry. Dendritic cells were then exposed to heat-inactivated cells and co-culturing of T cells tested for immunotherapeutic efficacy in vitro. In vivo, we investigated the GSC targeting effect of the GSC-DC vaccine combined with CD47 blockade. Results: Heat shock induced ICD in GCs and GSCs, as indicated by significant release of calreticulin, HSP70, and HSP90. Heat shock condition ICD lysates induce maturation and activation-associated marker expression on monocyte-derived DCs. Accordingly, DCs pulsed with GCs and GSCs inactivated reduced colony formation, sphere formation, migration, and invasion of glioma and GSCs in vitro. Glioma stem cell-DC vaccine in combination with anti-CD47 antibody significantly enhanced survival in mice with glioma, induced production of interferon (IFN)-γ, and enhanced T-cell expansion in vivo. Of note, DCs pulsed with inactivated GSCs were more effective to control tumor growth than DCs pulsed with inactive GCs. Conclusions: Severe heat shock induces ICD in vitro. These data showed that administration of anti-CD47 antibody combined with GSC-DC vaccine may represent an effective immunotherapeutic strategy for cancer patients in clinical. [ABSTRACT FROM AUTHOR]

Published

2024

11. Enrichment of Rare Variants of Hemophagocytic Lymphohistiocytosis Genes in Systemic Juvenile Idiopathic Arthritis.

Author

Correia Marques, Mariana, Rubin, Danielle, Shuldiner, Emily G., Datta, Mallika, Schmitz, Elizabeth, Gutierrez Cruz, Gustavo, Patt, Andrew, Bennett, Elizabeth, Grom, Alexei, Foell, Dirk, Gattorno, Marco, Bohnsack, John, Yeung, Rae S. M., Prahalad, Sampath, Mellins, Elizabeth, Anton, Jordi, Len, Claudio A., Oliveira, Sheila, Woo, Patricia, and Ozen, Seza

Subjects

*NON-langerhans-cell histiocytosis, *JUVENILE idiopathic arthritis, *CARRIER proteins, *GENOME-wide association studies, *RESEARCH funding, *DESCRIPTIVE statistics, *GENES, *GENETIC variation, *LONGITUDINAL method, *MEMBRANE glycoproteins, *MACROPHAGE activation syndrome, *DISEASE susceptibility, *COMPARATIVE studies, *SEQUENCE analysis, *GENOTYPES, *PHENOTYPES, *DISEASE complications

Abstract

Objective: Our objective was to evaluate whether there is an enrichment of rare variants in familial hemophagocytic lymphohistiocytosis (HLH)‐associated genes among patients with systemic juvenile idiopathic arthritis (sJIA) with or without macrophage activation syndrome (MAS). Methods: Targeted sequencing of HLH genes (LYST, PRF1, RAB27A, STX11, STXBP2, UNC13D) was performed in patients with sJIA from an established cohort. Sequence data from control participants were obtained in silico (database of Genotypes and Phenotypes: phs000280.v8.p2). Rare variant association testing (RVT) was performed with sequence kernel association test package. Significance was defined as P < 0.05 after 100,000 permutations. Results: Sequencing data from 524 sJIA cases were jointly called and harmonized with exome‐derived target data from 3,000 controls. Quality control operations produced a set of 480 cases and 2,924 ancestrally matched control participants. RVT of cases and controls revealed a significant association with rare protein‐altering variants (minor allele frequency [MAF] < 0.01) of STXBP2 (P = 0.020) and ultrarare variants (MAF < 0.001) of STXBP2 (P = 0.006) and UNC13D (P = 0.046). A subanalysis of 32 cases with known MAS and 90 without revealed a significant difference in the distribution of rare UNC13D variants (P = 0.0047) between the groups. Additionally, patients with sJIA more often carried two or more HLH variants than did controls (P = 0.007), driven largely by digenic combinations involving LYST. Conclusion: We identified an enrichment of rare HLH variants in patients with sJIA compared with controls, driven by STXBP2 and UNC13D. Biallelic variation in HLH genes was associated with sJIA, driven by LYST. Only UNC13D displayed enrichment in patients with MAS. This suggests that HLH variants may contribute to the pathophysiology of sJIA, even without MAS. [ABSTRACT FROM AUTHOR]

Published

2024

12. Cosmc regulates O-glycan extension in murine hepatocytes.

Author

Aryal, Rajindra P, Noel, Maxence, Zeng, Junwei, Matsumoto, Yasuyuki, Sinard, Rachael, Waki, Hannah, Erger, Florian, Reusch, Björn, Beck, Bodo B, and Cummings, Richard D

Subjects

*MEMBRANE glycoproteins, *LIVER cells, *GLYCOPROTEINS, *LIVER, *MICE, *CHOLESTEROL metabolism

Abstract

Hepatocytes synthesize a vast number of glycoproteins found in their membranes and secretions, many of which contain O-glycans linked to Ser/Thr residues. As the functions and distribution of O-glycans on hepatocyte-derived membrane glycoproteins and blood glycoproteins are not well understood, we generated mice with a targeted deletion of Cosmc (C1Galt1c1) in hepatocytes. Liver glycoproteins in WT mice express typical sialylated core 1 O-glycans (T antigen/CD176) (Galβ1-3GalNAcα1-O-Ser/Thr), whereas the Cosmc knockout hepatocytes (HEP- Cosmc -KO) lack extended O-glycans and express the Tn antigen (CD175) (GalNAcα1-O-Ser/Thr). Tn-containing glycoproteins occur in the sera of HEP- Cosmc -KO mice but not in WT mice. The LDL-receptor (LDLR), a well-studied O-glycosylated glycoprotein in hepatocytes, behaves as a ∼145kD glycoprotein in WT liver lysates, whereas it is reduced to ∼120 kDa in lysates from HEP- Cosmc -KO mice. Interestingly, the expression of the LDLR, as well as HMG-CoA reductase, which is typically altered in response to dysregulated cholesterol metabolism, are similar between WT and HEP- Cosmc -KO mice, indicating no significant effect by Cosmc deletion on either LDLR stability or cholesterol metabolism. Consistent with this, we observed no detectable phenotype in the HEP- Cosmc -KO mice regarding development, appearance or aging compared to WT. These results provide surprising, novel information about the pathway of O-glycosylation in the liver. [ABSTRACT FROM AUTHOR]

Published

2024

13. Differential expression of FSTL1 and its correlation with the pathological process of periodontitis.

Author

Jiang, Wenxin, Yu, Weijun, Hu, Shucheng, Shi, Yuanjie, Lin, Lu, Yang, Ruhan, Tang, Jiaqi, Gu, Yuting, Gong, Yuhua, Jin, Min, and Lu, Eryi

Subjects

CARRIER proteins, RESEARCH funding, RECEIVER operating characteristic curves, PHENOMENOLOGICAL biology, GINGIVA, NEUTROPHILS, REVERSE transcriptase polymerase chain reaction, BIOCHEMISTRY, SEVERITY of illness index, GENE expression, BIOINFORMATICS, IMMUNOHISTOCHEMISTRY, WESTERN immunoblotting, MEMBRANE glycoproteins, PATHOLOGIC neovascularization, PERIODONTITIS, PEROXIDASE, IMMUNITY

Abstract

Aims: This study aimed to elucidate the alterations in Follistatin‐like protein 1 (FSTL1) and its association with the pathological process of periodontitis. Methods: This study included 48 patients with periodontitis and 42 healthy controls. The expression level of FSTL1 in the gingiva was determined by RT‐qPCR, validated using the dataset GSE16134, and subsequently examined by western blotting. Bioinformatics analysis revealed a single‐cell distribution of FSTL1, characteristic of angiogenesis and immune cell infiltration. The expression and distribution of FSTL1, vascular endothelial marker protein CD31 and myeloperoxidase (MPO), the indicator of neutrophil activity, were determined by immunohistochemistry (IHC). A series of correlation analyses was performed to determine the associations between FSTL1 and clinical parameters, including probing depth (PD) and clinical attachment loss (CAL), and their potential role in angiogenesis (CD31) and neutrophil infiltration (MPO). Results: FSTL1 was significantly upregulated in the gingiva of patients with periodontitis compared to their healthy counterparts. In addition, FSTL1 was positively correlated with the clinical parameters PD (r =.5971, p =.0005) and CAL (r =.6078, p =.0004). Bioinformatic analysis and IHC indicated that high FSTL1 expression was significantly correlated with angiogenesis and neutrophil infiltration in periodontitis. Moreover, receiver operating characteristic (ROC) analysis demonstrated that FSTL1 could serve as an independent indicator for evaluating the severity of periodontitis (area under the curve [AUC] = 0.9011, p <.0001). Conclusion: This study demonstrated FSTL1 upregulation in periodontitis and its potential contribution to the disease via angiogenesis and neutrophil infiltration. [ABSTRACT FROM AUTHOR]

Published

2024

14. Regulation of ICAM-1 in human neutrophils.

Author

Vignarajah, Muralie, Wood, Alexander J T, Nelmes, Elizabeth, Subburayalu, Julien, Herre, Jurgen, Nourshargh, Sussan, Summers, Charlotte, Chilvers, Edwin R, and Farahi, Neda

Subjects

CD54 antigen, MEMBRANE glycoproteins, EPITHELIAL cells, REACTIVE oxygen species, LIPOTEICHOIC acid

Abstract

Intercellular cell adhesion molecule 1 (ICAM-1) is a cell surface glycoprotein with a vital role in the immune response to pathogens. The expression pattern of ICAM-1 is wide ranging, encompassing endothelial cells, epithelial cells, and neutrophils. Recent work has characterized the role of ICAM-1 in murine neutrophils, but the function of human neutrophil ICAM-1 is incompletely understood. Herein, we investigated the expression and role of ICAMs in human neutrophils in vitro and in vivo. Our findings show clear expression of ICAM-1, -3, and -4 on peripheral blood–derived neutrophils and demonstrate that the pathogen-associated molecular pattern lipoteichoic acid is an inducer of ICAM-1 expression in vitro. In vivo, neutrophils obtained from the pleural cavity of patients with a parapneumonic effusion display enhanced expression of ICAM-1 compared with peripheral blood– and oral cavity–derived neutrophils. Moreover, migration of peripheral blood–derived neutrophils across endothelial cells can upregulate neutrophil ICAM-1 expression. These findings indicate that pathogen-associated molecular patterns and/or cytokines, alongside transmigration, enhance neutrophil ICAM-1 expression at sites of inflammation. Mechanistically, we observed that ICAM-1high neutrophils display elevated S. aureus phagocytic capacity. However, unlike murine neutrophils, ICAM-1 intracellular signaling in human neutrophils was not essential for phagocytosis of Staphylococcus aureus and reactive oxygen species generation. Taken together, these results have important implications for the regulation of neutrophil-mediated pathogen clearance. [ABSTRACT FROM AUTHOR]

Published

2024

15. Serum TRPA1 mediates the association between olfactory function and cognitive function.

Author

Xiaoniu Liang, Zhenxu Xiao, Jie Wu, Xiaoxi Ma, Qianhua Zhao, and Ding Ding

Subjects

PEPPERMINT, PEARSON correlation (Statistics), RESEARCH funding, ENZYME-linked immunosorbent assay, SEX distribution, PILOT projects, LOGISTIC regression analysis, DESCRIPTIVE statistics, AGE distribution, MANN Whitney U Test, CHI-squared test, SMELL, ODDS ratio, MEMBRANE glycoproteins, COGNITION disorders, NEUROPSYCHOLOGICAL tests, FACTOR analysis, CONFIDENCE intervals, DATA analysis software, COGNITION, EDUCATIONAL attainment, OLD age

Abstract

Background: Olfactory dysfunction was associated with poorer cognition. However, the association between transient receptor potential cation channel subfamily A member 1 (TRPA1) and cognitive function have not been studied. This study aimed to evaluate the mediation effect of TRPA1 on the association between olfactory and cognitive function among Chinese older adults. Methods: We recruited 121 participants with cognitive impairment (CI) and 135 participants with normal cognition (NC) from a memory clinic and the "Shanghai Aging Study." Olfactory identification of each participant was measured by the Sniffin' Sticks Screening Test 12 (SSST-12). Serum TRPA1 were quantified using the Enzyme-Linked Immunosorbent Assay. The mediation effects of TRPA1 on the association between olfactory function and cognitive function were explored using mediation analysis. Results: The CI group had a significantly higher proportion of the high level of serum TRPA1 (58.7%) than the NC group (42.2%) (p = 0.0086). After adjusted for gender, age, and years of education, mediation analysis verified that TRPA1 partially mediated the association between SSST-12 and Mini Mental State Examination (MMSE). It also verified that TRPA1 partially mediated the association between the identification of peppermint and MMSE. Conclusion: Our study emphasizes the mediation role of TRPA1 in the relationship between olfactory and cognitive function among older adults. Further research is necessary to explore the mechanism of TRPA1 on the relationship between olfactory and cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2024

16. Evaluation of GARP immunohistochemical expression in papillary thyroid carcinoma.

Author

Atia, Esraa Adel Mahmoud Mohamed, Sammour, Sanaa Abd Elmaged, Ibrahim, Eman Abdel-Salam, Abou Gabal, Hoda Hassan, and Elgohary, Shimaa Abdelraouf

Subjects

CROSS-sectional method, EPITHELIAL cells, THYROID gland tumors, T cells, DATA analysis, RECEIVER operating characteristic curves, PAPILLARY carcinoma, IMMUNOTHERAPY, PARAMETERS (Statistics), KRUSKAL-Wallis Test, FISHER exact test, MANN Whitney U Test, DESCRIPTIVE statistics, IMMUNOHISTOCHEMISTRY, GENE expression, MATHEMATICAL statistics, MEMBRANE glycoproteins, ANALYSIS of variance, STATISTICS, COMPARATIVE studies, STAINS & staining (Microscopy), MICROSCOPY, DATA analysis software, REGULATORY T cells, NONPARAMETRIC statistics

Abstract

Background: Glycoprotein A repetitions predominant (GARP) is a novel transmembrane protein highly expressed on the surface of regulatory T cells (Tregs), which are a subset of immunosuppressive T lymphocytes that play a major role in inhibiting the antitumor immune response. Many studies documented increased GARP expression in various tumors, which is related to a poorer prognosis, and only one single paper investigated its expression in thyroid tumors. Aim: To evaluate the immunohistochemical expression of GARP in differentiated thyroid carcinomas and their tumor-infiltrating lymphocytes (TILs) in comparison to its expression in other benign and low-risk lesions. Methods: Sixty-nine cases of different thyroid lesions were subgrouped into 37 cases of malignant thyroid neoplasms, 25 cases of benign thyroid lesions, and 7 cases of low-risk neoplasms collected from the Pathology Department Laboratories of Ain Shams University Hospitals during the period from January 2017 to December 2021 and stained immunohistochemically for GARP. Immunohistochemical (IHC) results were evaluated in thyroid epithelial cells and TILs. The expression of GARP was correlated with the different clinicopathological parameters. Results: GARP expression discloses a significant statistical difference between the three studied groups (P < 0.001). High GARP expression was detected in 89.19% of the malignant cases and in 28.57% of low-risk neoplasms, while all benign lesions exhibited low GARP expression. High GARP expression of TILs was detected in 60% of the malignant cases. Synchronous high GARP expression in tumor tissue and in the surrounding TILs was detected in 63.16% of the malignant cases, yet these results did not reach statistical significance. Conclusion: GARP is a marker of Tregs, whose high expression is increased in malignant over benign and low-risk lesions. It might be a potential novel target for anticancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

17. Turkish coffee has an antitumor effect on breast cancer cells in vitro and in vivo.

Author

Amin, Mohamed N., Abdelmohsen, Usama Ramadan, and Samra, Yara A.

Subjects

*IN vitro studies, *BIOLOGICAL models, *COFFEE, *TRADITIONAL medicine, *COLORIMETRY, *ANTINEOPLASTIC agents, *BREAST tumors, *APOPTOSIS, *CELL proliferation, *ENZYME-linked immunosorbent assay, *IN vivo studies, *OXIDATIVE stress, *DESCRIPTIVE statistics, *CYTOSKELETAL proteins, *PLANT extracts, *CELL lines, *MICE, *GENE expression, *IMMUNOHISTOCHEMISTRY, *ANIMAL experimentation, *MEMBRANE glycoproteins, *ORGANIC compounds, *PEROXISOME proliferator-activated receptors, *CASPASES, *MALONDIALDEHYDE, *PHARMACODYNAMICS

Abstract

Background: Breast cancer is the most diagnosed cancer in women. Its pathogenesis includes several pathways in cancer proliferation, apoptosis, and metastasis. Some clinical data have indicated the association between coffee consumption and decreased cancer risk. However, little data is available on the effect of coffee on breast cancer cells in vitro and in vivo. Methods: In our study, we assessed the effect of Turkish coffee and Fridamycin-H on different pathways in breast cancer, including apoptosis, proliferation, and oxidative stress. A human breast cancer cell line (MCF-7) was treated for 48 h with either coffee extract (5% or 10 v/v) or Fridamycin-H (10 ng/ml). Ehrlich solid tumors were induced in mice for in vivo modeling of breast cancer. Mice with Ehrlich solid tumors were treated orally with coffee extract in drinking water at a final concentration (v/v) of either 3%, 5%, or 10% daily for 21 days. Protein expression levels of Caspase-8 were determined in both in vitro and in vivo models using ELISA assay. Moreover, P-glycoprotein and peroxisome proliferator-activated receptor gamma (PPAR-γ) protein expression levels were analyzed in the in vitro model. β-catenin protein expression was analyzed in tumor sections using immunohistochemical analysis. In addition, malondialdehyde (MDA) serum levels were analyzed using colorimetry. Results: Both coffee extract and Fridamycin-H significantly increased Caspase-8, P-glycoprotein, and PPAR-γ protein levels in MCF-7 cells. Consistently, all doses of in vivo coffee treatment induced a significant increase in Caspase-8 and necrotic zones and a significant decrease in β- catenin, MDA, tumor volume, tumor weight, and viable tumor cell density. Conclusion: These findings suggest that coffee extract and Fridamycin-H warrant further exploration as potential therapies for breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

18. Dual-role epitope on SARS-CoV-2 spike enhances and neutralizes viral entry across different variants.

Author

Ye, Gang, Bu, Fan, Pan, Ruangang, Mendoza, Alise, Saxena, Divyasha, Zheng, Jian, Perlman, Stanley, Liu, Bin, and Li, Fang

Subjects

*SARS-CoV-2 Omicron variant, *VIRUS diseases, *MEMBRANE glycoproteins, *SARS-CoV-2, *GLYCOPROTEINS

Abstract

Grasping the roles of epitopes in viral glycoproteins is essential for unraveling the structure and function of these proteins. Up to now, all identified epitopes have been found to either neutralize, have no effect on, or enhance viral entry into cells. Here, we used nanobodies (single-domain antibodies) as probes to investigate a unique epitope on the SARS-CoV-2 spike protein, located outside the protein's receptor-binding domain. Nanobody binding to this epitope enhances the cell entry of prototypic SARS-CoV-2, while neutralizing the cell entry of SARS-CoV-2 Omicron variant. Moreover, nanobody binding to this epitope enhances both receptor binding activity and post-attachment activity of prototypic spike, explaining the enhanced viral entry. The opposite occurs with Omicron spike, explaining the neutralized viral entry. This study reveals a unique epitope that can both enhance and neutralize viral entry across distinct viral variants, suggesting that epitopes may vary their roles depending on the viral context. Consequently, antibody therapies should be assessed across different viral variants to confirm their efficacy and safety. Author summary: Antibodies bind to specific epitopes on viral surface glycoproteins to perform their function: inhibiting viral infection, having no effect, or, in rare cases, enhancing viral infection. In our research, we used nanobodies (small, single-domain antibodies from camelid animals) as probes and identified a unique epitope on the SARS-CoV-2 spike protein with opposing functions across different SARS-CoV-2 variants. It enhances viral infection in pre-Omicron variants but inhibits it in the Omicron variant. We further investigated the molecular mechanism underlying these opposing effects. Although this epitope is not directly involved in receptor binding, nanobody binding to it modulates receptor binding and post-receptor-binding activities. This study marks the first discovery of a dual-function epitope on the SARS-CoV-2 spike protein that both enhances and inhibits viral infection across different viral variants. This discovery challenges the traditional categorization of epitopes, underscores the complex evolution of the SARS-CoV-2 spike protein, and offers new insights into antiviral antibody therapies. [ABSTRACT FROM AUTHOR]

Published

2024

19. Cellular translocation and secretion of sialidases.

Author

Aljohani, Majdi A., Hiroaki Sasaki, and Xue-Long Sun

Subjects

*MEMBRANE glycoproteins, *CELL physiology, *ENDOPLASMIC reticulum, *SIALIC acids, *GLYCOPROTEINS, *NEURAMINIDASE

Abstract

Sialidases (or neuraminidases) catalyze the hydrolysis of sialic acid (Sia)-containing molecules, mostly the removal of the terminal Sia on glycans (desialylation) of either glycoproteins or glycolipids. Therefore, sialidases can modulate the functionality of the target glycoprotein or glycolipid and are involved in various biological pathways in health and disease. In mammalian cells, there are four kinds of sialidase, which are Neu1, Neu2, Neu3, and Neu4, based on their subcellular locations and substrate specificities. Neu1 is the lysosomal sialidase, Neu2 is the cytosolic sialidase, Neu3 is the plasma membrane-associated sialidase, and Neu4 is found in the lysosome, mitochondria, and endoplasmic reticulum. In addition to specific subcellular locations, sialidases can translocate to different subcellular localizations within particular cell conditions and stimuli, thereby participating in different cellular functions depending on their loci. Lysosomal sialidase Neu1 can translocate to the cell surface upon cell activation in several cell types, including immune cells, platelets, endothelial cells, and epithelial cells, where it desialylates receptors and thus impacts receptor activation and signaling. On the other hand, cells secrete sialidases upon activation. Secreted sialidases can serve as extracellular sialidases and cause the desialylation of both extracellular glycoproteins or glycolipids and cell surface glycoproteins or glycolipids on their own and other cells, thus playing roles in various biological pathways as well. This review discusses the recent advances and understanding of sialidase translocation in different cells and secretion from different cells under different conditions and their involvement in physiological and pathological pathways. [ABSTRACT FROM AUTHOR]

Published

2024

20. A Computational Approach in the Systematic Search of the Interaction Partners of Alternatively Spliced TREM2 Isoforms †.

Author

Liang, Junyi, Menon, Aditya, Tomco, Taylor, Bhattarai, Nisha, Smith, Iris Nira, Khrestian, Maria, Formica, Shane V., Eng, Charis, Buck, Matthias, and Bekris, Lynn M.

Subjects

*MEMBRANE glycoproteins, *ALZHEIMER'S disease, *STRUCTURAL bioinformatics, *NEUROFIBRILLARY tangles, *MYELOID cells

Abstract

Alzheimer's disease is the most common form of dementia, characterized by the pathological accumulation of amyloid-beta (Aβ) plaques and tau neurofibrillary tangles. Triggering receptor expressed on myeloid cells 2 (TREM2) is increasingly recognized as playing a central role in Aβ clearance and microglia activation in AD. The TREM2 gene transcriptional product is alternatively spliced to produce three different protein isoforms. The canonical TREM2 isoform binds to DAP12 to activate downstream pathways. However, little is known about the function or interaction partners of the alternative TREM2 isoforms. The present study utilized a computational approach in a systematic search for new interaction partners of the TREM2 isoforms by integrating several state-of-the-art structural bioinformatics tools from initial large-scale screening to one-on-one corroborative modeling and eventual all-atom visualization. CD9, a cell surface glycoprotein involved in cell–cell adhesion and migration, was identified as a new interaction partner for two TREM2 isoforms, and CALM, a calcium-binding protein involved in calcium signaling, was identified as an interaction partner for a third TREM2 isoform, highlighting the potential role of cell adhesion and calcium regulation in AD. [ABSTRACT FROM AUTHOR]

Published

2024

21. Hydrogen Sulfide Modulation of Matrix Metalloproteinases and CD147/EMMPRIN: Mechanistic Pathways and Impact on Atherosclerosis Progression.

Author

Munteanu, Constantin, Galaction, Anca Irina, Poștaru, Mădălina, Rotariu, Mariana, Turnea, Marius, and Blendea, Corneliu Dan

Subjects

MEMBRANE glycoproteins, VASCULAR smooth muscle, MATRIX metalloproteinases, VASCULAR remodeling, ENDOTHELIUM diseases, ATHEROSCLEROTIC plaque

Abstract

Atherosclerosis is a chronic inflammatory condition marked by endothelial dysfunction, lipid accumulation, inflammatory cell infiltration, and extracellular matrix (ECM) remodeling within arterial walls, leading to plaque formation and potential cardiovascular events. Key players in ECM remodeling and inflammation are matrix metalloproteinases (MMPs) and CD147/EMMPRIN, a cell surface glycoprotein expressed on endothelial cells, vascular smooth muscle cells (VSMCs), and immune cells, that regulates MMP activity. Hydrogen sulfide (H₂S), a gaseous signaling molecule, has emerged as a significant modulator of these processes including oxidative stress mitigation, inflammation reduction, and vascular remodeling. This systematic review investigates the mechanistic pathways through which H₂S influences MMPs and CD147/EMMPRIN and assesses its impact on atherosclerosis progression. A comprehensive literature search was conducted across PubMed, Scopus, and Web of Science databases, focusing on studies examining H₂S modulation of MMPs and CD147/EMMPRIN in atherosclerosis contexts. Findings indicate that H₂S modulates MMP expression and activity through transcriptional regulation and post-translational modifications, including S-sulfhydration. By mitigating oxidative stress, H₂S reduces MMP activation, contributing to plaque stability and vascular remodeling. H₂S also downregulates CD147/EMMPRIN expression via transcriptional pathways, diminishing inflammatory responses and vascular cellular proliferation within plaques. The dual regulatory role of H₂S in inhibiting MMP activity and downregulating CD147 suggests its potential as a therapeutic agent in stabilizing atherosclerotic plaques and mitigating inflammation. Further research is warranted to elucidate the precise molecular mechanisms and to explore H₂S-based therapies for clinical application in atherosclerosis. [ABSTRACT FROM AUTHOR]

Published

2024

22. Alzheimer risk-increasing TREM2 variant causes aberrant cortical synapse density and promotes network hyperexcitability in mouse models.

Author

Das, Melanie, Mao, Wenjie, Voskobiynyk, Yuliya, Necula, Deanna, Lew, Irene, Petersen, Cathrine, Zahn, Allie, Yu, Gui-Qiu, Yu, Xinxing, Smith, Nicholas, Sayed, Faten, Gan, Li, Paz, Jeanne, and Mucke, Lennart

Subjects

Alzheimers disease, Amyloid precursor protein, EEG, Epilepsy, Glia, Hyperexcitability, Microglia, Network dysfunction, Synapses, TREM2, Humans, Animals, Mice, Alzheimer Disease, Alleles, Seizures, Amyloid beta-Peptides, Disease Models, Animal, Plaque, Amyloid, Synapses, Membrane Glycoproteins, Receptors, Immunologic

Abstract

The R47H variant of triggering receptor expressed on myeloid cells 2 (TREM2) increases the risk of Alzheimers disease (AD). To investigate potential mechanisms, we analyzed knockin mice expressing human TREM2-R47H from one mutant mouse Trem2 allele. TREM2-R47H mice showed increased seizure activity in response to an acute excitotoxin challenge, compared to wildtype controls or knockin mice expressing the common variant of human TREM2. TREM2-R47H also increased spontaneous thalamocortical epileptiform activity in App knockin mice expressing amyloid precursor proteins bearing autosomal dominant AD mutations and a humanized amyloid-β sequence. In mice with or without such App modifications, TREM2-R47H increased the density of putative synapses in cortical regions without amyloid plaques. TREM2-R47H did not affect synaptic density in hippocampal regions with or without plaques. We conclude that TREM2-R47H increases AD-related network hyperexcitability and that it may do so, at least in part, by causing an imbalance in synaptic densities across brain regions.

Published

2023

23. Frontotemporal dementia presentation in patients with heterozygous p.H157Y variant of TREM2.

Author

Ogonowski, Natalia, Santamaria-Garcia, Hernando, Baez, Sandra, Lopez, Andrea, Laserna, Andrés, Garcia-Cifuentes, Elkin, Ayala-Ramirez, Paola, Zarante, Ignacio, Suarez-Obando, Fernando, Reyes, Pablo, Kauffman, Marcelo, Cochran, Nick, Schulte, Michael, Kosik, Kenneth, Matallana, Diana, Ibáñez, Agustín, Spina, Salvatore, Miller, Bruce, Yokoyama, Jennifer, and Sirkis, Daniel

Subjects

Genetics, Neurodegenerative Diseases, Neurology, Humans, Frontotemporal Dementia, Alzheimer Disease, Brain, Atrophy, Membrane Glycoproteins, Receptors, Immunologic

Abstract

BACKGROUND: The triggering receptor expressed on myeloid cell 2 (TREM2) is a major regulator of neuroinflammatory processes in neurodegeneration. To date, the p.H157Y variant of TREM2 has been reported only in patients with Alzheimers disease. Here, we report three patients with frontotemporal dementia (FTD) from three unrelated families with heterozygous p.H157Y variant of TREM2: two patients from Colombian families (study 1) and a third Mexican origin case from the USA (study 2). METHODS: To determine if the p.H157Y variant might be associated with a specific FTD presentation, we compared in each study the cases with age-matched, sex-matched and education-matched groups-a healthy control group (HC) and a group with FTD with neither TREM2 mutations nor family antecedents (Ng-FTD and Ng-FTD-MND). RESULTS: The two Colombian cases presented with early behavioural changes, greater impairments in general cognition and executive function compared with both HC and Ng-FTD groups. These patients also exhibited brain atrophy in areas characteristic of FTD. Furthermore, TREM2 cases showed increased atrophy compared with Ng-FTD in frontal, temporal, parietal, precuneus, basal ganglia, parahippocampal/hippocampal and cerebellar regions. The Mexican case presented with FTD and motor neuron disease (MND), showing grey matter reduction in basal ganglia and thalamus, and extensive TDP-43 type B pathology. CONCLUSION: In all TREM2 cases, multiple atrophy peaks overlapped with the maximum peaks of TREM2 gene expression in crucial brain regions including frontal, temporal, thalamic and basal ganglia areas. These results provide the first report of an FTD presentation potentially associated with the p.H157Y variant with exacerbated neurocognitive impairments.

Published

2023

24. No evidence of spread of Linda pestivirus in the wild boar population in Southern Germany.

Author

Schulz, Doreen, Aebischer, Andrea, Wernike, Kerstin, and Beer, Martin

Subjects

*CLASSICAL swine fever virus, *WILD boar, *MEMBRANE glycoproteins, *VIRAL antibodies, *REVERSE genetics

Abstract

Lateral-shaking inducing neuro-degenerative agent virus (LindaV) is a novel member of the highly diverse genus Pestivirus within the family Flaviviridae. LindaV was first detected in Austria in 2015 and was associated with congenital tremor in piglets. Since then, the virus or specific antibodies have been found in a few further pig farms in Austria. However, the actual spatial distribution and the existence of reservoir hosts is largely unknown. Since other pestiviruses of pigs such as classical swine fever virus or atypical porcine pestivirus can also infect wild boar, the question arises whether LindaV is likewise present in the wild boar population. Therefore, we investigated the presence of neutralizing antibodies against LindaV in 200 wild boar samples collected in Southern Germany, which borders Austria. To establish a serological test system, we made use of the interchangeability of the surface glycoproteins and created a chimeric pestivirus using Bungowannah virus (species Pestivirus australiaense) as synthetic backbone. The E1 and E2 glycoproteins were replaced by the heterologous E1 and E2 of LindaV resulting in the chimera BV_E1E2_LV. Viable virus could be rescued and was subsequently applied in a neutralization test. A specific positive control serum generated against the E2 protein of LindaV gave a strong positive result, thereby confirming the functionality of the test system. All wild boar samples, however, tested negative. Hence, there is no evidence that LindaV has become highly prevalent in the wild boar population in Southern Germany. [ABSTRACT FROM AUTHOR]

Published

2024

25. A Nitroreductase‐Activatable Metabolic Reporter for Covalent Labeling of Pathological Hypoxic Cells in Tumorigenesis.

Author

Wang, Zhimin, Lau, Jun Wei, Liu, Songhan, Ren, Ziheng, Gong, Zhiyuan, Liu, Xiaogang, and Xing, Bengang

Subjects

*MEMBRANE glycoproteins, *CHEMICAL reactions, *NEOPLASTIC cell transformation, *HYPOXEMIA, *COMPANION diagnostics

Abstract

Aberrant hypoxic stress will initiate a cascade of pathological consequence observed prominently in tumorigenesis. Understanding of hypoxia's role in tumorigenesis is highly essential for developing effective therapeutics, which necessitates reliable tools to specifically distinguish hypoxic tumor cells (or tissues) and correlate their dynamics with the status of disease in complex living settings for precise theranostics. So far, disparate hypoxia‐responsive probe molecules and prodrugs were designed via chemical or enzymatic reactions, yet their capability in real‐time reporting pathogenesis development is often compromised due to unrestricted diffusion and less selectivity towards the environmental responsiveness. Herein we present an oxygen‐insensitive nitroreductase (NTR)‐activatable glycan metabolic reporter (pNB‐ManNAz) capable of covalently labeling hypoxic tumor cells and tissues. Under pathophysiological hypoxic environments, the caged non‐metabolizable precursor pNB‐ManNAz exhibited unique responsiveness to cellular NTR, culminating in structural self‐immolation and the resultant ManNAz could incorporate onto cell surface glycoproteins, thereby facilitating fluorescence labeling via bioorthogonal chemistry. This NTR‐responsive metabolic reporter demonstrated broad applicability for multicellular hypoxia labeling, particularly in the dynamic monitoring of orthotopic tumorigenesis and targeted tumor phototherapy in vivo. We anticipate that this approach holds promise for investigating hypoxia‐related pathological progression, offering valuable insights for accurate diagnosis and treatment. [ABSTRACT FROM AUTHOR]

Published

2024

26. Adaptation potential of H3N8 canine influenza virus in human respiratory cells.

Author

Sekine, Wataru, Kamiki, Haruhiko, Ishida, Hiroho, Matsugo, Hiromichi, Ohira, Kosuke, Li, Kaixin, Katayama, Misa, Takenaka-Uema, Akiko, Murakami, Shin, and Horimoto, Taisuke

Subjects

*REVERSE genetics, *MEMBRANE glycoproteins, *GREYHOUND racing, *DOGS, *MEMBRANE fusion, *AVIAN influenza, *INFLUENZA viruses, *INFLUENZA A virus

Abstract

In 2004, the equine-origin H3N8 canine influenza virus (CIV) first caused an outbreak with lethal cases in racing greyhounds in Florida, USA, and then spread to domestic dogs nationwide. Although transmission of this canine virus to humans has not been reported, it is important to evaluate its zoonotic potential because of the high contact opportunities between companion dogs and humans. To gain insight into the interspecies transmissibility of H3N8 CIV, we tested its adaptability to human respiratory A549 cells through successive passages. We found that CIV acquired high growth properties in these cells mainly through mutations in surface glycoproteins, such as hemagglutinin (HA) and neuraminidase (NA). Our reverse genetics approach revealed that HA2-K82E, HA2-R163K, and NA-S18L mutations were responsible for the increased growth of CIV in human cells. Molecular analyses revealed that both HA2 mutations altered the optimum pH for HA membrane fusion activity and that the NA mutation changed the HA-NA functional balance. These findings suggest that H3N8 CIV could evolve into a human pathogen with pandemic potential through a small number of mutations, thereby posing a threat to public health in the future. [ABSTRACT FROM AUTHOR]

Published

2024

27. A monoclonal antibody that recognizes a unique 13-residue epitope in the cytoplasmic tail of HLA-E.

Author

Verhaar, Elisha R., Gan, Jin, Buhl, Susan, Li, Ziao, Horowitz, Amir, and Ploegh, Hidde L.

Subjects

*MONOCLONAL antibodies, *STREPTAVIDIN, *MEMBRANE glycoproteins, *NON-muscle invasive bladder cancer

Abstract

The Class I MHC molecule (MHC-I) HLA-E presents peptides that are derived from the signal sequences, either those of other MHC-I products, or of viral type I membrane glycoproteins. Monoclonal antibodies with proven specificity for HLA-E, and with no cross-reactions with other MHC-I products, have yet to be described. To obtain anti-HLA-E-specific antibodies suitable for a range of applications, we generated monoclonal antibodies against a unique feature of HLA-E: its cytoplasmic tail. We created an immunogen by performing an enzymatically catalyzed transpeptidation reaction to obtain a fusion of the cytoplasmic tail of HLA-E with a nanobody that recognizes murine Class II MHC (MHC-II) products. We obtained a mouse monoclonal antibody that recognizes a 13-residue stretch in the HLA-E cytoplasmic tail. We cloned the genes that encode this antibody in expression vectors to place an LPETG sortase recognition motif at the C-terminus of the heavy and light chains. This arrangement allows the site-specific installation of fluorophores or biotin at these C-termini. The resulting immunoglobulin preparations, labeled with 4 equivalents of a fluorescent or biotinylated payload of choice, can then be used for direct immunofluorescence or detection of the tag by fluorescence or by streptavidin-based methods. We also show that the 13-residue sequence can serve as an epitope tag, independent of the site of its placement within a protein's sequence. The antibody can be used diagnostically to stain for HLA-E on patient tumor samples, it can be used as an antibody-epitope tag for extracellular proteins, and it enables research into the unique role of the cytoplasmic tail of HLA-E. • Mouse monoclonal antibody recognizes 13-residue stretch in the HLA-E cytoplasmic tail. • mAb can be modified directly with fluorophores or biotin with sortase. • mAb stains HLA-E on tumor samples with high affinity and specificity. • mAb recognizes HLA-E in flow cytometry, immunoblot, IP, IHC, and IF. • mAb can be used as antibody-epitope tag for extracellular proteins. [ABSTRACT FROM AUTHOR]

Published

2024

28. Sialic acid in the regulation of blood cell production, differentiation and turnover.

Author

Irons, Eric Edward, Gc, Sajina, and Lau, Joseph T. Y.

Subjects

*SIALIC acids, *GLYCOLIPIDS, *MEMBRANE glycoproteins, *CELLULAR control mechanisms, *BLOOD cells, *POST-translational modification

Abstract

Sialic acid is a unique sugar moiety that resides in the distal and most accessible position of the glycans on mammalian cell surface and extracellular glycoproteins and glycolipids. The potential for sialic acid to obscure underlying structures has long been postulated, but the means by which such structural changes directly affect biological processes continues to be elucidated. Here, we appraise the growing body of literature detailing the importance of sialic acid for the generation, differentiation, function and death of haematopoietic cells. We conclude that sialylation is a critical post‐translational modification utilized in haematopoiesis to meet the dynamic needs of the organism by enforcing rapid changes in availability of lineage‐specific cell types. Though long thought to be generated only cell‐autonomously within the intracellular ER‐Golgi secretory apparatus, emerging data also demonstrate previously unexpected diversity in the mechanisms of sialylation. Emphasis is afforded to the mechanism of extrinsic sialylation, whereby extracellular enzymes remodel cell surface and extracellular glycans, supported by charged sugar donor molecules from activated platelets. [ABSTRACT FROM AUTHOR]

Published

2024

29. Multifunctional aptamer grafted targeted nano‐drugs execute molecular cross‐talks with cancer cells.

Author

Manna, Sounik, Mahata, Rumi, Dey, Surya K., Das Chaudhuri, Angsuman, and Choudhury, Sujata M.

Subjects

EPIDERMAL growth factor receptors, MEMBRANE glycoproteins, CANCER chemotherapy, TARGETED drug delivery, NUCLEOLIN, APTAMERS

Abstract

The biggest obstacles in treating cancer with traditional chemotherapy are unpleasant side effects and drug resistance. A growing amount of interest has been exhibited in using aptamers as target ligands for targeted cancer therapy and specific cancer cell identification due to their distinct benefits. Aptamer‐conjugated nano‐materials have recently provided new prospects in cancer treatment with their improved therapeutic efficacy and capability of reducing toxicity. Consequently, they are not perceived as alien substances our body, which allows their comfortable acceptance. Several tumor markers such as nucleolin, mucin, and the epidermal growth factor receptor can be effectively recognized by aptamers. In addition, glycoproteins on the surface of tumor cells can be recognized using aptamers. So surface modification of drug by aptamer are accomplished for enhanced tumor‐specific recognition by which drug‐specific accretion, internalization, and drug retention in tumors increased through specific ligand‐mediated interactions and thus therapeutic index is increased. Here, we highlight some promising classes of aptamer‐conjugated nanoparticles for the specific recognition of cancer cells and targeted drug delivery and the molecular mechanism and immunomodulatory regulation of these aptamer have been focused. [ABSTRACT FROM AUTHOR]

Published

2024

30. Investigation of the Diagnostic Value of Cerebrospinal Fluid and Serum sTREM-1 Levels in Neonatal Meningitis.

Author

Çakır, Salih Çağrı, Dorum, Bayram Ali, Özkan, Hilal, Köksal, Nilgün, Kocael, Fatma, Budak, Ferah, Hacımustafaoğlu, Mustafa, Çelebi, Solmaz, Kızmaz, Muhammed Ali, Sivrikaya Yıldırım, Cansu, and Üstün Elmas, Kevser

Subjects

MENINGITIS diagnosis, CEREBROSPINAL fluid examination, ANTIBIOTICS, ACADEMIC medical centers, T-test (Statistics), RECEIVER operating characteristic curves, RESEARCH funding, MENINGITIS, NEONATAL intensive care units, NEONATAL intensive care, DESCRIPTIVE statistics, MANN Whitney U Test, CHI-squared test, LONGITUDINAL method, IMMUNOLOGIC receptors, MEMBRANE glycoproteins, DATA analysis software, SENSITIVITY & specificity (Statistics), NEONATAL sepsis, BLOOD, CHILDREN

Abstract

Background: The aim of this study is to investigate the diagnostic value of cerebrospinal fluid (CSF) and serum levels of the soluble form of triggering receptor-1 expressed on myeloid cells (sTREM-1) in neonatal meningitis. Methods: Serum sTREM-1 levels were measured in all neonatal sepsis patients at the start of antibiotic therapy and the 48th hour of treatment. At the beginning of antibiotic therapy, CSF samples were collected for sTREM-1 measurements. Control CSF samples were also collected from the patients with meningitis at the 48th hour of treatment. Results: A total of 77 preterm (50) and term (27) patients with neonatal sepsis were included in the study. There was no significant difference between the CSF sTREM-1 levels of patients with and without meningitis. The CSF sTREM-1 levels of preterm infants with meningitis decreased significantly after treatment (p = 0.038). Although the CSF/serum sTREM-1 ratios tended to increase in babies with meningitis, no significant difference was found between the groups. CSF/serum sTREM-1 ratios (mean ± SD) were 1.42 ± 0.91 and 1.14 ± 0.85 in preterm babies with and without meningitis and 1.15 ± 0.97 and 0.97 ± 0.55 in term babies with and without meningitis, respectively. Conclusions: Serum and CSF sTREM-1 levels increase in patients with neonatal sepsis. CSF s-TREM-1 levels decrease after treatment in preterm infants with meningitis. [ABSTRACT FROM AUTHOR]

Published

2024

31. Investigation of Saliva Parameters and Tissue Factor in Healthy Individuals Who Had Survived COVID-19 Infection.

Author

Oktay, Şehkar, Arslan, Eren, Akyol, Gökçe, Kaya, Saliha, and Karatepe, Füsun

Subjects

MEDICAL sciences, COVID-19, COVID-19 pandemic, SARS-CoV-2, MEMBRANE glycoproteins, XEROSTOMIA, BAD breath

Published

2024

32. 소아 시신경염.

Author

Surl, Dongheon and Han, Jinu

Subjects

ADRENOCORTICAL hormones, INTRAVENOUS immunoglobulins, MULTIPLE sclerosis, MAGNETIC resonance imaging, OPTIC neuritis, PEDIATRICS, MEMBRANE glycoproteins, DEMYELINATION, SERODIAGNOSIS, BIOMARKERS, SYMPTOMS

Abstract

Background: Pediatric optic neuritis is a demyelinating optic nerve inflammation in children, characterized by acute vision loss and visual field defects, often accompanied by eye movement pain, color vision abnormalities, and relative afferent pupillary defects. It can manifest as an isolated episode or as part of broader demyelinating disorders such as multiple sclerosis (MS), neuromyelitis optica spectrum disorder (NMOSD), and myelin oligodendrocyte glycoprotein (MOG) antibody-associated disease. Its incidence varies globally, with recent studies defining it as optic neuritis in individuals aged <16 years. Current Concepts: Pediatric optic neuritis has distinct clinical features compared to its adult counterpart, particularly in presentation patterns and associated systemic diseases. Children often experience greater visual acuity deficits and are more likely to develop bilateral eye involvement, severe optic disc swelling, and accompanying encephalopathic features than adults. Epidemiological studies have shown that it is relatively rare, with varying incidence rates across different regions. Diagnostic criteria are primarily based on clinical assessment, magnetic resonance imaging findings, and serological tests, including antibodies against specific biomarkers such as anti-MOG and anti-aquaporin-4 antibodies. Treatment strategies for pediatric optic neuritis involve high-dose corticosteroids followed by tapering and, in severe cases, plasma exchange or intravenous immunoglobulins. Long-term management may require immunosuppressants or biological agents, particularly in cases progressing to MS or NMOSD. Discussion and Conclusion: Understanding the unique aspects of pediatric optic neuritis is crucial for appropriate management and improving outcomes. Further studies are needed to refine diagnostic and therapeutic approaches for this condition. [ABSTRACT FROM AUTHOR]

Published

2024

33. 생체표지자로 진단되는 급성 시신경염.

Author

Lee, Haeng-Jin

Subjects

NEUROMYELITIS optica, MULTIPLE sclerosis, POSTVACCINAL encephalitis, EARLY medical intervention, OPTIC neuritis, NERVE tissue proteins, MEMBRANE glycoproteins, BIOMARKERS

Abstract

Background: Optic neuritis, an inflammation of the optic nerve, commonly occurs in young adults and often associated with demyelinating diseases, such as multiple sclerosis (MS), neuromyelitis optica spectrum disorder (NMOSD), myelin oligodendrocyte glycoprotein antibody disease (MOGAD), and acute disseminated encephalomyelitis. These conditions frequently exhibit recurrent and progressive inflammatory episodes, significantly impacting prognosis. Differentiating these diseases is crucial because of their distinct clinical presentations, treatment responses, and outcomes. Recent advancements in biomarkers, such as aquaporin-4 (AQP4) and myelin oligodendrocyte glycoprotein (MOG) antibodies, have enhanced diagnostic precision. Current Concepts: The introduction of AQP4 and MOG-immunoglobulin G (IgG) antibody testing has revolutionized diagnostic approaches for optic neuritis. AQP4-IgG is a highly specific marker for NMOSD, facilitating early diagnosis, essential for timely intervention and improved patient outcomes. MOG-IgG has been identified as a distinct marker for MOGAD, differentiating it from MS and NMOSD. These biomarkers aid in understanding the pathophysiological mechanisms underlying optic neuritis and in tailoring individualized treatment strategies. Discussion and Conclusion: The use of AQP4 and MOG-IgG antibodies represents a significant leap forward in managing optic neuritis. These biomarkers not only assist in accurate diagnosis but also provide insights into disease prognosis and therapeutic responses. Future studies should focus on the detailed clinical and pathological characteristics associated with these biomarkers to refine treatment protocols further and enhance patient care. Continued advancements in biomarker research hold promise for the development of new therapeutic avenues and the potential for improved long-term outcomes in patients with optic neuritis. [ABSTRACT FROM AUTHOR]

Published

2024

34. ABCA1 Deletion Does Not Affect Aqueous Humor Outflow Function in Mice.

Author

Qin, Bo, Hu, Chunchun, Zhang, Youjia, Chen, Yuhong, Lei, Yuan, and Cagini, Carlo

Subjects

*MEMBRANE transport proteins, *BIOLOGICAL models, *RESEARCH funding, *ANTERIOR chamber (Eye), *OPTICAL coherence tomography, *REVERSE transcriptase polymerase chain reaction, *MICE, *MESSENGER RNA, *GENE expression, *MEMBRANE glycoproteins, *ANIMAL experimentation, *SLIT lamp microscopy, *TONOMETRY, *ENUCLEATION of the eye, *WESTERN immunoblotting, *GENETIC mutation, *AQUEOUS humor, *STAINS & staining (Microscopy), *PHENOTYPES

Abstract

Background. ATP binding cassette transporter A1 (ABCA1) is a candidate gene within a POAG susceptibility locus by GWAS analysis, and it is involved in IOP modulation via the Cav1/eNOS/NO signaling pathway. We aim to examine the phenotype of ABCA1 deletion in the ABCA1 gene knockout (Abca1−/−) mice. Methods. The anterior segments of Abca1−/− eyes were imaged by slit‐lamp microscopy and anterior segment OCT. IOPs were measured by rebound tonometry. By perfusing enucleated eyes at various pressures, the aqueous humor outflow facility was determined. The mRNA expressions of ABCA1, Cav1, and eNOS were measured by RT‐qPCR. The protein expressions were analyzed by western blot and immunofluorescence staining. Results. There was no significant difference in the anterior segment morphology of Abca1−/− mice. IOP and aqueous humor outflow facility did not change in Abca1−/− mice compared with wild‐type mice. mRNA and protein expressions of ABCA1 were significantly lower in the outflow tissue of Abca1−/− eyes. The expressions of Cav1 and eNOS were both significantly upregulated in the outflow tissue of Abca1−/− eyes. Conclusion. ABCA1 deletion does not affect IOP and aqueous humor outflow function but the Cav1/eNOS/NO pathway is changed in Abca1−/− mice. The function of ABCA1 in aqueous humor outflow still requires further research. [ABSTRACT FROM AUTHOR]

Published

2024

35. Induction of acrosome reaction by 4-Br-A23187 alters the glycoproteomic profile of boar spermatozoa.

Author

Martín-Hidalgo, David, Izquierdo, Mercedes, Garrido, Nicolás, Bartolomé-García, Paloma, Macías-García, Beatriz, and González-Fernández, Lauro

Subjects

*ACROSOME reaction, *MEMBRANE proteins, *SPERMATOZOA, *MEMBRANE glycoproteins, *BOARS, *LECTINS, *SERINE/THREONINE kinases

Abstract

Protein glycosylation is a post-translational modification involved in wide range of biological processes. In mammalian spermatozoa this modification has been identified in numerous proteins, and membrane glycoproteins are involved in the fertilization process. The objective of the present study was to identify changes in protein glycosylation after acrosome reaction (AR) induction using the 4-Br-A23187 ionophore. Our results showed that treatment with 10 μM of 4-Br-A23187 for 20 min significantly increased the percentage of live acrosome-reacted spermatozoa compared to the control (69.8 ± 0.8 vs. 6.4 ± 0.5; mean % ± SEM, respectively). Also, we observed an increase in 32 kDa tyrosine-phosphorylated protein (p32) and a decrease in serine/threonine phosphorylation of the protein kinase A substrates (phospho-PKA-substrates) after ionophore treatment. Furthermore, changes in glycosylated proteins following AR induction were analyzed using different HRP-conjugated lectins (GNA, DSA, and SNA), revealing changes in mannose and sialic acid residues. Proteomic analysis of isolated proteins using GNA lectin revealed that 50 proteins exhibited significantly different abundance (q-value < 0.01). Subsequent analysis using Uniprot database identified 39 downregulated and 11 upregulated proteins in the presence of 4-Br-A23187. Notably, six of these proteins were classified as transmembrane proteins, namely LRRC37A/B like protein 1 C-terminal domain-containing protein, Membrane metalloendopeptidase like 1, VWFA domain-containing protein, Syndecan, Membrane spanning 4-domains A14 and Serine protease 54. This study shows a novel protocol to induce acrosome reaction in boar spermatozoa and identifies new transmembrane proteins containing mannose residues. Further work is needed to elucidate the role of these proteins in sperm-oocyte fusion. • Incubation with 4-Br-A23187 for 20 min induces acrosome reaction in boar spermatozoa. • Glycosylated protein profile changes after acrosome reaction induction. • 50 proteins containing mannose residues showed regulation after acrosome reaction. • 6 transmembrane proteins containing mannose residues were regulated. [ABSTRACT FROM AUTHOR]

Published

2024

36. Proteolytic cleavage of the TGFβ co‐receptor CD109 changes its conformation, resulting in protease inhibition via activation of its thiol ester, and dissociation from the cell membrane.

Author

Jensen, Kathrine Tejlgård, Nielsen, Nadia Sukusu, Viana Almeida, Ana, Thøgersen, Ida B., Enghild, Jan J., and Harwood, Seandean Lykke

Subjects

*MEMBRANE glycoproteins, *TRANSFORMING growth factors, *ESTERS, *PEPTIDE bonds, *PROTEOLYTIC enzymes

Abstract

The glycosylphosphatidylinositol (GPI)‐anchored protein cluster of differentiation 109 (CD109) is expressed on many human cell types and modulates the transforming growth factor β (TGF‐β) signaling network. CD109 belongs to the alpha‐macroglobulin family of proteins, known for their protease‐triggered conformational changes. However, the effect of proteolysis on CD109 and its conformation are unknown. Here, we investigated the interactions of CD109 with proteases. We found that a diverse selection of proteases cleaved peptide bonds within the predicted bait region of CD109, inducing a conformational change that activated the thiol ester of CD109. We show CD109 was able to conjugate proteases with this thiol ester and decrease their activity toward protein substrates, demonstrating that CD109 is a protease inhibitor. We additionally found that CD109 has a unique mechanism whereby its GPI‐anchored macroglobulin 8 (MG8) domain dissociates during its conformational change, allowing proteases to release CD109 from the cell surface by a precise mechanism and not unspecific shedding. We conclude that proteolysis of the CD109 bait region affects both its structure and location, and that interactions between CD109 and proteases may be important to understanding its functions, for example, as a TGF‐β co‐receptor. [ABSTRACT FROM AUTHOR]

Published

2024

37. Highlights in IBS-C From Digestive Disease Week 2024.

Author

Brenner, Darren M.

Subjects

IRRITABLE colon, PATIENT safety, TREATMENT effectiveness, MEMBRANE glycoproteins, DRUG efficacy, GASTROINTESTINAL agents, CONSTIPATION

Published

2024

38. Longitudinal assessment of human antibody binding to hemagglutinin elicited by split-inactivated influenza vaccination over six consecutive seasons.

Author

Carlock, Michael A., Allen, James D., Hanley, Hannah B., and Ross, Ted M.

Subjects

*INFLUENZA vaccines, *VACCINE effectiveness, *SEASONAL influenza, *MEMBRANE glycoproteins, *HEMAGGLUTININ

Abstract

Participants between the ages of 10–86 years old were vaccinated with split-inactivated influenza vaccine (Fluzone®) in six consecutive influenza seasons from 2016–2017 to 2021–2022. Vaccine effectiveness varies from season to season as a result of both host immune responses as well as evolutionary changes in the influenza virus surface glycoproteins that provide challenges to vaccine manufacturers to produce more effective annual vaccines. Next generation influenza vaccines are in development and may provide protective immune responses against a broader number of influenza viruses and reduce the need for annual vaccination. An improved understanding how current influenza vaccines are influenced by human host immune responses in people of different ages and co-morbidities is necessary for designing the next-generation of 'universal' or broadly-protective influenza vaccines. Overall, pre-existing immune responses to previous influenza virus exposures, either by past infections or vaccinations, is a critical factor influencing host responses to seasonal influenza vaccination. Participants vaccinated in consecutive seasons had reduced serum hemagglutination-inhibition (HAI) activity against strains included in the vaccine compared to participants that had not been vaccinated in the preceding 1–2 years prior to entering this study. The magnitude and breadth of these antibody responses were also modulated by the age of the participant. Elderly participants over 65 years of age, in general, had lower pre-existing HAI titers each season prior to vaccination with lower post-vaccination titers compared to children or young adults under the age of 35. The administration of higher doses (HD) of the split-inactivated vaccine enhanced the antibody titers in the elderly. This report showcases 6 consecutive years of antibody HAI activity in human subjects receiving seasonal split-inactivated influenza vaccine. [ABSTRACT FROM AUTHOR]

Published

2024

39. Decoding sTREM2: its impact on Alzheimer’s disease – a comprehensive review of mechanisms and implications.

Author

Cui Lin, Yu Kong, Qian Chen, Jixiang Zeng, Xiaojin Pan, and Jifei Miao

Subjects

ALZHEIMER'S disease diagnosis, BIOLOGICAL models, MYELOID cells, NEUROINFLAMMATION, CELLULAR signal transduction, MEMBRANE glycoproteins, MEDICAL research, BIOMARKERS, DISEASE progression

Abstract

Soluble Triggering Receptor Expressed on Myeloid Cells 2 (sTREM2) plays a crucial role in the pathogenesis of Alzheimer’s disease (AD). This review comprehensively examines sTREM2’s involvement in AD, focusing on its regulatory functions in microglial responses, neuroinflammation, and interactions with key pathological processes. We discuss the dynamic changes in sTREM2 levels in cerebrospinal fluid and plasma throughout AD progression, highlighting its potential as a therapeutic target. Furthermore, we explore the impact of genetic variants on sTREM2 expression and its interplay with other AD risk genes. The evidence presented in this review suggests that modulating sTREM2 activity could influence AD trajectory, making it a promising avenue for future research and drug development. By providing a holistic understanding of sTREM2’s multifaceted role in AD, this review aims to guide future studies and inspire novel therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

40. Determining the Affinity and Kinetics of Small Molecule Inhibitors of Galectin-1 Using Surface Plasmon Resonance.

Author

Kim, Henry, Kretz, Louis, Ronin, Céline, Starck, Christina, Roper, James A., Kahl-Knutson, Barbro, Peterson, Kristoffer, Leffler, Hakon, Nilsson, Ulf J., Pedersen, Anders, Zetterberg, Fredrik R., and Slack, Robert J.

Subjects

*SMALL molecules, *MEMBRANE glycoproteins, *CELL receptors, *SURFACE plasmon resonance, *DRUG discovery, *PHOSPHOLIPID antibodies, *LECTINS, *BINDING constant

Abstract

The beta-galactoside-binding mammalian lectin galectin-1 can bind, via its carbohydrate recognition domain (CRD), to various cell surface glycoproteins and has been implicated in a range of cancers. As a consequence of binding to sugar residues on cell surface receptors, it has been shown to have a pleiotropic effect across many cell types and mechanisms, resulting in immune system modulation and cancer progression. As a result, it has started to become a therapeutic target for both small and large molecules. In previous studies, we used fluorescence polarization (FP) assays to determine KD values to screen and triage small molecule glycomimetics that bind to the galectin-1 CRD. In this study, surface plasmon resonance (SPR) was used to compare human and mouse galectin-1 affinity measures with FP, as SPR has not been applied for compound screening against this galectin. Binding affinities for a selection of mono- and di-saccharides covering a 1000-fold range correlated well between FP and SPR assay formats for both human and mouse galectin-1. It was shown that slower dissociation drove the increased affinity at human galectin-1, whilst faster association was responsible for the effects in mouse galectin-1. This study demonstrates that SPR is a sound alternative to FP for early drug discovery screening and determining affinity estimates. Consequently, it also allows association and dissociation constants to be measured in a high-throughput manner for small molecule galectin-1 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2024

41. Association of soluble TREM2 with Alzheimer's disease and mild cognitive impairment: a systematic review and meta-analysis.

Author

Ruiqi Wang, Yijun Zhan, Wenyan Zhu, Qianwen Yang, and Jian Pei

Subjects

MEDICAL information storage & retrieval systems, ALZHEIMER'S disease, MILD cognitive impairment, RESEARCH funding, SCIENTIFIC observation, META-analysis, DESCRIPTIVE statistics, SYSTEMATIC reviews, MEDLINE, MEMBRANE glycoproteins, MEDICAL databases, NEUROPSYCHOLOGICAL tests, ONLINE information services, CONFIDENCE intervals, COMPARATIVE studies, QUALITY assurance, DATA analysis software, DISEASE progression

Abstract

Objective: Soluble triggering receptor expressed on myeloid cells 2 (sTREM2) is a potential neuroinflammatory biomarker linked to the pathogenesis of Alzheimer's disease (AD) and mild cognitive impairment (MCI). Previous studies have produced inconsistent results regarding sTREM2 levels in various clinical stages of AD. This study aims to establish the correlation between sTREM2 levels and AD progression through a meta-analysis of sTREM2 levels in cerebrospinal fluid (CSF) and blood. Methods: Comprehensive searches were conducted in PubMed, Embase, Web of Science, and the Cochrane Library to identify observational studies reporting CSF and blood sTREM2 levels in AD patients, MCI patients, and healthy controls. A random effects meta-analysis was used to calculate the standardized mean difference (SMD) and 95% confidence intervals (CIs). Results: Thirty-six observational studies involving 3,016 AD patients, 3,533 MCI patients, and 4,510 healthy controls were included. CSF sTREM2 levels were significantly higher in both the AD [SMD = 0.28, 95% CI (0.15, 0.41)] and MCI groups [SMD = 0.30, 95% CI (0.13, 0.47)] compared to the healthy control group. However, no significant differences in expression were detected between the AD and MCI groups [SMD = 0.09, 95% CI (-0.09, 0.26)]. Furthermore, increased plasma sTREM2 levels were associated with a higher risk of AD [SMD = 0.42, 95% CI (0.01, 0.83)]. Conclusion: CSF sTREM2 levels are positively associated with an increased risk of AD and MCI. Plasma sTREM2 levels were notably higher in the AD group than in the control group and may serve as a promising biomarker for diagnosing AD. However, sTREM2 levels are not effective for distinguishing between different disease stages of AD. Further investigations are needed to explore the longitudinal changes in sTREM2 levels, particularly plasma sTREM2 levels, during AD progression. [ABSTRACT FROM AUTHOR]

Published

2024

42. A 21‐bp deletion in the complement regulator CD55 promotor region is associated with multifocal motor neuropathy and its disease course.

Author

Bos, Jeroen W., Groen, Ewout J. N., Otten, Henny G., Budding, Kevin, van Eijk, Ruben P. A., Curial, Chantall, Kardol‐Hoefnagel, Tineke, Goedee, H. Stephan, van den Berg, Leonard H., and van der Pol, W. Ludo

Subjects

*COMPLEMENT (Immunology), *PROMOTERS (Genetics), *DESCRIPTIVE statistics, *GENETIC polymorphisms, *MEMBRANE glycoproteins, *POLYNEUROPATHIES, *COMPARATIVE studies, *CONFIDENCE intervals, *MOTOR neuron diseases, *SEQUENCE analysis, *GENOTYPES

Abstract

Background and Aims: To further substantiate the role of antibody‐mediated complement activation in multifocal motor neuropathy (MMN) immunopathology, we investigated the distribution of promotor polymorphisms of genes encoding the membrane‐bound complement regulators CD46, CD55, and CD59 in patients with MMN and controls, and evaluated their association with disease course. Methods: We used Sanger sequencing to genotype five common polymorphisms in the promotor regions of CD46, CD55, and CD59 in 133 patients with MMN and 380 controls. We correlated each polymorphism to clinical parameters. Results: The genotype frequencies of rs28371582, a 21‐bp deletion in the CD55 promotor region, were altered in patients with MMN as compared to controls (p.009; Del/Del genotype 16.8% vs. 7.7%, p.005, odds ratio: 2.43 [1.27–4.58]), and patients carrying this deletion had a more favorable disease course (mean difference 0.26 Medical Research Council [MRC] points/year; 95% confidence interval [CI]: 0.040–0.490, p.019). The presence of CD59 rs141385724 was associated with less severe pre‐diagnostic disease course (mean difference 0.940 MRC point/year; 95% CI: 0.083–1.80, p.032). Interpretation: MMN susceptibility is associated with a 21‐bp deletion in the CD55 promotor region (rs2871582), which is associated with lower CD55 expression. Patients carrying this deletion may have a more favorable long‐term disease outcome. Taken together, these results point out the relevance of the pre‐C5 level of the complement cascade in the inflammatory processes underlying MMN. [ABSTRACT FROM AUTHOR]

Published

2024

43. The Association Between Serum Levels of Glial Biomarkers, Clinical Severity and Electro-encephalography Features in Idiopathic West and Lennox- Gastaut Syndromes.

Author

CHERKEZZADE, Minara, SOYLU, Selen, TÜZÜN, Erdem, YILMAZ, Vuslat, SEZGİN, Mine, YAPICI, Zuhal, KÜÇÜKALİ, Cem İsmail, and TOPALOĞLU, Pınar

Subjects

*PROTEINS, *RESEARCH funding, *ELECTROENCEPHALOGRAPHY, *ENZYME-linked immunosorbent assay, *LENNOX-Gastaut syndrome, *CYTOSKELETAL proteins, *SEVERITY of illness index, *GLYCOPROTEINS, *DESCRIPTIVE statistics, *NEUROINFLAMMATION, *ANTIGENS, *MEMBRANE glycoproteins, *BIOMARKERS, *CHILDREN

Abstract

Introduction: Although the contribution of enhanced glial activity in seizure induction is increasingly recognized, the role of glia-induced neuroinflammation in the physiopathology of epileptic encephalopathy (EE) has been scarcely investigated. Methods: To delineate the contribution of glial activity in EE, we measured levels of glia-derived mediators with previously described biomarker value, including glial fibrillary acidic protein (GFAP), high mobility group box 1 (HMGB1), chitinase-3-like protein 1 (CHI3L1), soluble CD163 (sCD163) and triggering receptor expressed on myeloid cells 2 (TREM2) by ELISA in sera of patients with idiopathic West syndrome (WS, n=18), idiopathic Lennox-Gastaut syndrome (LGS, n=13) and healthy controls (n=31). Results: Patients with EE showed significantly higher CHI3L1 levels compared to healthy controls. Levels of HMGB1, CHI3L1, sCD163 and TREM2 were higher in LGS patients than WS patients and/or healthy controls. One or more of the investigated mediators were associated with treatment responsiveness, disease severity and presence of pathological features on electroencephalography (EEG). Conclusions: To our knowledge, our findings provide the initial patient-based evidence that astrocyte- and microglia-mediated neuroinflammation might be involved in the pathogenesis of LGS and WS. Moreover, glial mediators may serve as prognostic biomarkers in patients with idiopathic EE. [ABSTRACT FROM AUTHOR]

Published

2024

44. Lymphangiogenesis in Odontogenic Keratocysts Compared with Dentigerous Cysts.

Author

Zolfaghari, Reza, Bijani, Fatima, Seyedmajidi, Seyedali, and Seyedmajidi, Maryam

Subjects

T-test (Statistics), STATISTICAL significance, MANN Whitney U Test, CHI-squared test, DESCRIPTIVE statistics, IMMUNOHISTOCHEMISTRY, GENE expression, EXPERIMENTAL design, MEMBRANE glycoproteins, CYTOPLASM, ENDOTHELIAL cells, ODONTOGENIC cysts, DATA analysis software

Abstract

Statment of the Problem: Podoplanin can indicate the lymphangiogenesis. On the other hand, lymphangiogenesis affects the biological behavior of lesions. The clinical behavior of odontogenic keratocysts (OKC) and dentigerous cysts (DC) is different. Purpose: This study aimed to evaluate the immunohistochemical expression of podoplanin and to investigate lymphangiogenesis in OKCs as compared to DCs. Materials and Method: In this experimental laboratory study, sixty paraffined blocks, including 30 OKC and 30 DC samples, were examined in this study, all of which were histopathologically non-inflamed. To evaluate lymphangiogenesis, the immunohistochemical reaction of D2-40 was evaluated via cytoplasmic and membrane staining of lymphatic endothelial cells. The expression of podoplanin in the epithelial cells of two cyst groups was also examined. To analyze the collected data and compare the results between the two groups of cysts, independent samples t-test, Mann-Whitney U test, and Chi-square test were performed in SPSS version 22. The significance level was set at 0.05. Results: The mean lymph node count and podoplanin expression were significantly higher in the OKC epithelium as compared to DC (p< 0.001). Based on the results, 90% of OKC samples and 43.3% of DC samples showed grade 3 staining. Conclusion: The rate of lymphangiogenesis and podoplanin expression in the epithelium were higher in OKCs compared to DCs. According to the results, the expression of podoplanin may be a useful marker for determining the invasiveness and proliferation of OKC. [ABSTRACT FROM AUTHOR]

Published

2024

45. Designing a multi-epitope candidate vaccine against SARS-CoV-2 through in silico approach for producing in plant systems.

Author

Goudarziasl, Fatemeh, Kheiri, Fatemeh, Rahbar, Azam, Mohammadhassan, Reza, Mohammadi-Asl, Javad, Jalili, Arsalan, and Hajkazemian, Melika

Subjects

COVID-19 vaccines, AMINO acid sequence, MEMBRANE glycoproteins

Abstract

The COVID-19 is considered as a type of severe acute respiratory syndrome (SARS-CoV-2). The current pandemic causes a vital destruction in international social and economic systems. Current available vaccines involve entire viruses; however, peptide-based vaccines could be also beneficial. In the present study, a computationally candidate vaccine was designed against SARS-CoV-2. Surface glycoproteins (E, M, and S proteins) and N protein amino acid sequences were analyzed to predict high score of the B and T cell epitopes as antigenic proteins of the virus. High score epitopes, and the B subunit of Vibrio cholerae toxin, as an adjuvant put together by appropriate linkers to construct a multi-epitope candidate vaccine. Bioinformatics tools were used to predict the secondary, tertiary structure and physicochemical properties, such as aliphatic index, theoretical pH, molecular weight, and estimated half-life of the multi-epitope candidate vaccine. The interaction of candidate vaccine with TLR2 and TLR4 was computationally evaluated by molecular docking. Finally, the codon optimization and the secondary structure of mRNA were calculated, and in silico cloning was performed into plant expression vector by SnapGENE. This designed candidate vaccine along with the computational results requires laboratory evaluations to be confirmed as a candidate vaccine against SARS-COV-2 infection. [ABSTRACT FROM AUTHOR]

Published

2024

46. CTLA4 depletes T cell endogenous and trogocytosed B7 ligands via cis-endocytosis.

Author

Xu, Xiaozheng, Dennett, Preston, Zhang, Jibin, Sherrard, Alice, Bui, Jack, Chen, Xu, Hui, Enfu, Masubuchi, Takeya, and Zhao, Yunlong

Subjects

Humans, CTLA-4 Antigen, CD28 Antigens, Antigens, CD, Ligands, Antigens, Differentiation, Abatacept, B7-2 Antigen, Membrane Glycoproteins, Immunoconjugates, B7-1 Antigen, Cell Adhesion Molecules

Abstract

CD28 and CTLA4 are T cell coreceptors that competitively engage B7 ligands CD80 and CD86 to control adaptive immune responses. While the role of CTLA4 in restraining CD28 costimulatory signaling is well-established, the mechanism has remained unclear. Here, we report that human T cells acquire antigen-presenting-cell (APC)-derived B7 ligands and major histocompatibility complex (MHC) via trogocytosis through CD28:B7 binding. Acquired MHC and B7 enabled T cells to autostimulate, and this process was limited cell-intrinsically by CTLA4, which depletes B7 ligands trogocytosed or endogenously expressed by T cells through cis-endocytosis. Extending this model to the previously proposed extrinsic function of CTLA4 in human regulatory T cells (Treg), we show that blockade of either CD28 or CTLA4 attenuates Treg-mediated depletion of APC B7, indicating that trogocytosis and CTLA4-mediated cis-endocytosis work together to deplete B7 from APCs. Our study establishes CTLA4 as a cell-intrinsic molecular sink that limits B7 availability on the surface of T cells, with implications for CTLA4-targeted therapy.

Published

2023

47. The C-type lectin domain of CD62P (P-selectin) functions as an integrin ligand

Author

Takada, Yoko K, Simon, Scott I, and Takada, Yoshikazu

Subjects

Biochemistry and Cell Biology, Biological Sciences, Aetiology, 2.1 Biological and endogenous factors, Protein Domains, Lectins, C-Type, Humans, Animals, CHO Cells, Cricetulus, P-Selectin, Recombinant Proteins, Ligands, Mutation, Integrin alphaVbeta3, Membrane Glycoproteins, Membrane Proteins, ADAM Proteins, Protein Binding, Allosteric Site, Cell Communication, Cell Adhesion, Biological sciences, Biomedical and clinical sciences

Abstract

Recognition of integrins by CD62P has not been reported and this motivated a docking simulation using integrin αvβ3 as a target. We predicted that the C-type lectin domain of CD62P functions as a potential integrin ligand and observed that it specifically bound to soluble β3 and β1 integrins. Known inhibitors of the interaction between CD62P-PSGL-1 did not suppress the binding, whereas the disintegrin domain of ADAM-15, a known integrin ligand, suppressed recognition by the lectin domain. Furthermore, an R16E/K17E mutation in the predicted integrin-binding interface located outside of the glycan-binding site within the lectin domain, strongly inhibited CD62P binding to integrins. In contrast, the E88D mutation that strongly disrupts glycan binding only slightly affected CD62P-integrin recognition, indicating that the glycan and integrin-binding sites are distinct. Notably, the lectin domain allosterically activated integrins by binding to the allosteric site 2. We conclude that CD62P-integrin binding may function to promote a diverse set of cell-cell adhesive interactions given that β3 and β1 integrins are more widely expressed than PSGL-1 that is limited to leukocytes.

Published

2023

48. Systematic assessment of the contribution of structural variants to inherited retinal diseases.

Author

Wen, Shu, Wang, Meng, Qian, Xinye, Li, Yumei, Wang, Keqing, Choi, Jongsu, Pennesi, Mark, Yang, Paul, Marra, Molly, Koenekoop, Robert, Lopez, Irma, Matynia, Anna, Sui, Ruifang, Yao, Fengxia, Goetz, Kerry, Porto, Fernanda, Chen, Rui, and Gorin, Michael

Subjects

Humans, Retinal Diseases, Mutation, Whole Genome Sequencing, Exome Sequencing, Alleles, Membrane Glycoproteins, Molecular Chaperones, Eye Proteins

Abstract

Despite increasing success in determining genetic diagnosis for patients with inherited retinal diseases (IRDs), mutations in about 30% of the IRD cases remain unclear or unsettled after targeted gene panel or whole exome sequencing. In this study, we aimed to investigate the contributions of structural variants (SVs) to settling the molecular diagnosis of IRD with whole-genome sequencing (WGS). A cohort of 755 IRD patients whose pathogenic mutations remain undefined were subjected to WGS. Four SV calling algorithms including include MANTA, DELLY, LUMPY and CNVnator were used to detect SVs throughout the genome. All SVs identified by any one of these four algorithms were included for further analysis. AnnotSV was used to annotate these SVs. SVs that overlap with known IRD-associated genes were examined with sequencing coverage, junction reads and discordant read pairs. Polymerase Chain Reaction (PCR) followed by Sanger sequencing was used to further confirm the SVs and identify the breakpoints. Segregation of the candidate pathogenic alleles with the disease was performed when possible. A total of 16 candidate pathogenic SVs were identified in 16 families, including deletions and inversions, representing 2.1% of patients with previously unsolved IRDs. Autosomal dominant, autosomal recessive and X-linked inheritance of disease-causing SVs were observed in 12 different genes. Among these, SVs in CLN3, EYS and PRPF31 were found in multiple families. Our study suggests that the contribution of SVs detected by short-read WGS is about 0.25% of our IRD patient cohort and is significantly lower than that of single nucleotide changes and small insertions and deletions.

Published

2023

49. cis-B7:CD28 interactions at invaginated synaptic membranes provide CD28 co-stimulation and promote CD8+ T cell function and anti-tumor immunity

Author

Zhao, Yunlong, Caron, Christine, Chan, Ya-Yuan, Lee, Calvin K, Xu, Xiaozheng, Zhang, Jibin, Masubuchi, Takeya, Wu, Chuan, Bui, Jack D, and Hui, Enfu

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, 2.1 Biological and endogenous factors, Aetiology, Mice, Animals, CD28 Antigens, CD8-Positive T-Lymphocytes, Antigens, CD, Ligands, Synaptic Membranes, B7-2 Antigen, Membrane Glycoproteins, B7-1 Antigen, Cell Adhesion Molecules, Lymphocyte Activation, B7, CD28, PI3K, PKCθ, SNX9, T cell, anti-tumor immunity, cis-interactions, endocytosis, membrane curvatures

Abstract

B7 ligands (CD80 and CD86), expressed by professional antigen-presenting cells (APCs), activate the main co-stimulatory receptor CD28 on T cells in trans. However, in peripheral tissues, APCs expressing B7 ligands are relatively scarce. This raises the questions of whether and how CD28 co-stimulation occurs in peripheral tissues. Here, we report that CD8+ T cells displayed B7 ligands that interacted with CD28 in cis at membrane invaginations of the immunological synapse as a result of membrane remodeling driven by phosphoinositide-3-kinase (PI3K) and sorting-nexin-9 (SNX9). cis-B7:CD28 interactions triggered CD28 signaling through protein kinase C theta (PKCθ) and promoted CD8+ T cell survival, migration, and cytokine production. In mouse tumor models, loss of T cell-intrinsic cis-B7:CD28 interactions decreased intratumoral T cells and accelerated tumor growth. Thus, B7 ligands on CD8+ T cells can evoke cell-autonomous CD28 co-stimulation in cis in peripheral tissues, suggesting cis-signaling as a general mechanism for boosting T cell functionality.

Published

2023

50. Anti-CD22 Calicheamicin-Inotuzumab Ozogamicin Combined with Venetoclax + Azacitidine in the Treatment of Mixed-Phenotype Acute Leukemia: A Case Report.

Author

Kongfei Li, Yuxiao Wang, Renzhi Pei, Ying Lu, Junjie Cao, Xianxu Zhuang, Jiaying Lian, and Bibo Zhang

Subjects

*THERAPEUTIC use of antineoplastic agents, *THERAPEUTIC use of monoclonal antibodies, *HETEROCYCLIC compounds, *ANEMIA, *FLOW cytometry, *HEMATOPOIETIC stem cell transplantation, *AZACITIDINE, *ALKENES, *ANTINEOPLASTIC agents, *CANCER chemotherapy, *MONOCLONAL antibodies, *MEMBRANE glycoproteins, *AMINOGLYCOSIDES, *LEUCOCYTE disorders, *TREATMENT failure, *CHEMICAL inhibitors, BONE marrow examination

Published

2024