Showing total 16,019 results

101. Decrease in Heparan Sulphate Binding in Tropism-Retargeted Oncolytic Herpes Simplex Virus (ReHV) Delays Blood Clearance and Improves Systemic Anticancer Efficacy.

Author

Vannini, Andrea, Parenti, Federico, Forghieri, Cristina, Vannini, Gaia, Barboni, Catia, Zaghini, Anna, Gianni, Tatiana, and Campadelli-Fiume, Gabriella

Subjects

TREATMENT of lung tumors, ONCOLYTIC virotherapy, RODENTS, RESEARCH funding, HERPESVIRUSES, GLYCOPROTEINS, TREATMENT effectiveness, IN vivo studies, BLOOD cells, METASTASIS, INTRAVENOUS therapy, CHONDROITIN sulfates, ENDOTHELIAL cells, ANIMAL experimentation, GENETIC mutation, GLYCOSAMINOGLYCANS

Abstract

Simple Summary: Oncolytic herpes simplex viruses (oHSVs) employ as natural entry receptors nectin1 or HVEM. In contrast, retargeted oHSVs (ReHVs) employ as an entry receptor a tumor-associated antigen that no longer interacts with nectin1/HVEM and, thus, spares normal cells. Prior to entry, both oHSVs and ReHVs attach to cells by interaction of gC and gB glycoproteins with heparan sulphates and chondroitin sulphates (glycosaminoglycans–GAGs). The systemic delivery of oncolytic viruses would be the ideal route for hard-to-reach or metastatic cancers that constitute unmet clinical needs. In an accompanying paper, we reported that the blood complement and the antiviral neutralizing antibodies represent the major blood factors that inactivate systemically administered ReHVs. Here, we asked whether ReHV adsorption to GAGs acts as a sink and subtracts the virus from circulation. We report that a genetic modification in gC, which reduced its interaction with GAGs, resulted in a longer half-life of circulating ReHV and a higher anticancer efficacy of systemically (but not intratumorally) administered ReHV. The role of the interaction with cell-surface glycosaminoglycans (GAGs) during in vivo HSV infection is currently unknown. The rationale of the current investigation was to improve the anticancer efficacy of systemically administered retargeted oHSVs (ReHVs) by decreasing their binding to GAGs, including those of endothelial cells, blood cells, and off-tumor tissues. As a proof-of-principle approach, we deleted seven amino acids critical for interacting with GAGs from the glycoprotein C (gC) of R-337 ReHV. The modification in the resulting R-399 recombinant prolonged the half-life in the blood of systemically administered R-399 and enhanced its biodistribution to tumor-positive lungs and to the tumor-negative liver. Ultimately, it greatly increased the R-399 efficacy against metastatic-like lung tumors upon IV administration but not against subcutaneous tumors upon IT administration. These results provide evidence that the increased efficacy seen upon R-399 systemic administration correlated with the slower clearance from the circulation. To our knowledge, this is the first in vivo evidence that the partial impairment of the gC interaction with GAGs resulted in a prolonged half-life of circulating ReHV, an increase in the amount of ReHV taken up by tissues and tumors, and, ultimately, an enhanced anticancer efficacy of systemically administered ReHV. [ABSTRACT FROM AUTHOR]

Published

2024

102. A comparison of three models for ethical evaluation of proposed animal experiments.

Author

de Cock Buning T and Theune EP

Subjects

Animal Care Committees, Animal Testing Alternatives, Animals, Canada, Evaluation Studies as Topic, International Cooperation, Internationality, Methods, Netherlands, Pain, United Kingdom, Animal Experimentation, Animal Welfare, Ethical Review, Ethics, Models, Theoretical

Published

1994

103. Empirical Study on the Relationship between Agricultural Economic Structure Growth and Environmental Pollution Based on Time-Varying Parameter Vector Autoregressive Model.

Author

Li, Xiaozhong and Huang, Feng

Subjects

AUTOREGRESSIVE models, POLLUTION, ECONOMIC structure, ENERGY intensity (Economics), ECONOMIC expansion, POLLUTANTS, POULTRY, AGRICULTURE, ANIMAL experimentation, INDUSTRIES, ECONOMICS

Abstract

In order to better demonstrate the relationship between agricultural economic structure growth and environmental pollution, an autoregressive model based on time-varying parameter vector was proposed. In the process of developing the research, this paper introduces the LDMI method, based on the time-varying parameter vector autoregression model, with the help of sampling formula calculation and other methods. Efforts were made to obtain credible conclusions. The experiment result shows that in this study, a total of 10,000 samples were taken. According to this value, 10000/116.15 = 86, which means that at least 86 unrelated samples can be obtained. Therefore, we can determine that each indicator mentioned in this paper has valid samples when it is introduced into the time-varying parameter vector autoregression (TVP-VAR) model for parameter estimation. After sampling detection image analysis and data calculation, the effect of energy structure, energy intensity industrial structure, and scale effect on the emission scale of environmental pollutants was obtained. It is proved that through the research of this paper, two main conclusions are finally obtained, and the influence of the five factors mentioned above is summarized. [ABSTRACT FROM AUTHOR]

Published

2022

104. PETA SENDS EVERY MEMBER OF CONGRESS TOILET PAPERBUT THERE'S A CATCH

Subjects

United States. National Institutes of Health, Legislators, Animal experimentation, Brain damage, Psychology, Rubber, Health, Paper, News, opinion and commentary

Abstract

WASHINGTON -- The following information was released by People for the Ethical Treatment of Animals (PETA): With toilet paper in high demand during the COVID-19 lockdown, PETA is helping to [...]

Published

2020

105. Development of Two Korean IACUC Guidance Documents to Foster Implementation of the Three Rs.

Author

Lee GH, Kim HJ, Joo YS, Kim SY, Reed B, Hart LA, and Choe BI

Subjects

Animals, Language, Republic of Korea, Animal Care Committees, Animal Experimentation

Abstract

In Korea, Institutional Animal Care and Use Committees (IACUCs) have been legally required to apply the Three Rs principles (i.e. replacement , reduction and refinement ) and undertake the ethical review of animal study protocols, since 2008. According to Korean law, each IACUC is required to appoint at least one lay member recommended by a non-governmental animal protection organisation, who participates in the ethical review process as part of this role. Despite the importance of the Three Rs and the ethical review process, limited information and practical resources are available for IACUC members in the Korean language, particularly for lay members who are inexperienced in animal experimentation. In January 2020, the Animal and Plant Quarantine Agency announced the funding for a six-month research project to develop guidance to assist IACUC members in carrying out effective and efficient protocol reviews in line with Korean legislative requirements. This funding was awarded for the production of two IACUC guidance documents - 'Guide for Animal Study Protocols' and 'Guide for the IACUC Lay Member' - which were published in December 2020. These guidance documents aim to foster the implementation of the Three Rs and provide practical resources for IACUC members, researchers and other relevant personnel. This paper describes the framework for animal use in Korea and the overall production of these two IACUC Guidance Documents.

Published

2023

106. Proteomic analysis of rat skeletal muscle submitted to one bout of incremental exercise.

Author

Gandra, P. G., Valente, R. H., Perales, J., Pacheco, A. G., and Macedo, D. V.

Subjects

SKELETAL muscle physiology, PHYSIOLOGICAL adaptation, ANALYSIS of variance, ANIMAL experimentation, CONFIDENCE intervals, ELECTROPHORESIS, DIGITAL image processing, MASS spectrometry, PAPER chromatography, PEPTIDES, PROBABILITY theory, PROTEINS, RATS, RESEARCH funding, T-test (Statistics), PROTEOMICS, EXERCISE intensity, TISSUE arrays

Abstract

Exercise can alter gene transcriptional and protein translational rates leading to changes in protein abundance toward adaptation to exercise. We investigated the alterations in protein abundance in skeletal muscle after one bout of an exhaustive exercise through proteomic analysis. Gastrocnemius muscles were sampled from non-exercised control rats and from rats exercised on a treadmill with incremental increases in speed until exhaustion (approximately 30 min). Rats were sacrificed 3 and 24 h after exercise cessation. Two-dimensional gel electrophoresis was performed and spots with a significant alteration in relative volume were identified by mass spectrometry. Six spots presented statistically significant altered abundances after exercise. The spots identified as the metabolic related proteins triosephosphate isomerase 1, glyceraldehyde-3-phosphate dehydrogenase, the β subunit of pyruvate dehydrogenase E1 and carnitine palmitoyltransferase 2 were all more abundant after exercise. One spot identified as heat shock cognate 70 was also more abundant after exercise. One spot demonstrated a decreased abundance after exercise and was identified as α-actin. These results suggest that a single session of exhaustive incremental exercise in untrained muscle can alter thin filaments synthesis/degradation rate and enhance cytosolic and mitochondrial proteins synthesis. The identified proteins may be important to a general preconditioning of skeletal muscle for subsequent exercise sessions. [ABSTRACT FROM AUTHOR]

Published

2012

107. Congenital word-blindness -- making sense of wiring diagrams and 'black boxes': discussion paper.

Author

Husain, M.

Subjects

DYSLEXIA, LANGUAGE disorders, MEDICAL experimentation on humans, ANIMAL experimentation, VISION, HEARING

Abstract

The article discusses the implications of developmental dyslexia, which is also called the congenital word-blindness, as well as recent speculations which have yet to be confirmed. These are derived from experiments conducted on normal humans and monkeys, as well as humans suffering from the experiments of nature. The notion that linguistic competence depends upon associations between vision and hearing implies that the mechanism employed in reading may not be unique to the reading-process.

Published

1986

108. Functional foods: benefits, concerns and challenges-a position paper from the american council on science and health.

Author

Hasler, Clare M.

Subjects

*ANIMAL experimentation, *COMPARATIVE studies, *FOOD, *RESEARCH methodology, *MEDICAL cooperation, *PLANTS, *RESEARCH, *HEALTH self-care, *EVALUATION research

Abstract

Functional foods can be considered to be those whole, fortified, enriched or enhanced foods that provide health benefits beyond the provision of essential nutrients (e.g., vitamins and minerals), when they are consumed at efficacious levels as part of a varied diet on a regular basis. Linking the consumption of functional foods or food ingredients with health claims should be based on sound scientific evidence, with the "gold standard" being replicated, randomized, placebo-controlled, intervention trials in human subjects. However, not all foods on the market today that are claimed to be functional foods are supported by enough solid data to merit such claims. This review categorizes a variety of functional foods according to the type of evidence supporting their functionality, the strength of that evidence and the recommended intakes. Functional foods represent one of the most intensively investigated and widely promoted areas in the food and nutrition sciences today. However, it must be emphasized that these foods and ingredients are not magic bullets or panaceas for poor health habits. Diet is only one aspect of a comprehensive approach to good health. [ABSTRACT FROM AUTHOR]

Published

2002

109. Characterization of the mouse islet-specific glucose-6-phosphatase catalytic subunit-related protein gene promoter by in situ footprinting: correlation with fusion gene expression in the islet-derived betaTC-3 and hamster insulinoma tumor cell lines.

Author

Bischof, Larry J., Martin, Cyrus C., Svitek, Christina A., Stadelmaier, Beth T., Hornbuckle, Lauri A., Goldman, Joshua K., Oeser, James K., Hutton, John C., O'Brien, Richard M., Bischof, L J, Martin, C C, Svitek, C A, Stadelmaier, B T, Hornbuckle, L A, Goldman, J K, Oeser, J K, Hutton, J C, and O'Brien, R M

Subjects

GENE expression, PROTEINS, ANIMAL experimentation, CELL lines, CHEMISTRY, COMPARATIVE studies, DOCUMENTATION, GENES, GENETIC techniques, HAMSTERS, ISLANDS of Langerhans, ISLANDS of Langerhans tumors, RESEARCH methodology, MEDICAL cooperation, MICE, NUCLEOTIDES, PAPER chromatography, PEPTIDES, PHOSPHATASES, RESEARCH, TRANSCRIPTION factors, TRANSFERASES, DNA-binding proteins, EVALUATION research, NUCLEAR proteins, PHYSIOLOGY

Abstract

Glucose-6-phosphatase (G6Pase) is a multicomponent system located in the endoplasmic reticulum comprising a catalytic subunit and transporters for glucose-6-phosphate, inorganic phosphate, and glucose. We have recently cloned a novel gene that encodes an islet-specific G6Pase catalytic subunit-related protein (IGRP) (Ebert et al., Diabetes 48:543-551, 1999). To begin to investigate the molecular basis for the islet-specific expression of the IGRP gene, a series of truncated IGRP-chloramphenicol acetyltransferase (CAT) fusion genes were transiently transfected into the islet-derived mouse betaTC-3 and hamster insulinoma tumor cell lines. In both cell lines, basal fusion gene expression decreased upon progressive deletion of the IGRP promoter sequence between -306 and -66, indicating that multiple promoter regions are required for maximal IGRP-CAT expression. The ligation-mediated polymerase chain reaction footprinting technique was then used to compare trans-acting factor binding to the IGRP promoter in situ in betaTC-3 cells, which express the endogenous IGRP gene, and adrenocortical Y1 cells, which do not. Multiple trans-acting factor binding sites were selectively identified in betaTC-3 cells that correlate with regions of the IGRP promoter identified as being required for basal IGRP-CAT fusion gene expression. The data suggest that hepatocyte nuclear factor 3 may be important for basal IGRP gene expression, as it is for glucagon, GLUT2, and Pdx-1 gene expression. In addition, binding sites for several trans-acting factors not previously associated with islet gene expression, as well as binding sites for potentially novel proteins, were identified. [ABSTRACT FROM AUTHOR]

Published

2001

110. Feasibility of Laparoscopic Combined Para-Orthotopic Pancreas and Orthotopic Kidney Transplantation: Initial Research with a Pig Model

Author

Yansheng Li, Yongwei Zhao, Xuhui Zhu, Tao Li, Yuanhao Chen, Bulang He, Peng Zhang, Xiuwu Han, and Gao Li

Subjects

Animal Experimentation, medicine.medical_specialty, Swine, medicine.medical_treatment, 030230 surgery, Anastomosis, Pancreas transplantation, Kidney, Nephrectomy, 03 medical and health sciences, 0302 clinical medicine, Renal Artery, medicine.artery, medicine, Animals, Kidney surgery, Right Renal Artery, Renal artery, Kidney transplantation, Transplantation, Original Paper, business.industry, Anastomosis, Surgical, General Medicine, medicine.disease, Kidney Transplantation, Surgery, medicine.anatomical_structure, Models, Animal, Feasibility Studies, 030211 gastroenterology & hepatology, Female, Laparoscopy, Pancreas Transplantation, Ureter, Pancreas, business

Abstract

BACKGROUND The aim of this study was to investigate the feasibility of laparoscopic combined para-orthotopic pancreas and orthotopic kidney transplantation in a pig model. MATERIAL AND METHODS Twelve white female pigs, (4-5 months old, weight range 40-45 kg) were used as donors and recipients, and 6 laparoscopic-combined pancreas and kidney transplantations were performed. After bilateral nephrectomy, the pancreatic artery and vein were anastomosed to the right renal artery and vein, respectively, and the pancreatic fluid was diverted to the duodenum or jejunum. The renal artery and vein were anastomosed to the left renal artery and vein, respectively. The ureter (or kidney pelvis) was anastomosed to the left native ureter (or kidney pelvis). The data of the operations were recorded, and grafts were inspected at autopsy. RESULTS Four of the 6 recipient pigs underwent the entire procedure. The duodenum-to-duodenum anastomosis was unfinished in 1 case, and both the duodenum-to-duodenum and renal pelvis-to-pelvis anastomoses were left unperformed in another case. The mean recipient operative time was 429±43 minutes. The mean venous and arterial anastomotic times were 69±15 minutes and 37±18 minutes, respectively, for pancreas transplantation and 56±09 minutes and 42±06 minutes, respectively, for kidney transplantation. The time for renal pelvis-to-pelvis anastomosis was 56±13 minutes and for duodenum-to-duodenum anastomosis was 90±13 minutes. The mean blood loss for recipient pigs was 98±35 mL. An immediate viable blood supply was seen in the 4 pancreatic grafts and in the 5 kidney grafts during the operation by the appearance of a bright red color after revascularization. Five pancreatic grafts had autopsy-proven reliable artery anastomoses and 4 reliable vein anastomoses. All 6 kidney grafts had autopsy-proven reliable artery anastomoses; however, 1 had a vein anastomotic stricture. CONCLUSIONS Our study showed that laparoscopic-combined para-orthotopic pancreas and orthotopic kidney transplantation in pigs is surgically possible.

Published

2018

111. Inhibition of Oxidative Stress-Induced Ferroptosis Can Alleviate Rheumatoid Arthritis in Human.

Author

Liu, Yang, Liang, Jiang, Sha, Zongge, and Yang, Changfu

Subjects

EXPERIMENTAL arthritis, SYNOVITIS, RHEUMATOID arthritis, FERRITIN, DISEASE remission, MEMBRANE potential, MITOCHONDRIAL membranes, ANIMAL experimentation

Abstract

Rheumatoid arthritis (RA) is a chronic autoimmunity illness, mainly featured with synovitis of the joint. The specificity of ferroptosis is disparate in different diseases, and the mechanism of ferroptosis in RA has some uncertainty yet. Therefore, the mechanism of ferroptosis was deeply observed in RA patients and animal models. In this paper, plasma of RA patients, the tumor necrosis factor-alpha-induced human synovial fibroblasts, and an animal model of arthritis induced by collagen were applied to initially inquire about the therapeutic effect of ferroptosis. For the RA patients, ELISA detected protein expression of glutathione (GSH), GPX4, Nrf2, Keap-1, and ferritin. In cell experiments, erastin or fer-1 regulated the invasion of human synovial fibroblast cells, mitochondrial membrane potential, reactive oxygen species (ROS) expression, marker protein, and so on. For the animal experiments, 32 Sprague–Dawley male rats were randomly separated into four groups with a collagen-induced RA model for 14 days and administered with erastin or fer-1 for 35 days. The expressions of GSH, GPX4, Nrf2, and Keap-1 were lower, and the ferritin was higher in RA patients, and the expressions of these proteins varied significantly after disease remission. In addition, ferroptosis inactivation also reduced the proliferation and migration ability, mitochondrial membrane potential, and ROS in cells. We discovered unexpectedly that activation of ferroptosis meaningfully forbore the foot swelling in animals with CIA, reduced arthritis scores, destruction of bone, and articular synovitis, and also decreased the high expression of inflammatory factors in plasma. There is a nonlinear relationship between human disease manifestations and animal model pathology. Ferroptosis regulating in RA for humans or animals may produce different effects. [ABSTRACT FROM AUTHOR]

Published

2024

112. Injectable hydrogel-based combination therapy for myocardial infarction: a systematic review and Meta-analysis of preclinical trials.

Author

Gao, Han, Liu, Song, Qin, Shanshan, Yang, Jiali, Yue, Tian, Ye, Bengui, Tang, Yue, Feng, Jie, Hou, Jun, and Danzeng, Dunzhu

Subjects

MYOCARDIAL infarction, LITERATURE reviews, ANIMAL experimentation, EXTRACELLULAR vesicles, LABORATORY animals, ACUTE diseases

Abstract

Introduction: This study evaluates the effectiveness of a combined regimen involving injectable hydrogels for the treatment of experimental myocardial infarction. Patient concerns: Myocardial infarction is an acute illness that negatively affects quality of life and increases mortality rates. Experimental models of myocardial infarction can aid in disease research by allowing for the development of therapies that effectively manage disease progression and promote tissue repair. Diagnosis: Experimental animal models of myocardial infarction were established using the ligation method on the anterior descending branch of the left coronary artery (LAD). Interventions: The efficacy of intracardiac injection of hydrogels, combined with cells, drugs, cytokines, extracellular vesicles, or nucleic acid therapies, was evaluated to assess the functional and morphological improvements in the post-infarction heart achieved through the combined hydrogel regimen. Outcomes: A literature review was conducted using PubMed, Web of Science, Scopus, and Cochrane databases. A total of 83 papers, including studies on 1332 experimental animals (rats, mice, rabbits, sheep, and pigs), were included in the meta-analysis based on the inclusion and exclusion criteria. The overall effect size observed in the group receiving combined hydrogel therapy, compared to the group receiving hydrogel treatment alone, resulted in an ejection fraction (EF) improvement of 8.87% [95% confidence interval (CI): 7.53, 10.21] and a fractional shortening (FS) improvement of 6.31% [95% CI: 5.94, 6.67] in rat models, while in mice models, the improvements were 16.45% [95% CI: 11.29, 21.61] for EF and 5.68% [95% CI: 5.15, 6.22] for FS. The most significant improvements in EF (rats: MD = 9.63% [95% CI: 4.02, 15.23]; mice: MD = 23.93% [95% CI: 17.52, 30.84]) and FS (rats: MD = 8.55% [95% CI: 2.54, 14.56]; mice: MD = 5.68% [95% CI: 5.15, 6.22]) were observed when extracellular vesicle therapy was used. Although there have been significant results in large animal experiments, the number of studies conducted in this area is limited. Conclusion: The present study demonstrates that combining hydrogel with other therapies effectively improves heart function and morphology. Further preclinical research using large animal models is necessary for additional study and validation. [ABSTRACT FROM AUTHOR]

Published

2024

113. Derivatives of Betulin and Betulinic Acid Containing a Phosphonate Group—In Silico Studies and Preliminary In Vitro Assessment of Antiviral Activity.

Author

Bębenek, Ewa, Pęcak, Paweł, Kadela-Tomanek, Monika, Orzechowska, Beata, and Chrobak, Elwira

Subjects

BETULINIC acid, BETULIN, ANTIVIRAL agents, PHOSPHONATES, MOLECULAR docking, VIRUS diseases, ANIMAL experimentation

Abstract

Viral diseases affecting both humans and animals are a serious public problem. Chemical modifications of the structure of compounds of natural origin, e.g., betulin, seem to be a promising model in the search for new antiviral agents. The subject of our work was to conduct preliminary tests on the antiviral activity of phosphonic derivatives of betulin and betulinic acid and to assess the pharmacokinetic profile of target compounds. Human (HHV-1, HAdV-5) and animal viruses (BEV, VSV) were used in the in vitro tests. Additionally, this paper presents the results of research using in silico methods (ADMET and molecular docking). Two compounds (betulin 29-phosphonate 3 and 3-(3′,3′-dimethylsuccinyl)betulin acid 29-phosphonate 8a) showed antiviral activity against BEV, and compound 3 was also active against HAdV-5. For compound 3, which showed advantageous pharmacokinetic parameters, molecular docking was performed to determine possible interactions with the cellular target HAdV-5 endopeptidase, which plays an important role in various functions of the virus. Selecting the most active derivatives makes it possible to plan tests on an animal model. [ABSTRACT FROM AUTHOR]

Published

2024

114. Triptolide Reduces Neoplastic Progression in Hepatocellular Carcinoma by Downregulating the Lipid Lipase Signaling Pathway.

Author

Chang, Wei, Wang, Jingjing, You, Yuanqi, Wang, Hongqian, Xu, Shendong, Vulcano, Stephen, Xu, Changlu, Shen, Chenlin, Li, Zhi, and Wang, Jie

Subjects

LIPID metabolism, LIPASES, EXPERIMENTAL design, TERPENES, CELL migration, ANALYSIS of variance, CARCINOGENESIS, ANTI-inflammatory agents, ANIMAL experimentation, MICROBIOLOGICAL assay, IMMUNOHISTOCHEMISTRY, APOPTOSIS, CELLULAR signal transduction, RESEARCH funding, CELL lines, POLYMERASE chain reaction, DATA analysis software, HEPATOCELLULAR carcinoma, MICE, PHARMACODYNAMICS, DISEASE risk factors

Abstract

Simple Summary: TP is a widely utilized anticancer medication, particularly effective in treating HCC. Thorough investigation into TP's molecular mechanism in HCC treatment is crucial for precise and combination therapy. In this paper, we have unveiled a novel mechanism of TP in HCC treatment, where it inhibits tumor growth by reducing lipid accumulation. While the inhibition of P53 gene activity is commonly thought to be the reason for TP's effectiveness in treating HCC, this new mechanism serves as a significant complement to the current understanding, paving the way for innovative approaches to HCC treatment. Hepatocellular carcinoma (HCC), which is the third leading cause of cancer-related mortality in the world, presents a significant medical challenge. Triptolide (TP) has been identified as an effective therapeutic drug for HCC. However, its precise therapeutic mechanism is still unknown. Understanding the mechanism of action of TP against HCC is crucial for its implementation in the field of HCC treatment. We hypothesize that the anti-HCC actions of TP might be related to its modulation of HCC lipid metabolism given the crucial role that lipid metabolism plays in promoting the progression of HCC. In this work, we first demonstrate that, both in vitro and in vivo, TP significantly reduces lipid accumulation in HCC cells. Additionally, we notice that lipoprotein lipase (LPL) expression is markedly upregulated in HCC, and that its levels are positively connected with the disease's progression. It is interesting to note that TP dramatically reduces LPL activity, which in turn prevents HCC growth and reduces lipid accumulation. Additionally, the effect of TP on LPL is a direct correlation. These results definitely demonstrate that TP protects hepatocytes against abnormal accumulation of lipids by transcriptionally suppressing LPL, which reduces the development of HCC. This newly identified pathway provides insight into the process through which TP exerts its anti-HCC actions. [ABSTRACT FROM AUTHOR]

Published

2024

115. Optimizing Immature Testicular Tissue and Cell Transplantation Results: Comparing Transplantation Sites and Scaffolds.

Author

Anvari, Alireza, Movahedin, Mansoureh, and Hamzeh, Maedeh

Subjects

BIOLOGICAL models, INJECTIONS, GOATS, ANIMAL experimentation, SWINE, RABBITS, RATS, COMPARATIVE studies, INFERTILITY, TREATMENT effectiveness, STEM cells, QUALITY assurance, SPERMATOZOA, TISSUE scaffolds, CELL transplantation, MICE, CRYOPRESERVATION of organs, tissues, etc.

Abstract

For patients who had testicular tissue cryopreserved before receiving gonadotoxic therapies, transplantation of testicular tissues and cells has been recommended as a potential therapeutic option. There are no studies that indicate the generation of sperm after human immature testicular tissue (ITT) or spermatogonial stem cells (SSCs) transplantation. The use of releasing scaffolds and localized drug delivery systems as well as the optimizing transplantation site can play an effective role in increasing the efficiency and improving the quality of testicular tissue and cell transplantation in animal models. Current research is focused on optimizing ITT and cell transplantation, the use of releasing scaffolds, and the selection of the right transplantation site that might restore sperm production or male infertility treatment. By searching the PubMed and Google Scholar databases, original and review papers were collected. Search terms were relevant for SSCs and tissue transplantation. In this review, we'll focus on the potential advantages of using scaffolds and choosing the right transplantation site to improve transplantation outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

116. Continuous Electrode Models and Application of Exact Schemes in Modeling of Electrical Impedance Measurements.

Author

Vizvari, Zoltan, Klincsik, Mihaly, Odry, Peter, Tadic, Vladimir, Gyorfi, Nina, Toth, Attila, and Sari, Zoltan

Subjects

ELECTRIC impedance, ELECTRODES, ANIMAL experimentation, CONTINUOUS functions, POTENTIAL functions, DIFFERENTIAL equations

Abstract

The crucial issue in electrical impedance (EI) measurements lies in the galvanic interaction between the electrodes and the investigated material. This paper brings together the basic and applied research experience and combines their results with excellent properties. Consequently, innovative precise methodologies have emerged, enabling the direct modeling of EI measurements, free from the inaccuracies often associated with numerical approaches. As an outcome of the efficiency and robustness of the applied method, the conductivity of the material and the electrodes are represented by a common piecewise function, which is used to solve the differential equation modeling of the EI measurement. Moreover, this allows the possibility for modeling the conductivity of electrodes with continuous functions, providing an important generalization of the Complete Electrode Model (CEM), which has been widely used so far. The effectiveness of the novel approach was showcased through two distinct case studies. In the first case study, potential functions within both the material and the electrodes were computed using the CEM. In the second case study, calculations were performed utilizing the newly introduced continuous electrode model. The simulation results suggest that the new method is a powerful tool for biological research, from in vitro experiments to animal studies and human applications. [ABSTRACT FROM AUTHOR]

Published

2024

117. Intestinal absorption of D-fructose isomers, D-allulose, D-sorbose and D-tagatose, via glucose transporter type 5 (GLUT5) but not sodium-dependent glucose cotransporter 1 (SGLT1) in rats.

Author

Kishida, Kunihiro, Iida, Tetsuo, Yamada, Takako, and Toyoda, Yukiyasu

Subjects

MONOSACCHARIDES, ANIMAL experimentation, FRUCTOSE, RATS, COMPARATIVE studies, T-test (Statistics), GENE expression, INTESTINAL absorption, MEMBRANE transport proteins, DESCRIPTIVE statistics, RESEARCH funding, MESSENGER RNA, DATA analysis software, SODIUM-glucose cotransporter 2 inhibitors, CARRIER proteins

Abstract

D-allulose, D-sorbose and D-tagatose are D-fructose isomers that are called rare sugars. These rare sugars have been studied intensively in terms of biological production and food application as well as physiological effects. There are limited papers with regard to the transporters mediating the intestinal absorption of these rare sugars. We examined whether these rare sugars are absorbed via sodium-dependent glucose cotransporter 1 (SGLT1) as well as via GLUT type 5 (GLUT5) using rats. High-fructose diet fed rats, which express more intestinal GLUT5, exhibited significantly higher peripheral concentrations, Cmax and AUC0–180 min when D-allulose, D-sorbose and D-tagatose were orally administrated. KGA-2727, a selective SGLT1 inhibitor, did not affect the peripheral and portal vein concentrations and pharmacokinetic parameters of these rare sugars. The results suggest that D-allulose, D-sorbose and D-tagatose are likely transported via GLUT5 but not SGLT1 in rat small intestine. [ABSTRACT FROM AUTHOR]

Published

2023

118. Ethics and regulation of neuronal optogenetics in the European Union.

Author

Faltus, Timo, Freise, Johannes, Fluck, Carsten, and Zillmann, Hans

Subjects

*OPTOGENETICS, *PARKINSON'S disease, *ANIMAL experimentation, *ETHICS, *ION channels, *STROKE

Abstract

Neuronal optogenetics is a technique to control the activity of neurons with light. This is achieved by artificial expression of light-sensitive ion channels in the target cells. By optogenetic methods, cells that are naturally light-insensitive can be made photosensitive and addressable by illumination and precisely controllable in time and space. So far, optogenetics has primarily been a basic research tool to better understand the brain. However, initial studies are already investigating the possibility of using optogenetics in humans for future therapeutic approaches for neuronal based diseases such as Parkinson's disease, epilepsy, or to promote stroke recovery. In addition, optogenetic methods have already been successfully applied to a human in an experimental setting. Neuronal optogenetics also raises ethical and legal issues, e.g., in relation to, animal experiments, and its application in humans. Additional ethical and legal questions may arise when optogenetic methods are investigated on cerebral organoids. Thus, for the successful translation of optogenetics from basic research to medical practice, the ethical and legal questions of this technology must also be answered, because open ethical and legal questions can hamper the translation. The paper provides an overview of the ethical and legal issues raised by neuronal optogenetics. In addition, considering the technical prerequisites for translation, the paper shows consistent approaches to address these open questions. The paper also aims to support the interdisciplinary dialogue between scientists and physicians on the one hand, and ethicists and lawyers on the other, to enable an interdisciplinary coordinated realization of neuronal optogenetics. [ABSTRACT FROM AUTHOR]

Published

2023

119. Erythrocyte Sedimentation Rate for Assisted Diagnosis of Pediatric Osteomyelitis: A Meta-Analysis.

Author

Qi, Han, Zhu, Zhitao, and Zhu, Dongsheng

Subjects

BLOOD sedimentation, OSTEOMYELITIS, LEUKOCYTE count, RECEIVER operating characteristic curves, ANIMAL experimentation

Abstract

For the diagnosis of pediatric osteomyelitis, the sensitivity, specificity, and predictive value of erythrocyte sedimentation rate (ESR) were evaluated in this study.Methods: A systematic computer-based search was performed for relevant articles focusing on the ESR diagnosis of pediatric osteomyelitis in PubMed, Embase, and the Cochrane Library with an inclusion criteria: 1) the diagnostic utility of ESR for diagnosing osteomyelitis patients under the age of 18;2) two-by-two contingency tables can be obtained. Case reports, review papers, and animal experiments were excluded.Results: The diagnostic meta-analysis included 8 studies involving 348 children with osteomyelitis, all of whom were tested for ESR. Diagnostic meta-analysis revealed a sensitivity and specificity of 0.90, 95% confidence interval (CI) (0.86– 0.93), and 0.50 (95% CI,0.47– 0.54) for ESR in pediatric osteomyelitis diagnosis, respectively. The positive likelihood ratio (LR), negative LR, and diagnostic odds ratio were 1.38,(95% CI,1.08– 1.78), 0.46, (95% CI,0.26– 0.73), and 3.20, (95% CI,1.33– 7.69), respectively. The area under the curve (AUC) was determined to be 0.80 based on the summary receiver operating characteristic curve (SROC).Conclusion: The literature on the use of ESR in pediatric osteomyelitis diagnosis was thoroughly reviewed in this study. It was also found that ESR may be useful as a biomarker for pediatric osteomyelitis diagnosis. Due to its low specificity, it should be used in combination with other markers such as C-reactive protein, neutrophil percentage, and white blood cell count. [ABSTRACT FROM AUTHOR]

Published

2023

120. Alleviate oxidative stress in diabetic retinopathy: antioxidant therapeutic strategies.

Author

Gao, Jie, Tao, Liming, and Jiang, Zhengxuan

Subjects

DIABETIC retinopathy, REACTIVE oxygen species, ANIMAL experimentation, RETINAL degeneration, DATABASE searching

Abstract

This review outlines the function of oxidative stress in DR and discusses therapeutic strategies to treat DR with antioxidants. Published papers on oxidative stress in DR and therapeutic strategies to treat DR with antioxidants were collected and reviewed via database searching on PubMed. The abnormal development of DR is a complicated process. The pathogenesis of DR has been reported to involve oxidative stress, despite the fact that the mechanisms underlying this are still not fully understood. Excessive reactive oxygen species (ROS) accumulation can damage retina, eventually leading to DR. Increasing evidence have demonstrated that antioxidant therapy can alleviate the degeneration of retinal capillaries in DR. Oxidative stress can play an important contributor in the pathogenesis of DR. Furthermore, animal experiments have shown that antioxidants are a beneficial therapy for treating DR, but more clinical trial data is needed. [ABSTRACT FROM AUTHOR]

Published

2023

121. Figuring the 'cynical scientist' in British animal science: the politics of invisibility.

Author

Holmes, Tarquin and Friese, Carrie

Subjects

ANIMAL science, INVISIBILITY, ZOOLOGY, ANIMAL experimentation, LABORATORY animals, CYNICISM

Abstract

This paper investigates the 'cynical scientist' as a figure in British animal science discourse that developed in relation to the nineteenth-century emergence of the 'sceptical scientist'. Here, efforts by scientists to demarcate their profession's territory led to religious backlash against an alleged 'divorce' of British science from Christian morality. Animal experimentation became embroiled in this controversy through antivivisectionists' conviction that animal research was symptomatic of scientific scepticism and Continental atheism's malign influence. Accusations of cynicism ultimately forced British scientists to accept legal regulation following the 1875 Royal Commission on Vivisection. British scientists were, however, able to utilise their political leverage and credibility as experts to favourably influence licensing and inspection. We suggest that efforts to silence public claims of scientific cynicism may have enabled 'cynical scientists' to remain invisible and that this was marked by privilege and power, not marginality. Nevertheless, we argue that regulation and reforms have also worked to internalise within British animal science the notion that scientific cynicism must be combatted through proper governance and internal discipline. [ABSTRACT FROM AUTHOR]

Published

2023

122. Evaluation of a Balloon Implant for Simultaneous Magnetic Nanoparticle Hyperthermia and High-Dose-Rate Brachytherapy of Brain Tumor Resection Cavities.

Author

Wan, Shuying, Rodrigues, Dario B., Kwiatkowski, Janet, Khanna, Omaditya, Judy, Kevin D., Goldstein, Robert C., Overbeek Bloem, Marty, Yu, Yan, Rooks, Sophia E., Shi, Wenyin, Hurwitz, Mark D., and Stauffer, Paul R.

Subjects

PROSTHETICS, FEVER, BIOPSY, ANIMAL experimentation, ARTIFICIAL implants, GLIOMAS, MAGNETOTHERAPY, BRAIN tumors, RADIATION doses, RESEARCH funding, RADIOISOTOPE brachytherapy, NANOPARTICLES, RADIATION dosimetry, IN vivo toxicity testing

Abstract

Simple Summary: Glioblastoma (GBM) generally recurs locally with a dismal median survival of <18 months. Combining thermal therapy with radiation therapy enhances radiation response and improves clinical outcomes. This study evaluates a thermobrachytherapy balloon implant intended for the simultaneous heat and radiation treatment of tumor resection cavities. The data demonstrate that our prototype implant produces spherically symmetric heat and radiation dose distributions around the balloon, while the in vivo experiments confirm our ability to heat ≥40 °C at a 5 mm distance from the balloon surface in highly perfused pig brain tissue. The device is now ready for the finalization of regulatory approvals in anticipation of early-stage clinical investigation. Previous work has reported the design of a novel thermobrachytherapy (TBT) balloon implant to deliver magnetic nanoparticle (MNP) hyperthermia and high-dose-rate (HDR) brachytherapy simultaneously after brain tumor resection, thereby maximizing their synergistic effect. This paper presents an evaluation of the robustness of the balloon device, compatibility of its heat and radiation delivery components, as well as thermal and radiation dosimetry of the TBT balloon. TBT balloon devices with 1 and 3 cm diameter were evaluated when placed in an external magnetic field with a maximal strength of 8.1 kA/m at 133 kHz. The MNP solution (nanofluid) in the balloon absorbs energy, thereby generating heat, while an HDR source travels to the center of the balloon via a catheter to deliver the radiation dose. A 3D-printed human skull model was filled with brain-tissue-equivalent gel for in-phantom heating and radiation measurements around four 3 cm balloons. For the in vivo experiments, a 1 cm diameter balloon was surgically implanted in the brains of three living pigs (40–50 kg). The durability and robustness of TBT balloon implants, as well as the compatibility of their heat and radiation delivery components, were demonstrated in laboratory studies. The presence of the nanofluid, magnetic field, and heating up to 77 °C did not affect the radiation dose significantly. Thermal mapping and 2D infrared images demonstrated spherically symmetric heating in phantom as well as in brain tissue. In vivo pig experiments showed the ability to heat well-perfused brain tissue to hyperthermic levels (≥40 °C) at a 5 mm distance from the 60 °C balloon surface. [ABSTRACT FROM AUTHOR]

Published

2023

123. The Reification of Non-Human Animals.

Author

Caprioglio Panizza, Silvia

Subjects

SOCIOLOGY, HUMAN research subjects, ETHICS, ANIMAL experimentation, RESEARCH ethics, INTERPERSONAL relations, ANIMAL rights, PHILOSOPHY

Abstract

This paper takes up Axel Honneth's suggestion that we, in the 21st century Western world, should revisit the Marxian idea of reification; unlike Honneth, however, this paper applies reification to the ways in which humans relate to non-human animals, particularly in the context of scientific experiments. Thinking about these practices through the lens of reification, the paper argues, yields a more helpful understanding of what is regarded as problematic in those practices than the standard animal rights approaches. The second part of the paper offers ways of overcoming reification that go beyond Honneth's idea of recognition by introducing Iris Murdoch's idea of attention. This proposed strategy makes the ethical relevance of reification more salient and makes it possible to counter reification through a practice such as attention which, unlike recognition, can be consciously established. [ABSTRACT FROM AUTHOR]

Published

2023

124. The use of NAMs and omics data in risk assessment.

Author

Miccoli, Andrea, Marx‐Stoelting, Philip, and Braeuning, Albert

Subjects

RISK assessment, MORAL reasoning, ANIMAL experimentation, TOXICOGENOMICS, TWENTY-first century, CHEMICAL safety

Abstract

The animal‐centric approach so far predominantly employed in risk assessment has been questioned in recent years due to a number of shortcomings regarding performance, consistency, transferability of results, sustainability, costs and ethical reasons. Alternatives to animal testing, collectively termed NAMs, may have the potential to deliver sound, cost‐effective, prompt and reliable information, but their regulatory acceptance has not been established yet. The main reasons behind this are mostly related to actual methodological obstacles, with particular reference to addressing complex endpoints such as repeated‐dose toxicity, the issue of translating the concept of adversity to NAMs, and doubts of stakeholders about the level of chemical safety ensured by NAMs. With the aim of providing an updated view on major conceptual and methodological developments in the field of toxicology, a symposium and a workshop were organised by the German Federal Institute for Risk Assessment (Bundesinstitut für Risikobewertung, BfR) and Helmholtz Centre for Environmental Research on 15–17 November 2021 in Berlin. The conference, entitled 'Challenges in Public Health Protection in the 21st Century: New Methods, Omics and Novel Concepts in Toxicology' brought together eminent scientists with representatives from industry and regulatory authorities. The organisation, day‐to‐day operations and the reporting of the event main outcomes in a position paper were the main focus of the present EFSA EU‐FORA work programme. Tasks pertaining to 'The use of NAMs and omics data in risk assessment' were implemented under the shared supervision of units 'Testing and Assessment Strategies Pesticides' and 'Effect‐based Analytics and Toxicogenomics' of the German Federal Institute for Risk Assessment. [ABSTRACT FROM AUTHOR]

Published

2022

125. Design and Experimental Setup of a Robotic Medical Instrument for Brachytherapy in Non-Resectable Liver Tumors.

Author

Tucan, Paul, Vaida, Calin, Horvath, Daniel, Caprariu, Andrei, Burz, Alin, Gherman, Bogdan, Iakab, Stefan, and Pisla, Doina

Subjects

LIVER analysis, ROBOTICS equipment, TISSUE analysis, LIVER tumors, ANIMAL experimentation, SWINE, PRODUCT design, HYPODERMIC needles, INTERPROFESSIONAL relations, RADIOISOTOPE brachytherapy, SYSTEMS development

Abstract

Simple Summary: This paper presents an experimental study on a brachytherapy multi-needle insertion device, manipulated using a collaborative robot, to assess a set of characteristics: accuracy, needle deflection due to resistance forces, instrument and needle wear and the influence of insertion speed and rotation during needle manipulation inside the liver parenchyma. This paper presents a study regarding the design and the experimental setup of a medical robotic system for brachytherapy using tribology analysis. The robotic system is composed of a collaborative robotic arm and a multi-needle brachytherapy instrument controlled using a unified control system embedding a haptic device and force-feedback. This work is oriented towards identifying the technical characteristics of the system components to determine the accuracy of the procedure, as well as using different scenarios for needle insertion in ex vivo porcine liver tissue in order to determine the forces required for insertion and extraction of the needle and the friction coefficient that accompanies the previously mentioned forces. Subsequent to the computation of the friction forces, the normal forces and the wear during the needle insertion are determined with the scope of predicting the lifecycle of some components of the medical device. [ABSTRACT FROM AUTHOR]

Published

2022

126. Osteoinductive biomaterials: Machine learning for prediction and interpretation.

Author

Lin, Sicong, Zhuang, Yan, Chen, Ke, Lu, Jian, Wang, Kefeng, Han, Lin, Li, Mufei, Li, Xiangfeng, Zhu, Xiangdong, Yang, Mingli, Yin, Guangfu, Lin, Jiangli, and Zhang, Xingdong

Subjects

DATABASES, MACHINE learning, POROSITY, ANIMAL experimentation, BONE growth

Abstract

Biomaterials with osteoinductivity are widely used for bone defect repair due to their unique structures and functions. Machine learning (ML) is pivotal in analyzing osteoinductivity and accelerating new material design. However, challenges include creating a comprehensive database of osteoinductive materials and dealing with low-quality, disparate data. As a standard for evaluating the osteoinductivity of biomaterials, ectopic ossification has been used. This paper compiles research findings from the past thirty years, resulting in a robust database validated by experts. To tackle issues of limited data samples, missing data, and high-dimensional sparsity, a data enhancement strategy is developed. This approach achieved an area under the curve (AUC) of 0.921, a precision of 0.839, and a recall of 0.833. Model interpretation identified key factors such as porosity, bone morphogenetic protein-2 (BMP-2), and hydroxyapatite (HA) proportion as crucial determinants of outcomes. Optimizing pore structure and material composition through partial dependence plot (PDP) analysis led to a new bone area ratio of 14.7 ± 7 % in animal experiments, surpassing the database average of 10.97 %. This highlights the significant potential of ML in the development and design of osteoinductive materials. This study leverages machine learning to analyze osteoinductive biomaterials, addressing challenges in database creation and data quality. Our data enhancement strategy significantly improved model performance. By optimizing pore structure and material composition, we increased new bone formation rates, showcasing the vast potential of machine learning in biomaterial design. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

127. Effects of Flavonoids on Alcoholic Liver Disease: A Review.

Author

Li, Xiaoqing, Su, Yu, Zhao, Xinyue, Zhu, Hongguang, and Li, Zichao

Subjects

*HEPATIC fibrosis, *CIRRHOSIS of the liver, *TREATMENT effectiveness, *ANIMAL experimentation, *CYANIDIN, *QUERCETIN

Abstract

Alcoholic liver disease (ALD) encompasses a spectrum of manifestations from simple steatosis to steatohepatitis, progressive fibrosis, cirrhosis and liver cancer. Emerging research has spotlighted flavonoids as promising candidates for interfering the initiation, promotion and progression of ALD. Thus this paper provides a comprehensive exposition on the effects of flavonoids on ALD and elucidates the underlying mechanisms. The results show that luteolin, soyasaponin, and isoliquiritigenin have demonstrated the ability to reduce liver fat synthesis, regulate lipid metabolism, and mitigate the undesirable accumulation of fat in hepatocytes. Quercetin and genistein exhibit excellent antioxidant properties, inhibiting lipid peroxidation and oxidative stress, thereby alleviating cellular inflammation and reducing the damage caused by alcohol to hepatocytes. Naringin, cyanidin, and butein also show promise in resisting liver fibrosis. The therapeutic effects of flavonoids on ALD have been validated through cell and animal experiments. However, the application development of flavonoids in functional foods still faces challenges due to insufficient research and industrialization hurdles. [ABSTRACT FROM AUTHOR]

Published

2024

128. Ethical and societal aspects of radiological protection for offspring and next generations.

Author

Zölzer, F., Schneider, T., Ainsbury, E., Goto, A., Liutsko, L., O'Reilly, G., and Lochard, J.

Subjects

*VALUES (Ethics), *JUSTICE, *RISK perception, *ANIMAL experimentation, *RADIATION protection

Abstract

Purpose: Over the last decade or so, ethical and societal aspects of radiological protection have received increasing attention. This is also reflected in the publications of the International Commission on Radiological Protection (ICRP). The current paper aims at identifying relevant ethical and societal topics which should receive attention in the context of radiological protection for offspring and next generations. Materials and Methods: We present a non-comprehensive review of the subject, based on presentation made at an ICRP workshop in Budapest in 2022. We first discuss the ethical values promoted by ICRP, and the application of these values in cases of (potential) pre-conceptual and prenatal radiation exposures. We then consider experience gained after the Fukushima accident indicating particular societal concerns about the health effects of such exposures. Results and Conclusions: Beneficence/non-maleficence, prudence, justice and dignity, the "core values" of the system of radiological protection have special roles to play when heritable and/or in utero effects are to be considered. Prudence, in particular, must be taken account of in view of the fact that solid scientific data in humans are largely lacking in this area, and it is necessary to rely on insights from animal experiments as well as theoretical considerations. As regards societal considerations, the perception of risk among (potentially) affected populations needs to be taken seriously. Accountability, transparency, and inclusivity, the "procedural values" promoted by ICRP for the practical implementation of the system of radiological protection play a central role in overcoming skepticism and creating trust. Stakeholder involvement should emphasize cooperation and dialogue, which allows for the joint evaluation of an exposure situation by experts and affected people. [ABSTRACT FROM AUTHOR]

Published

2024

129. AALAS Position Statement on the Humane Care and Use of Laboratory Animals.

Subjects

Animals, United States, Animals, Laboratory, Animal Welfare, Animal Experimentation

Abstract

The American Association for Laboratory Animal Science endorses the United States Government "Principles for the Utilization and Care of Vertebrate Animals Used in Testing, Research, and Training" and requires that all papers published in Comparative Medicine report research conducted in conformance with these principles. Research for papers submitted from outside the United States must be in conformance with the guidelines of that country's government. The Editor reserves the right to reject papers reporting results of research not adhering to these principles.

Published

2023

130. AALAS Position Statement on the Humane Care and Use of Laboratory Animals.

Subjects

Animals, United States, Animals, Laboratory, Animal Welfare, Animal Experimentation

Abstract

The American Association for Laboratory Animal Science endorses the United States Government "Principles for the Utilization and Care of Vertebrate Animals Used in Testing, Research, and Training" and requires that all papers published in Comparative Medicine report research conducted in conformance with these principles. Research for papers submitted from outside the United States must be in conformance with the guidelines of that country's government. The Editor reserves the right to reject papers reporting results of research not adhering to these principles.

Published

2023

131. The power of effective study design in animal experimentation: Exploring the statistical and ethical implications of asking multiple questions of a data set.

Author

Ankeny RA, Whittaker AL, Ryan M, Boer J, Plebanski M, Tuke J, and Spencer SJ

Subjects

Male, Animals, Causality, Research Design, Animal Experimentation

Abstract

One of the chief advantages of using highly standardised biological models including model organisms is that multiple variables can be precisely controlled so that the variable of interest is more easily studied. However, such an approach often obscures effects in sub-populations resulting from natural population heterogeneity. Efforts to expand our fundamental understanding of multiple sub-populations are in progress. However, such stratified or personalised approaches require fundamental modifications of our usual study designs that should be implemented in Brain, Behavior and Immunity (BBI) research going forward. Here we explore the statistical feasibility of asking multiple questions (including incorporating sex) within the same experimental cohort using statistical simulations of real data. We illustrate and discuss the large explosion in sample numbers necessary to detect effects with appropriate power for every additional question posed using the same data set. This exploration highlights the strong likelihood of type II errors (false negatives) for standard data and type I errors when dealing with complex genomic data, where studies are too under-powered to appropriately test these interactions. We show this power may differ for males and females in high throughput data sets such as RNA sequencing. We offer a rationale for the use of alternative experimental and statistical strategies based on interdisciplinary insights and discuss the real-world implications of increasing the complexities of our experimental designs, and the implications of not attempting to alter our experimental designs going forward., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

132. The ethics of animal research and testing: A US perspective.

Author

Maciejewski EC, Basso MA, Miller CT, and Bailey MR

Subjects

Animals, Ethics, Research, Animal Welfare, Animal Testing Alternatives, Animal Experimentation

Abstract

Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.

Published

2023

133. Application of Implantable Polylactic-Co-Glycolic Acid Microcapsule in Repairing Alveolar Bone Defects.

Author

Jiang, Jun, Xiao, Jianpeng, Wang, Dongqing, and Cai, Huazhong

Subjects

PERIODONTITIS treatment, DIPHOSPHONATES, BONE resorption, PHARMACEUTICAL encapsulation, ANIMAL experimentation, BIOAVAILABILITY, ONE-way analysis of variance, ALVEOLAR process, POLYESTERS, RATS, HYDROCARBONS, DESCRIPTIVE statistics, DOSAGE forms of drugs, PHARMACODYNAMICS

Abstract

Alveolar bone defects (ABDs) were a perennial problem, especially in the aged. Bisphosphonates, especially etidronate sodium (ET), were frequently used in clinical treatment of ABD. However, the oral administration of ET had poor absorption (<1%). Therefore, optimization of a suitable dosage form substituted with ET to locally repair the ABD was a straightforward approach. Polylactide-co-glycolide (PLGA) is a biodegradable material and had been used in locally implanted medical devices. Therefore, an ET-PLGA microcapsule may help local delivery and prolong the activity of healing ABD. In this paper, a preparation method of ET-PLGA microcapsule was optimized by the single-factor investigation and response surface method. Subsequently, the rat ABD model was used to evaluate the enhancement effect of these microcapsules. Finally, the optimum parameters were determined as follows: 40% dichloromethane, 160 mg/mL PLGA, 10% internal aqua/oil phase, 4% PVA, and emulsifying for 10 min. These microcapsules were spherical in shape and fairly monodisperse in a particle size of 27,51 μm (PDI = 0.3), encapsulation rate 96.6%, and drug loading 4.58%. Compared with the ET groups, the total healing volume of ABD in ET-PLGA groups was significantly increased P < 0.05 . ET-PLGA microcapsules significantly enhanced the effect of ET on ABD. This study provided important technical support for the treatment of ABD with bisphosphonates by local administration. This paper has an exploratory significance for the development of water-soluble bioactive components with low bioavailability for ABD. [ABSTRACT FROM AUTHOR]

Published

2021

134. The 3Rs Principle in Animal Experimentation: A Legal Review of the State of the Art in Europe and the Case in Italy.

Author

Maestri, Enrico

Subjects

ANIMAL experimentation, ANIMAL welfare, LAW enforcement

Abstract

The aim of this paper is to describe the essential points of Italian and European legislation governing the use of animals in biomedical experimentation. A close look will be taken at the principles of the 3Rs, which represent the mainstay of the legal architecture based on which a correct interpretation may be drawn of the legislative documents on animal experimentation. Furthermore, this paper will address the ways in which Directive 2010/63/EU is implemented in Italian legislation on the welfare of laboratory animals. In addition to an assessment of legal issues (such as the scope of jurisdiction of supervisory authorities tasked with issuing authorizations), it will include a discussion of cases of inadequate and insufficient implementation of the requirements laid down by Directive 2010/63/EU. Both the consistency of the interpretation of national legislation with the Directive and the direct effectiveness of the Directive in national law, in which animal testing has been and still is the subject of heated debate between supporters and opponents, will be examined. [ABSTRACT FROM AUTHOR]

Published

2021

135. A State-of-the-Art Review on the Alternatives to Animal Testing for the Safety Assessment of Cosmetics.

Author

Silva, Rita José and Tamburic, Slobodanka

Subjects

ANIMAL experimentation, COSMETICS, COSMETICS industry, IRRITATION (Pathology)

Abstract

Almost a decade after the stipulated deadline in the 7th amendment to the EU Cosmetics Directive, which bans the marketing of animal-tested cosmetics in the EU from 2013, animal experimentation for cosmetic-related purposes remains a topic of animated debate. Cosmetic industry continues to be scrutinised for the practice, despite its leading role in funding and adopting innovation in this field. This paper aims to provide a state-of-the-art review of the field on alternative testing methods, also known as New Approach Methodologies (NAMs), with the focus on assessing the safety of cosmetic ingredients and products. It starts with innovation drivers and global regulatory responses, followed by an extensive, endpoint-specific overview of accepted/prospective NAMs. The overview covers main developments in acute toxicity, skin corrosion/irritation, serious eye damage/irritation, skin sensitisation, repeated dose toxicity, reproductive toxicity/endocrine disruption, mutagenicity/genotoxicity, carcinogenicity, photo-induced toxicity, and toxicokinetics. Specific attention was paid to the emerging in silico methodology. This paper also provides a brief overview of the studies on public perception of animal testing in cosmetics. It concludes with a view that educating consumers and inviting them to take part in advocacy could be an effective tool to achieve policy changes, regulatory acceptance, and investment in innovation. [ABSTRACT FROM AUTHOR]

Published

2022

136. Microscopic changes in the spleen due to feline infectious peritonitis.

Author

Lisova, Viktoriia and Kotliarov, Eduard

Subjects

MEDICAL cadavers, PERITONITIS, STAINS & staining (Microscopy), ANIMAL experimentation, AUTOPSY, FORMALDEHYDE, MICROSCOPY, CATS, DESCRIPTIVE statistics, SPLEEN

Abstract

The relevance of the study is that pathological and morphological changes with feline infectious peritonitis have been studied by few authors and are not fully described. The purpose of this study was to investigate the effect of the causative agent of infectious peritonitis on the structure of the spleen in cats. The paper highlights the results of histological studies of sections obtained from distinct parts of the spleen of cats of different ages who died from mixed (26 animals) and dry (7 animals) forms of infectious peritonitis. Sections were stained with haematoxylin and eosin according to the generally accepted method. The paper describes the details of microscopic changes in the spleen in dry and mixed forms of feline infectious peritonitis. It was found that these changes are not affected by the form of the disease but are characterized by features depending on the duration of its course. In cats in which the disease lasted up to three weeks before death, the red pulp of the spleen was unevenly swollen, infiltrated by lymphocytes and monocytes, in some places contained foci of necrotic cells, and red blood cells were absent. Changes in the white pulp were represented by hyperplasia of lymphoid nodules. These nodules were of varied sizes and were located eccentrically relative to the central arteries. There are no distinct lymphoid nodules around part of the central arteries. On the surface of the capsule, fibrinous-necrotic overlays are present in places, under which there is no mesothelium, and the capsule is infiltrated with lymphocytes and monocytes. In other areas, mesotheliocytes underwent distinct metaplasia from flat cells, they turned into columnar cells. In some areas of the spleen, some animals have no serous membrane. In cats with the disease lasting over three weeks, the red pulp is noticeably more swollen, and the lymphoid nodules are single and small. Other microscopic changes were the same as in animals that were ill for less than three weeks. The results of the study are of practical value for pathologists, as well as for scientists investigating the pathogenesis of feline infectious peritonitis [ABSTRACT FROM AUTHOR]

Published

2022

137. Factors influencing preclinicalin vivoevaluation of mumps vaccine strain immunogenicity

Author

Tihana Kurtović, Beata Halassy, Dubravko Forčić, Marija Brgles, and M. Lang Balija

Subjects

Animal Experimentation, Guinea Pigs, Immunology, Population, Drug Evaluation, Preclinical, Mumps Vaccine, Mumps virus, medicine.disease_cause, Virus, In vivo, Animals, Immunology and Allergy, Medicine, education, Immunization Schedule, Pharmacology, education.field_of_study, business.industry, Immunogenicity, Body Weight, Non-clinical vaccine immunogenicity assessment, In vivo bioassay optimization, Design of Experiments (DoE), Assay sensitivity, Vaccine efficacy, Research Papers, Treatment Outcome, Research Design, Mumps vaccine, Female, business

Abstract

Immunogenicity testing in animals is a necessary preclinical assay for demonstration of vaccine efficacy the results of which are often the basis for the decision whether to proceed or withdraw the further development of the novel vaccine candidate. However, in vivo assays are rarely, if at all, optimized and validated. Here we clearly demonstrate the importance of in vivo assay (mumps virus immunogenicity testing in guinea pigs) optimization for gaining reliable results and the suitability of Fractional factorial design of experiments (DoE) for such a purpose. By the use of DoE with resolution IV (2IV(4-1)) we clearly revealed that the parameters significantly increasing assay sensitivity were interval between animal immunisations followed by the body weight of experimental animals. The quantity (0 versus 2%) of the stabilizer (foetal bovine serum, FBS) in the sample was shown as non-influencing parameter in DoE setup. However, the separate experiment investigating only the FBS influence, and performed under other parameters optimally set, showed that FBS also influences the results of immunogenicity assay. Such finding indicated that (a) factors with strong influence on the measured outcome can hide the effects of parameters with modest/low influence and (b) the matrix of mumps virus samples to be compared for immunogenicity must be identical for reliable virus immunogenicity comparison. Finally the three mumps vaccine strains widely used for decades in the licenced vaccines were for the first time compared in an animal model, and results obtained were in line with their reported immunogenicity in human population supporting the predictive power of the optimized in vivo assay.

Published

2015

138. Potential for using a hermetically-sealed, positive-pressured isocage system for studies involving germ-free mice outside a flexible-film isolator

Author

Charlie C Hsu, Adeline M. Hajjar, Jaehun J Yi, Olesya Pershutkina, Lillian Maggio-Price, Susan Dowling, Stacey M Meeker, David A. C. Beck, and Jisun Paik

Subjects

Animal Experimentation, Microbiology (medical), Air, Isolator, Gastroenterology, Fecal bacteriotherapy, Fecal Microbiota Transplantation, Biology, Gut flora, biology.organism_classification, Housing, Animal, Microbiology, Gastrointestinal Microbiome, Mice, fluids and secretions, Infectious Diseases, Immunology, Hydrostatic Pressure, Animals, Germ-Free Life, Microbiome, Research Paper

Abstract

Germ-free mice are used to examine questions about the role of the gut microbiota in development of diseases. Generally these animals are maintained in semi-rigid or flexible-film isolators to ensure their continued sterility or, if colonized with specific microbiota, to ensure that no new species are introduced. Here, we describe the use of a caging system in which individual cages are hermetically sealed and have their own filtered positive airflow. This isopositive caging system requires less space and reduces animal housing costs. By using strict sterile techniques, we kept mice germ-free in this caging system for 12 weeks. We also used this caging system and approach to conduct studies evaluating a) the stability of the microbiome in germ-free mice receiving a fecal transplant and b) the stability of dietary-induced microbiota changes in fecal-transplanted mice. As has been shown in fecal transfer studies in isolators, we found that the transferred microbiota stabilizes as early as 2 weeks post transfer although recipient microbiota did not completely recapitulate those of the donors. Interestingly, we also noted some sex effects in these studies indicating that the sex of recipients or donors may play a role in colonization of microbiota. However, a larger study will be needed to determine what role, if any, sex plays in colonization of microbiota. Based on our studies, an isopositive caging system may be utilized to test multiple donor samples for their effects on phenotypes of mice in both normal and disease states even with limited available space for housing.

Published

2015

139. A Survey of Stakeholder Organisations on the Proposed New European Chemicals Policy

Author

Robert Combes and J. Dandrea

Subjects

Animal Experimentation, Drug Industry, Public Policy, Context (language use), Legislation, Animal Testing Alternatives, Animal Welfare, Toxicology, General Biochemistry, Genetics and Molecular Biology, White paper, Toxicity Tests, Member state, Animals, Humans, media_common.cataloged_instance, Medicine, European Union, European union, Health policy, media_common, business.industry, Research, Stakeholder, Public consultation, General Medicine, Public relations, Legislation, Drug, United Kingdom, Europe, Medical Laboratory Technology, Government, Law, business

Abstract

In February 2001, the European Commission published a White Paper proposing that a single new system of chemical regulation should be applied throughout the Member States of the European Union. The proposed Registration, Evaluation and Authorisation of Chemicals (REACH) system was to include both new and existing chemicals, with the aim of ensuring that sufficient pertinent data were made available to enable human health and the environment to be protected. The policy was founded on the principle of sustainable industrial development, and ambitiously attempted to incorporate the needs and views of key stakeholder organisations, such as industry, trade associations, consumer groups, environmentalists, animal welfarists and Member State governments. During the period between the publication of the White Paper and the on-line publication of consultation documents, as part of a public consultation exercise, in May 2003, many of these key stakeholder organisations produced material in support of or critical of the White Paper, either in part or as a whole. In this paper, we have attempted to review this extensive material and to present it in the context of the current chemical regulatory system that the REACH system will replace. Emphasis is placed on the impact of the new policy on the number of animals used in the testing regimes within the REACH system and the inclusion of alternative methods into the legislation. Although supportive of the overriding aims of the new policy, FRAME believes that the fundamental concept of a risk-free environment is flawed, and that the new REACH system will involve the unjustifiable use of millions of laboratory animals. The new policy does include alternative methods, particularly for baseset substances. Nevertheless, alternative testing methods that are already available have been excluded and replaced with outdated in vivo versions. There is also insufficient detail with regard to the further development and validation of alternative methods, particularly for substances of high concern, such as endocrine disrupters or reproductive toxins, for which no alternative testing methods currently exist.

Published

2003

140. Downregulation of lncRNA NEAT1 interacts with miR-374b-5p/PGAP1 axis to aggravate the development of osteoarthritis.

Author

Huang, Feiri, Su, Zhongliang, Yang, Jie, Zhao, Xizhen, and Xu, Yaozeng

Subjects

RNA metabolism, BIOCHEMISTRY, CARTILAGE cells, LIPOPOLYSACCHARIDES, REVERSE transcriptase polymerase chain reaction, FLOW cytometry, INTERLEUKINS, STAINS & staining (Microscopy), PHENOMENOLOGICAL biology, ANIMAL experimentation, WESTERN immunoblotting, APOPTOSIS, RATS, GENE expression, CELL cycle, OSTEOARTHRITIS, CELL proliferation, TUMOR necrosis factors, ENZYME-linked immunosorbent assay

Abstract

Background: Osteoarthritis (OA), characterized by inflammation and articular cartilage degradation, is a prevalent arthritis among geriatric population. This paper was to scrutinize the novel mechanism of long noncoding RNA (lncRNA) NEAT1 in OA etiology. Methods: A total of 10 OA patients and 10 normal individuals was included in this study. Cell model of OA was built in human normal chondrocytes induced by lipopolysaccharide (LPS). An OA Wistar rat model was established through intra-articular injection of L-cysteine and papain mixtures (proportion at 1:2) into the right knee. Quantitative reverse transcription-polymerase chain reaction was employed to ascertain the expression levels of NEAT1, microRNA (miR)-374b-5p and post-GPI attachment to protein 1 (PGAP1), while dual-luciferase reporter experiments were used for the validation of target relationship among them. Cell cycle and apoptosis were calculated by flow cytometry analysis. CCK-8 assay was done to evaluate the proliferative potentials of chondrocytes. The levels of cell cycle-related proteins (Cyclin A1, Cyclin B1 and Cyclin D2) and pro-apoptotic proteins (Caspase3 and Caspase9) were measured by western blotting. Tumor necrosis factor-alpha (TNF-α), interleukin-1beta (IL-1β) and IL-6 levels were determined via ELISA. Hematoxylin & eosin (HE) Staining was used for pathological examination in OA rats. Results: Pronounced downregulation of NEAT1 and PGAP1 and high amounts of miR-374b-5p were identified in OA patients, LPS-induced chondrocytes and OA rats. NEAT1 targeted miR-374b-5p to control PGAP1 expression. Loss of NEAT1 or upregulation of miR-374b-5p dramatically accelerated apoptosis, led to the G1/S arrest and promoted the secretion of inflammatory cytokines in LPS-induced chondrocytes, while ectopic expression of PGAP1 exhibited the opposite influences on chondrocytes. Additionally, we further indicated that upregulation of miR-374b-5p attenuated the effects of PGAP1 overexpression on LPS-induced chondrocytes. Conclusions: Reduced NEAT1 induces the development of OA via miR-374b-5p/PGAP1 pathway. This suggests that the regulatory axis NEAT1/miR-374b-5p/PGAP1 is a novel and prospective target for OA treatment. [ABSTRACT FROM AUTHOR]

Published

2023

141. A Comparative Analysis of Orthotopic and Subcutaneous Pancreatic Tumour Models: Tumour Microenvironment and Drug Delivery.

Author

Fernandez, Jessica Lage, Årbogen, Sara, Sadeghinia, Mohammad Javad, Haram, Margrete, Snipstad, Sofie, Torp, Sverre Helge, Einen, Caroline, Mühlenpfordt, Melina, Maardalen, Matilde, Vikedal, Krister, and Davies, Catharina de Lange

Subjects

PANCREATIC tumors, BIOLOGICAL models, DRUG delivery systems, COLLAGEN, ANIMAL experimentation, CELL physiology, RESEARCH funding, HISTOLOGY, MICE

Abstract

Simple Summary: Pancreatic tumours present significant treatment challenges due to their resistance to chemotherapy and complex tumour microenvironment. Choosing the appropriate preclinical models and understanding how their characteristics affect drug delivery to the tumours is essential for designing clinically relevant experiments. This study investigates pancreatic tumours growing orthotopically or subcutaneously and presents the properties of their tumour microenvironments and their impacts on drug delivery. Pancreatic ductal adenocarcinoma (PDAC) remains a challenging malignancy, mainly due to its resistance to chemotherapy and its complex tumour microenvironment characterised by stromal desmoplasia. There is a need for new strategies to improve the delivery of drugs and therapeutic response. Relevant preclinical tumour models are needed to test potential treatments. This paper compared orthotopic and subcutaneous PDAC tumour models and their suitability for drug delivery studies. A novel aspect was the broad range of tumour properties that were studied, including tumour growth, histopathology, functional vasculature, perfusion, immune cell infiltration, biomechanical characteristics, and especially the extensive analysis of the structure and the orientation of the collagen fibres in the two tumour models. The study unveiled new insights into how these factors impact the uptake of a fluorescent model drug, the macromolecule called 800CW. While the orthotopic model offered a more clinically relevant microenvironment, the subcutaneous model offered advantages for drug delivery studies, primarily due to its reproducibility, and it was characterised by a more efficient drug uptake facilitated by its collagen organisation and well-perfused vasculature. The tumour uptake seemed to be influenced mainly by the structural organisation and the alignment of the collagen fibres and perfusion. Recognising the diverse characteristics of these models and their multifaceted impacts on drug delivery is crucial for designing clinically relevant experiments and improving our understanding of pancreatic cancer biology. [ABSTRACT FROM AUTHOR]

Published

2023

142. Validation of the presence of fast exchanging amine CEST effect at low saturation powers and its influence on the quantification of APT.

Author

Sun, Casey, Zhao, Yu, and Zu, Zhongliang

Subjects

ANIMAL experimentation, AMINES, FOREIGN exchange rates, MAGNETIZATION transfer

Abstract

Purpose: Accurately quantifying the amide proton transfer (APT) effect and the underlying exchange parameters is crucial for its applications, but previous studies have reported conflicting results. In these quantifications, the CEST effect from the fast exchange amine was always ignored because it was considered weak with low saturation powers. This paper aims to evaluate the influence of the fast exchange amine CEST on the quantification of APT at low saturation powers. Methods: A quantification method with low and high saturation powers was used to distinguish APT from the fast exchange amine CEST effect. Simulations were conducted to assess the method's capability to separate APT from the fast exchange amine CEST effect. Animal experiments were performed to assess the relative contributions from the fast exchange amine and amide to CEST signals at 3.5 ppm. Three APT quantification methods, each with varying degrees of contamination from the fast exchange amine, were employed to process the animal data to assess the influence of the amine on the quantification of APT effect and the exchange parameters. Results: The relative size of the fast exchange amine CEST effect to APT effect gradually increases with increasing saturation power. At 9.4 T, it increases from approximately 20% to 40% of APT effect with a saturation power increase from 0.25 to 1 μT. Conclusion: The fast exchange amine CEST effect leads overestimation of APT effect, fitted amide concentration, and amide–water exchange rate, potentially contributing to the conflicting results reported in previous studies. [ABSTRACT FROM AUTHOR]

Published

2023

143. Damage of the swarmer Pseudomonas soil isolate cell by UVc as revealed by transmission electron microscopy.

Author

Ben Ghorbal Salma, Kloula, Abdelwahed Inès, Mehri, Rim, Werhani, and Chatti, Abdelwaheb

Subjects

MICROBIAL ecology, ELECTRONS, ANIMAL experimentation, ELECTRON microscopy, PSEUDOMONAS, CYTOLOGY, ULTRAVIOLET radiation, BACTERIA, CELL death, MICROBIAL sensitivity tests, CYTOPLASM

Abstract

The modeling of the response of living organisms to a change in environment is an important issue of current interest. An example is the effect of ultraviolet radiation on biological systems. In this paper, molecular and analytical identification of Pseudomonas isolate were reported. Then, swarmer Pseudomonas cells were exposed to UVc radiations. The spatiotemporal response of swarmer Pseudomonas, to UVc exposure, was followed. Observing alterations in bacterial membrane integrity by electron microscopy can help to clarify the detailed mechanisms of resistance to UVc. The most evident changes were related to membrane structures. In the cytoplasm, the main finding was the appearance of round mesosomes as intracellular bilayered membranes. Another impact of UVc on Pseudomonas was evident from the appearance of additional membrane structures. In accordance with the viability results, UVc-induced ultrastructural changes of Pseudomonas membrane structures were identified, resulting in cell death, through a multistage model of UVc inactivation. [ABSTRACT FROM AUTHOR]

Published

2023

144. Zebrafish Model Insights into Mediterranean Diet Liquids: Olive Oil and Wine.

Author

Silva, Paula, Rodríguez-Pérez, María, and Burgos-Ramos, Emma

Subjects

OLIVE oil, MEDITERRANEAN diet, BRACHYDANIO, WINES, LIQUIDS, ANIMAL experimentation

Abstract

In this review, we explored the potential of a zebrafish model to investigate the antioxidant effects of key components of the Mediterranean diet, namely, olive oil and wine, in the context of preventing age-related diseases, particularly cardiovascular conditions. This paper explores the spectrum of observational studies to preclinical investigations and ultimately converges toward potential translational insights derived from animal experimentation. This review highlights the potential and underutilization of zebrafish as an experimental model in this domain. We highlighted the genetic proximity of zebrafish to humans, offering a unique opportunity for translational insights into the health benefits of olive oil and wine. Indeed, we wanted to focus on the potential of zebrafish to elucidate the health benefits of olive oil and wine while calling for continued exploration to unlock its full potential to advance our knowledge of age-related disease prevention within the Mediterranean diet framework. [ABSTRACT FROM AUTHOR]

Published

2023

145. KNOWLEDGE MAPPING OF INFLAMMASOME AND PYROPTOSIS IN STROKE: A BIBLIOMETRIC ANALYSIS (2007-2023).

Author

Mingfen Wu, Aning Sun, Hailun Jiang, Yinan Zhang, Zhigang Zhao, and Bin Zhu

Subjects

*STROKE, *BIBLIOMETRICS, *INFLAMMASOMES, *PYROPTOSIS, *ANIMAL experimentation

Abstract

Background: Stroke is a major contributor to disability and death worldwide. Studies have demonstrated that inflammasome/pyroptosis and its mediated inflammatory response are important factors aggravating brain injury after stroke. We aimed to investigate and map the knowledge structure and global trends on inflammasome/pyroptosis in stroke. Methods: All relevant documents were obtained from the Web of Science on 5 June 2023. Bibliometric visualization diagrams were created using VOSviewer and CiteSpace. Excel was used for statistical analysis and drawing graphs. Results: A total of 1106 publications were included, with more articles published each year, especially since 2014. China (740 papers), Zhejiang University (57 papers), Wang J (25 papers), and the Journal of Neuroinflammation (45 papers) were the most productive countries, institutions, authors, and journals, respectively. The United States was the country with highest centrality (0.56) and total link strength (171), and all of the top 10 institutions were in China. China and the U.S. cooperated closely. The centralities of the top 10 authors were all lower than 0.01; no leader has yet emerged in this field. "NLRP3 inflammasome" ranked first with 447 occurrences among 2136 keywords, of which 56 terms appeared more than 10 times when categorized into four clusters: cluster 1 (inflammation), cluster 2 (pyroptosis), cluster 3 (NLRP3 inflammasome), and cluster 4 (neuroinflammation). The studies focused on the mechanisms of inflammasome/pyroptosis in stroke were mainly limited to cell and animal experiments. Conclusion: Interest in inflammasome/pyroptosis in stroke is progressively increasing. The NLRP3 inflammasome is the most extensively studied and has been a research hotspot. The mechanisms of cell death in stroke are complex and future studies are needed to strengthen the clinical research on the relationship between pyroptosis-related processes and stroke, determine at which stage NLRP3 inflammasome activation, and clarify the detailed mechanism of NLRP3 in stroke. [ABSTRACT FROM AUTHOR]

Published

2023

146. Application of three-dimensional cell culture technology in screening anticancer drugs.

Author

Sun, Yaqian and Ma, Haiyang

Subjects

CELL culture, ANTINEOPLASTIC agents, MEDICAL screening, ANIMAL experimentation, DRUG resistance, DRUG efficacy

Abstract

The drug development process involves a variety of drug activity evaluations, which can determine drug efficacy, strictly analyze the biological indicators after the drug action, and use these indicators as the preclinical drug evaluation criteria. At present, most of the screening of preclinical anticancer drugs mainly relies on traditional 2D cell culture. However, this traditional technology cannot simulate the tumor microenvironment in vivo, let alone reflect the characteristics of solid tumors in vivo, and has a relatively poor ability to predict drug activity. 3D cell culture is a technology between 2D cell culture and animal experiments, which can better reflect the biological state in vivo and reduce the consumption of animal experiments. 3D cell culture can link the individual study of cells with the study of the whole organism, reproduce in vitro the biological phenotype of cells in vivo more greatly, and thus predict the activity and resistance of anti-tumor drugs more accurately. In this paper, the common techniques of 3D cell culture are discussed, with emphasis on its main advantages and application in the evaluation of anti-tumor resistance, which can provide strategies for the screening of anti-tumor drugs. [ABSTRACT FROM AUTHOR]

Published

2023

147. The Putative S1PR1 Modulator ACT-209905 Impairs Growth and Migration of Glioblastoma Cells In Vitro.

Author

Bien-Möller, Sandra, Chen, Fan, Xiao, Yong, Köppe, Hanjo, Jedlitschky, Gabriele, Meyer, Ulrike, Tolksdorf, Céline, Grube, Markus, Marx, Sascha, Tzvetkov, Mladen V., Schroeder, Henry W. S., and Rauch, Bernhard H.

Subjects

ANIMAL experimentation, CULTURE media (Biology), GLIOMAS, CELL receptors, ANTINEOPLASTIC agents, CULTURES (Biology), CELL motility, CELL survival, IMMUNOBLOTTING, CELLULAR signal transduction, TRANSFERASES, RESEARCH funding, CELL lines, DRUG resistance in cancer cells, ANTIGENS, MONOCYTES, PHARMACODYNAMICS

Abstract

Simple Summary: In this paper, we report on the inhibition of glioblastoma (GBM) cell growth and migration by the putative S1PR1 modulator ACT-2009905, using appropriate in vitro models. This work is based on our previously published finding that S1PR1 expression is strongly up-regulated in human glioblastoma samples and the fact that there is an association between S1PR1 with patients' survival times. We now show that pharmacological modulation by the putative S1PR1 modulator ACT-209905 inhibits GBM cell growth and migration. Furthermore, we investigated the influence of co-culture of GBM cells with THP-1 cells as a model for human monocytes, showing pro-tumoral effects and arguing for a complex interplay between GBM cells, immune cells and underlying signaling pathways. We believe that this manuscript fits the interests of the readership of the journal Cancers as it addresses the impact of alternative therapeutic options using ACT-209905 for improving GBM therapy. Glioblastoma (GBM) is still a deadly tumor due to its highly infiltrative growth behavior and its resistance to therapy. Evidence is accumulating that sphingosine-1-phosphate (S1P) acts as an important tumor-promoting molecule that is involved in the activation of the S1P receptor subtype 1 (S1PR1). Therefore, we investigated the effect of ACT-209905 (a putative S1PR1 modulator) on the growth of human (primary cells, LN-18) and murine (GL261) GBM cells. The viability and migration of GBM cells were both reduced by ACT-209905. Furthermore, co-culture with monocytic THP-1 cells or conditioned medium enhanced the viability and migration of GBM cells, suggesting that THP-1 cells secrete factors which stimulate GBM cell growth. ACT-209905 inhibited the THP-1-induced enhancement of GBM cell growth and migration. Immunoblot analyses showed that ACT-209905 reduced the activation of growth-promoting kinases (p38, AKT1 and ERK1/2), whereas THP-1 cells and conditioned medium caused an activation of these kinases. In addition, ACT-209905 diminished the surface expression of pro-migratory molecules and reduced CD62P-positive GBM cells. In contrast, THP-1 cells increased the ICAM-1 and P-Selectin content of GBM cells which was reversed by ACT-209905. In conclusion, our study suggests the role of S1PR1 signaling in the growth of GBM cells and gives a partial explanation for the pro-tumorigenic effects that macrophages might have on GBM cells. [ABSTRACT FROM AUTHOR]

Published

2023

148. Animal experiments on respiratory viruses and analogous studies of infection factors for interpersonal transmission.

Author

Liao Y, Guo S, Mao N, Li Y, Li J, and Long E

Subjects

Humans, Animals, SARS-CoV-2, Conservation of Natural Resources, Environmental Policy, COVID-19, Animal Experimentation

Abstract

Air pollution caused by SARS-CoV-2 and other viruses in human settlements will have a great impact on human health, but also a great risk of transmission. The transmission power of the virus can be represented by quanta number in the Wells-Riley model. In order to solve the problem of different dynamic transmission scenarios, only a single influencing factor is considered when predicting the infection rate, which leads to large differences in quanta calculated in the same space. In this paper, an analog model is established to define the indoor air cleaning index RL and the space ratio parameter. Based on infection data analysis and rule summary in animal experiments, factors affecting quanta in interpersonal communication were explored. Finally, by analogy, the factors affecting person-to-person transmission mainly include viral load of infected person, distance between individuals, etc., the more severe the symptoms, the closer the number of days of illness to the peak, and the closer the distance to the quanta. In summary, there are many factors that affect the infection rate of susceptible people in the human settlement environment. This study provides reference indicators for environmental governance under the COVID-19 epidemic, provides reference opinions for healthy interpersonal communication and human behavior, and provides some reference for accurately judging the trend of epidemic spread and responding to the epidemic., (© 2023. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2023

149. Reporting and interpreting non-significant results in animal cognition research.

Author

Farrar BG, Vernouillet A, Garcia-Pelegrin E, Legg EW, Brecht KF, Lambert PJ, Elsherif M, Francis S, O'Neill L, Clayton NS, and Ostojić L

Subjects

Animals, Cognition, Research Design, Animal Experimentation

Abstract

How statistically non-significant results are reported and interpreted following null hypothesis significance testing is often criticized. This issue is important for animal cognition research because studies in the field are often underpowered to detect theoretically meaningful effect sizes, i.e. , often produce non-significant p -values even when the null hypothesis is incorrect. Thus, we manually extracted and classified how researchers report and interpret non-significant p -values and examined the p -value distribution of these non-significant results across published articles in animal cognition and related fields. We found a large amount of heterogeneity in how researchers report statistically non-significant p -values in the result sections of articles, and how they interpret them in the titles and abstracts. Reporting of the non-significant results as "No Effect" was common in the titles (84%), abstracts (64%), and results sections (41%) of papers, whereas reporting of the results as "Non-Significant" was less common in the titles (0%) and abstracts (26%), but was present in the results (52%). Discussions of effect sizes were rare (<5% of articles). A p -value distribution analysis was consistent with research being performed with low power of statistical tests to detect effect sizes of interest. These findings suggest that researchers in animal cognition should pay close attention to the evidence used to support claims of absence of effects in the literature, and-in their own work-report statistically non-significant results clearly and formally correct, as well as use more formal methods of assessing evidence against theoretical predictions., Competing Interests: Ljerka Ostojić is an Academic Editor for PeerJ., (©2023 Farrar et al.)

Published

2023

150. The Role of TAMs in Tumor Microenvironment and New Research Progress.

Author

Feng, Yawei, Ye, Zhiqiang, Song, Furong, He, Yufeng, and Liu, Jun

Subjects

TUMOR microenvironment, METASTASIS, ANIMAL experimentation, CANCER treatment

Abstract

Tumor-associated macrophages (TAMs) are an important part of tumor microenvironment (TME) and play a key role in TME, participating in the process of tumor occurrence, growth, invasion, and metastasis. Among them, metastasis to tumor tissue is the key step of malignant development of tumor. In this paper, the latest progress in the role of TAMs in the formation of tumor microenvironment is summarized. It is particularly noteworthy that cell and animal experiments show that TAMs can provide a favorable microenvironment for the occurrence and development of tumors. At the same time, clinical pathological experiments show that the accumulation of TAMs in tumor is related to poor clinical efficacy. Finally, this paper discusses the feasibility of TAMs-targeted therapy as a new indirect cancer therapy. This paper provides a theoretical basis for finding a potentially effective macrophage-targeted tumor therapy. [ABSTRACT FROM AUTHOR]

Published

2022