Your search keyword '"CHEMICAL inhibitors"' showing total 6,671 results

1. Genetically Proxied Interleukin‐13 Inhibition Is Associated With Risk of Psoriatic Disease: A Mendelian Randomization Study.

Author

Zhao, Sizheng Steven, Hyrich, Kimme, Yiu, Zenas, Barton, Anne, and Bowes, John

Subjects

*PREVENTION of drug side effects, *THERAPEUTIC use of monoclonal antibodies, *RISK assessment, *LEUKOCYTE count, *PSORIATIC arthritis, *PSORIASIS, *MOLECULAR epidemiology, *RESEARCH funding, *ANKYLOSIS, *IMMUNOGLOBULINS, *CELLULAR signal transduction, *DESCRIPTIVE statistics, *MONOCLONAL antibodies, *ODDS ratio, *PHYSICIAN practice patterns, *GENETIC mutation, *HUMAN genome, *SPONDYLOARTHROPATHIES, *CONFIDENCE intervals, *DRUG prescribing, *PHYSICIANS, *INTERLEUKINS, *GENETICS, *EOSINOPHILS, *BIOMARKERS, *DISEASE risk factors, *CHEMICAL inhibitors

Abstract

Objective: Inhibitors of the interleukin 13 (IL‐13) pathway, such as dupilumab, are licensed for atopic dermatitis and asthma. Adverse events resembling psoriatic disease after dupilumab initiation have been reported, but evidence is limited to case reports with uncertain causality. We aimed to investigate whether genetically mimicked IL‐13 inhibition (IL‐13i) is associated with risk of psoriatic arthritis (PsA) and psoriasis. Methods: We instrumented IL‐13i using a protein‐coding variant in the IL13 gene, rs20541, that is associated with circulating eosinophil count (biomarker of IL‐13i) at genome‐wide significance in a study of 563,946 individuals. Outcome genetic data were taken from studies of PsA, psoriasis, and related spondyloarthritis traits in up to 10,588 cases and 209,287 controls. Colocalization analysis was performed to examine genetic confounding. We additionally used circulating IgE as a biomarker to test whether associations were replicated, both in the test and in an independent genetic dataset. We also replicated analyses using individual‐level data from the UK Biobank. Results: Genetically proxied IL‐13i was associated with increased risk of PsA (odds ratio [OR] 37.39; 95% confidence interval [95% CI] 11.52–121.34; P = 1.64 × 10−9) and psoriasis (OR 20.08; 95% CI 4.38–92.01; P = 1.12 × 10−4). No consistent associations were found for Crohn disease, ulcerative colitis, ankylosing spondylitis, or iritis. Colocalization showed no strong evidence of genetic confounding for psoriatic disease. Results were replicated using circulating IgE for the exposure, using independent outcome data and using individual‐level data. Conclusion: We provide supportive genetic evidence that IL‐13i is linked to increased risk of PsA and psoriasis. Physicians prescribing IL‐13 inhibitors should be vigilant for these adverse events. [ABSTRACT FROM AUTHOR]

Published

2024

2. Safety, Tolerability, and Pharmacokinetics of Single Doses of Exidavnemab (BAN0805), an Anti‐α‐Synuclein Antibody, in Healthy Western, Caucasian, Japanese, and Han Chinese Adults.

Author

Boström, Emma, Bachhav, Sagar S., Xiong, Hao, Zadikoff, Cindy, Li, Qingbo, Cohen, Eric, Dreher, Ingeborg, Torrång, Anna, Osswald, Gunilla, Moge, Mikael, Appelkvist, Paulina, Fälting, Johanna, and Odergren, Tomas

Subjects

*DRUG therapy for Parkinson's disease, *RISK assessment, *PATIENT safety, *RESEARCH funding, *SYNUCLEINS, *WHITE people, *DESCRIPTIVE statistics, *DOSE-effect relationship in pharmacology, *DRUG efficacy, *DOSAGE forms of drugs, *GENETIC techniques, *BIOMARKERS, *EVALUATION, *CHEMICAL inhibitors, *ADULTS

Abstract

Exidavnemab is a monoclonal antibody (mAb) with a high affinity and selectivity for pathological aggregated forms of α‐synuclein and a low affinity for physiological monomers, which is in clinical development as a disease‐modifying treatment for patients with synucleinopathies such as Parkinson's disease. Safety, tolerability, pharmacokinetics, immunogenicity, and exploratory biomarkers were assessed in two separate Phase 1 single ascending dose studies, including single intravenous (IV) (100 to 6000 mg) or subcutaneous (SC) (300 mg) administration of exidavnemab in healthy volunteers (HVs). Across the two studies, a total of 98 Western, Caucasian, Japanese, and Han Chinese HVs were enrolled, of which 95 completed the study. Exidavnemab was generally well tolerated. There were no serious adverse events or safety issues identified in laboratory analyses. Headache, asymptomatic COVID‐19, back pain, and post lumbar puncture syndrome were the most frequently reported treatment‐emergent adverse events. Following IV infusion, the pharmacokinetics of exidavnemab was approximately dose linear in the range 100‐6000 mg. The terminal half‐life was approximately 30 days, and the exposure was comparable across Western, Caucasian, Japanese, and Han Chinese volunteers. The absolute SC bioavailability was ∼71%. Cerebrospinal fluid exposure relative to serum after single dose was within the range expected for mAbs (approximately 0.2%). The anti‐drug antibody rates were low and there was no effect of immunogenicity on the pharmacokinetics or safety. Dose‐dependent reduction of free α‐synuclein in plasma was observed. In summary, exidavnemab was found to have an excellent pharmacokinetic profile and was well tolerated in HVs, supporting the continued clinical development. [ABSTRACT FROM AUTHOR]

Published

2024

3. A Model‐Informed Drug Development Approach Supporting the Approval of an Unstudied Valbenazine Dose for Patients With Tardive Dyskinesia.

Author

Nguyen, Hoa Q., Kuan, Han‐Yi Steve, Crass, Ryan L., Quinlan, Lauren, Chapel, Sunny, Kim, Kristine, Brar, Satjit, and Loewen, Gordon

Subjects

*HETEROCYCLIC compounds, *TARDIVE dyskinesia, *RESEARCH funding, *CARRIER proteins, *STATISTICAL sampling, *BLIND experiment, *PILOT projects, *RANDOMIZED controlled trials, *DESCRIPTIVE statistics, *DOSE-effect relationship in pharmacology, *DRUG approval, *VALINE, *LONGITUDINAL method, *DRUG efficacy, *ADRENERGIC uptake inhibitors, *DRUG development, *COMPARATIVE studies, *CONFIDENCE intervals, *MEMBRANE proteins, *CHEMICAL inhibitors

Abstract

Valbenazine is a highly potent and selective inhibitor of synaptic vesicular monoamine transporter 2. The current therapeutic doses of valbenazine for tardive dyskinesia (TD) are 40, 60, or 80 mg capsules, given orally, once daily (QD). While 40 and 80 mg were investigated in phase 3 KINECT® 3 trial and initially approved, the approval of valbenazine 60 mg was based on the analysis utilizing the Model‐informed drug development (MIDD) approach, facilitated through the US Food and Drug Administration's MIDD Pilot Program. This study aimed to demonstrate the efficacy of 60 mg QD dose through model simulations using an established exposure‐response (E‐R) relationship between valbenazine active metabolite [+]‐α‐dihydrotetrabenazine exposure and the change from baseline in Abnormal Involuntary Movement Scale total score (AIMS‐CFB). A longitudinal E–R model was constructed based on the 40 and 80 mg data from the KINECT 3 trial. The final Emax model adequately predicted dose‐dependent improvement in the primary endpoint and was used to interpolate AIMS‐CFB for 60 mg at week 6. The efficacy of the unstudied 60 mg dose regimen is expected to be within the range of doses studied clinically with predicted mean AIMS‐CFB (95% confidence interval) of −2.69 (−3.30, −2.13) between observed mean AIMS‐CFB for 40 mg of −1.92 and 80 mg of −3.39. Results from this analysis provided the key evidence to establish efficacy of 60 mg QD without the need for an additional clinical trial. The availability of valbenazine 60 mg dose fills an existing medical need for patients with TD who could benefit from this third effective dose. [ABSTRACT FROM AUTHOR]

Published

2024

4. Safety, Pharmacokinetics, and Pharmacodynamics of the New Aldose Reductase Inhibitor Govorestat (AT‐007) After a Single and Multiple Doses in Participants in a Phase 1/2 Study.

Author

Perfetti, Riccardo, Bailey, Evan, Wang, Stella, Mills, Richard, Mohanlal, Ramon, and Shendelman, Shoshana

Subjects

*PATIENT safety, *RESEARCH funding, *ENZYME inhibitors, *STATISTICAL sampling, *HEXOSES, *RANDOMIZED controlled trials, *DESCRIPTIVE statistics, *GALACTOSEMIA, *DOSE-effect relationship in pharmacology, *OXIDOREDUCTASES, *RESEARCH, *ALCOHOLS (Chemical class), *TRANSFERASES, *CONFIDENCE intervals, *DATA analysis software, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

In classic galactosemia (CG) patients, aldose reductase (AR) converts galactose to galactitol. In a phase 1/2, placebo‐controlled study (NCT04117711), safety, pharmacokinetics (PK), and pharmacodynamics (PD) of govorestat were evaluated after single and multiple ascending doses (0.5‐40 mg/kg) in healthy adults (n = 81) and CG patients (n = 14). Levels of govorestat in plasma and cerebrospinal fluid (CSF) and blood levels of galactitol, galactose, and galactose‐1‐phosphate (Gal‐1p) were measured for population PK and PK/PD analyses. Govorestat was well tolerated. Adverse event frequency was comparable between placebo and govorestat. Govorestat PK displayed a 2‐compartment model with sequential zero‐ and first‐order absorption, and no effect of demographic factors. Multiple‐dose PK of govorestat was linear in the 0.5‐40 mg/kg range, and CSF levels increased dose dependently. Elimination half‐life was ∼10 h. PK/PD modeling supported once‐daily dosing. Change from baseline in galactitol was −15% ± 9% with placebo and −19% ± 10%, −46% ± 4%, and −51% ± 5% with govorestat 5, 20, and 40 mg/kg, respectively, thus was similar for 20 and 40 mg/kg. Govorestat did not affect galactose or Gal‐1p levels. In conclusion, govorestat displayed a favorable safety, PK, and PD profile in humans, and reduced galactitol levels in the same magnitude (∼50%) as in a rat model of CG that demonstrated an efficacy benefit on neurological, behavioral, and ocular outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

5. Drug‐Drug Interaction between Oral Zamicastat and Continuous Epoprostenol Infusion at Steady‐State Conditions in Healthy Subjects.

Author

Fonseca, Marlene, Guimarães, Andreia, Gama, Helena, Magalhães, Luís, Henriques, Sara Carolina, Silva, Nuno, Almeida, Luis, and Soares‐da‐Silva, Patrício

Subjects

*PROSTACYCLIN, *RESEARCH funding, *DOPAMINE uptake inhibitors, *ORAL drug administration, *DESCRIPTIVE statistics, *INTRAVENOUS therapy, *METABOLITES, *OXIDOREDUCTASES, *DRUG interactions, *CONFIDENCE intervals, *BIOAVAILABILITY, *DRUG tolerance, *CARDIOVASCULAR system, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

This study intended to evaluate the interactions between zamicastat and epoprostenol in healthy human subjects. This was a single‐center, open‐label, two‐period study. In period 1, epoprostenol 8 ng/kg/min was administered alone. In period 2, epoprostenol 8 ng/kg/min was administered following an 8‐day treatment with zamicastat. Since the initial dose of epoprostenol showed to be insufficiently tolerated, it was decreased to 6 ng/kg/min. Blood samples were collected to determine the metabolites of epoprostenol and concentrations of zamicastat and its metabolites. A total of 54 subjects were enrolled and data from 28 subjects were available for pharmacokinetic analysis. The epoprostenol plus zamicastat‐to‐epoprostenol geometric means ratio (GMR) and corresponding 90% confidence interval (CI) for Cav,ss and area under the plasma concentration–time curve from time 0 up to 16 h at steady state (AUC0‐16,ss) of the metabolites of epoprostenol were within the acceptance bioequivalence range (80.00%‐125.00%). The intrasubject coefficient of variation (ISCV) was below 10% for both parameters, on both metabolites. For zamicastat AUC0‐τ,ss, the zamicastat plus epoprostenol‐to‐zamicastat GMR and corresponding 90% CI were within the bioequivalence acceptance range, while for zamicastat Cmax,ss, the lower limit of the 90% CI was slightly below the acceptance range. For zamicastat metabolites, Cmax,ss and AUC0‐τ,ss and the zamicastat plus epoprostenol‐to‐zamicastat GMR were below the acceptance bioequivalence range. ISCV was between 30% and 41% for Cmax,ss and between 21% and 41% for AUC0‐τ,ss, for zamicastat and both metabolites. This study showed that the administration of zamicastat did not significantly modify the cardiovascular effects of epoprostenol and that the interactions between zamicastat and epoprostenol are not expected to be clinically relevant. [ABSTRACT FROM AUTHOR]

Published

2024

6. Temperature‐sensitive sodium beta‐glycerophosphate/chitosan hydrogel loaded with all‐trans retinoic acid regulates Pin1 to inhibit the formation of spinal cord injury‐induced rat glial scar.

Author

Zhang, Rongmou, Tang, Ting, Zhuang, Huafeng, Wang, Peiwen, Yu, Haiming, Xu, Hao, and Yao, Xuedong

Subjects

*NERVOUS system regeneration, *CHEMICAL inhibitors, *SPINAL cord injuries, *SPINAL cord, *TRETINOIN

Abstract

Glial scar formation is a major obstacle to nerve regeneration following spinal cord injury (SCI). Pin1 and the PI3K/AKT/CDK2 signaling pathway play crucial roles in neuronal regulation, but research on their involvement in glial scarring remains limited. In this study, we have for the first time observed that Pin1, PI3K, AKT, and CDK2 are upregulated and interact with each other following SCI. Further experiments revealed that Pin1 contributes to the development of glial scars by promoting astrocyte proliferation, inhibiting apoptosis, and activating the PI3K/AKT/CDK2 pathway. Additionally, all‐trans retinoic acid (ATRA), a specific chemical inhibitor of Pin1, effectively suppresses Pin1 expression. However, its clinical application is limited by its short half‐life and susceptibility to inactivation. To address these issues, we have developed a thermosensitive sodium beta‐glycerophosphate (β‐GP)/chitosan (CS) hydrogel loaded with ATRA (β‐GP/CS@ATRA). This hydrogel exhibits favorable morphology and biocompatibility. Compared to free ATRA, the β‐GP/CS@ATRA hydrogel significantly enhances functional motor recovery after SCI and protects spinal cord tissue, thereby inhibiting glial scar formation. Mechanistically, ATRA administration blocks the development of glial scars and the activation of the PI3K/AKT/CDK2 pathway by inhibiting Pin1 expression. This study suggests that combining ATRA with a hydrogel to target Pin1 expression may be a promising strategy for treating glial scar formation following SCI. [ABSTRACT FROM AUTHOR]

Published

2024

7. A dramatic response to an immune checkpoint inhibitor plus chemotherapy in a patient with metastatic metaplastic carcinoma of the breast: A case report.

Author

Koi, Yumiko, Tajiri, Wakako, Kawasaki, Junji, Akiyoshi, Sayuri, Ijichi, Hideki, Nakamura, Yoshiaki, Koga, Chinami, Koga, Yutaka, Taguchi, Kenichi, and Tokunaga, Eriko

Subjects

*THERAPEUTIC use of antineoplastic agents, *BREAST tumor diagnosis, *THERAPEUTIC use of monoclonal antibodies, *PNEUMONIA, *CANCER relapse, *IMMUNOTHERAPY, *BREAST tumors, *PROGRAMMED death-ligand 1, *ANTINEOPLASTIC agents, *CARBOPLATIN, *IMMUNE checkpoint inhibitors, *CANCER chemotherapy, *METASTASIS, *METAPLASIA, *IMMUNOHISTOCHEMISTRY, *ADJUVANT chemotherapy, *LUNG tumors, *GEMCITABINE, *DRUG efficacy, *COMBINED modality therapy, *CHEMICAL inhibitors

Abstract

We present a unique case of metastatic metaplastic breast carcinoma responding dramatically to immunochemotherapy. A 46‐year‐old Japanese woman with primary metaplastic carcinoma of the breast, which was immunohistochemically confirmed to be triple‐negative breast cancer, underwent radical surgery, followed by adjuvant chemotherapy with an anthracycline and a taxane. Since multiple lung metastases were detected two months post‐chemotherapy and the primary site was shown to be PD‐L1‐positive, the immune checkpoint inhibitor (ICI) pembrolizumab plus gemcitabine/carboplatin was initiated. While the treatment was discontinued after 15 days due to suspected drug‐induced pneumonitis, the lung metastases significantly shrank with no development of new lesions for three months. The patient remained alive as of approximately 15 months after the recurrence date. This case highlights the potential of immunochemotherapy in treating metaplastic breast carcinomas. [ABSTRACT FROM AUTHOR]

Published

2024

8. Effect of blockage of Trem1 on the M1 polarization of macrophages in the regulation dental pulp inflammation.

Author

Wang, Ting‐Ting, Jiang, Wen‐Rui, Xu, Li, Zhou, Mei‐Yun, and Huang, Yong‐Song

Subjects

*BIOLOGICAL models, *DENTAL pulp, *MACROPHAGES, *THERAPEUTICS, *RESEARCH funding, *MICE, *PEPTIDES, *ANIMAL experimentation, *GENE expression profiling, *INFLAMMATION, *CHEMICAL inhibitors

Abstract

Dental pulp inflammation is a common and significant factor related to poor dental prognosis. Current treatment strategies primarily concentrate on managing the inflammatory response, with specific targets for intervention still under investigation. Triggering receptors expressed on myeloid cells (TREMs) are a group of receptor molecules extensively present on myeloid cell surfaces, crucial in the regulation of inflammatory process. Our analysis of transcriptomic sequencing data from clinical pulp samples of dataset GSE77459 and animal models revealed up‐regulation of Trem1 during pulpitis. Administration of the Trem1‐blocking peptide LP17 led to lower (more than 1‐fold) levels of several pro‐inflammatory factors and inhibition of M1 macrophage polarization both in vivo and in vitro. This study of the expression patterns and functions of Trem1 in the development of dental pulp inflammation provides novel insights into the therapeutic strategies for clinical pulpitis. [ABSTRACT FROM AUTHOR]

Published

2024

9. Efficacy and Safety of Upadacitinib or Elsubrutinib Alone or in Combination for Patients With Systemic Lupus Erythematosus: A Phase 2 Randomized Controlled Trial.

Author

Merrill, Joan T., Tanaka, Yoshiya, D'Cruz, David, Vila‐Rivera, Karina, Siri, Daniel, Zeng, Xiaofeng, Saxena, Amit, Aringer, Martin, D'Silva, Kristin M., Cheng, Ling, Mohamed, Mohamed‐Eslam F., Siovitz, Lucia, Bhatnagar, Sumit, Gaudreau, Marie‐Claude, Doan, Thao T., and Friedman, Alan

Subjects

*THERAPEUTIC use of monoclonal antibodies, *COMBINATION drug therapy, *PATIENT safety, *DATA analysis, *STATISTICAL sampling, *BLIND experiment, *SYSTEMIC lupus erythematosus, *RANDOMIZED controlled trials, *CHI-squared test, *DESCRIPTIVE statistics, *JANUS kinases, *PROTEIN-tyrosine kinases, *DRUG efficacy, *RESEARCH, *STATISTICS, *NEUROTRANSMITTER uptake inhibitors, *DATA analysis software, *GLUCOCORTICOIDS, *PROPORTIONAL hazards models, *CHEMICAL inhibitors

Abstract

Objective: The 48‐week, phase 2 SLEek study (NCT03978520) evaluated the efficacy and safety of upadacitinib (JAK inhibitor) and elsubrutinib (BTK inhibitor) alone or in combination (ABBV‐599) in adults with moderately to severely active systemic lupus erythematosus (SLE). Methods: Patients were randomized 1:1:1:1:1 to elsubrutinib 60 mg and upadacitinib 30 mg once daily (ABBV‐599 high dose), elsubrutinib 60 mg and upadacitinib 15 mg once daily (ABBV‐599 low dose), elsubrutinib 60 mg once daily (QD), upadacitinib 30 mg QD, or placebo QD. The primary endpoint was the proportion of patients achieving both Systemic Lupus Erythematosus Responder Index 4 (SRI‐4) and glucocorticoid dose ≤10 mg QD at week 24. Additional assessments through week 48 included British Isles Lupus Assessment Group‐Based Composite Lupus Assessment (BICLA) and Lupus Low Disease Activity State (LLDAS) responses, number of flares, time to first flare, and adverse events. Results: The study enrolled 341 patients. The ABBV‐599 low dose and elsubrutinib arms were discontinued after a planned interim analysis showed lack of efficacy (no safety concerns). More patients achieved the primary endpoint with upadacitinib (54.8%; P = 0.028) and ABBV‐599 high dose (48.5%; P = 0.081) versus placebo (37.3%). SRI‐4, BICLA, and LLDAS response rates were higher for both upadacitinib and ABBV‐599 high dose versus placebo at weeks 24 and 48. Flares were reduced, and time to first flare through week 48 was substantially delayed with both upadacitinib and ABBV‐599 high dose versus placebo. No new safety signals were observed beyond those previously reported for upadacitinib or elsubrutinib. Conclusion: Upadacitinib 30 mg alone or in combination with elsubrutinib (ABBV‐599 high dose) demonstrated significant improvements in SLE disease activity and reduced flares and were well tolerated through 48 weeks. [ABSTRACT FROM AUTHOR]

Published

2024

10. Dementia risk reduction between DOACs and VKAs in AF: A systematic review and meta‐analysis.

Author

Chokesuwattanaskul, Anthipa, Prasitlumkum, Narut, Cooley, Ryan, Bunch, T. Jared, Chokesuwattanaskul, Ronpichai, and Navaravong, Leenhapong

Subjects

DEMENTIA risk factors, ANTICOAGULANTS, RISK assessment, MEDICAL information storage & retrieval systems, VITAMIN K, ORAL drug administration, META-analysis, DESCRIPTIVE statistics, AGE distribution, CHI-squared test, SYSTEMATIC reviews, MEDLINE, ATRIAL fibrillation, MEDICAL databases, CONFIDENCE intervals, DEMENTIA patients, CHEMICAL inhibitors

Abstract

Introduction: Direct oral anticoagulants (DOACs) become the recommended treatment over vitamin K antagonists (VKA) in patients with non‐valvular atrial fibrillation (AF). However, their effectiveness in reducing cognitive impairment and dementia compared to VKA remains unclear. Methods: A systematic literature search was conducted on Ovid MEDLINE, EMBASE, and Cochrane Database. Randomized controlled trials, cohort, or case–control study that assessed incident dementia between AF patients who received DOAC compared to VKA were selected. Relevant study characteristics and the number of incident dementia diagnosis or hazard ratios (HRs) for incident dementia and each dementia subtypes were extracted. Random‐effects model was used to perform meta‐analysis. Standardized mean differences (SMDs) were used to estimate effect sizes for continuous data. Results: Twelve cohort studies comprising 1 451 069 individuals were included. The incidence of dementia was lower in AF patients prescribed DOACs compared to VKA (HR 0.88, 95% CI 0.83–0.93, I2 = 61.2%). A lower incident dementia in DOACs group relative to VKA was significantly observed in those less than 75 years of age (< 65 years, HR 0.83 (95% CI 0.72–0.97, I2 = 0%); 65–74 years, HR 0.86 (95% CI 0.81–0.92, I2 = 55.4%); and ≥ 75 years, HR 1.07 (95% CI 0.74–1.55, I2 = 92.5%)) and for the subgroup of patients with vascular dementia (HR 0.91, 95% CI 0.824–0.997, I2 = 0%). Conclusions: This meta‐analysis reveals a reduction in incidence of dementia in AF patients prescribed DOACs compared to VKA, particularly in those less than 75 years old and in the vascular dementia subtype. [ABSTRACT FROM AUTHOR]

Published

2024

11. Investigating the Catalytic Site of Human 15‐Lipoxygenase‐1 via Marine Natural Products.

Author

Spacho, Ntaniela, Casertano, Marcello, Imperatore, Concetta, Papadopoulos, Christos, Menna, Marialuisa, and Eleftheriadis, Nikolaos

Subjects

*MARINE natural products, *STEREOCHEMISTRY, *SMALL molecules, *CHIRALITY, *CATALYSTS, *ENZYME inhibitors, *CHEMICAL inhibitors

Abstract

Human 15‐lipoxygenase‐1 (15‐LOX‐1) is a key enzyme that possesses an important role in (neuro)inflammatory diseases. The pocket of the enzyme plays the role of a chiral catalyst, and therefore chirality could be an important component for the design of effective enzyme inhibitors. To advance our knowledge on this concept, we developed a library of the identified chiral 15‐LOX‐1 inhibitors and applied cheminformatic tools. Our analysis highlighted specific structural elements, which we integrated them in small molecules, and employed them as "smart" tools to effectively navigate the chemical space of previously unexplored regions. To this purpose, we utilized the marine derived natural product phosphoeleganin (PE) among with a small library of synthetic fragment derivatives, including a certain degree of stereochemical diversity. Enzyme inhibition/kinetic and molecular modelling studies has been performed in order to characterize structurally novel PE‐based inhibitors, which proved to present a different type of inhibition with low micromolar potency, according to their structural features. We demonstrate that different warheads work as anchor, and either guide specific stereochemistry, or causing a time‐depended inhibition. Finally, we prove that the positioning of the chiral substituents or/and the favorable stereochemistry can be crucial, as it can lead from active to completely inactive compounds. [ABSTRACT FROM AUTHOR]

Published

2024

12. Selective Covalent Inhibiting JNK3 by Small Molecules for Parkinson's Diseases.

Author

Shuai, Wen, Yang, Panpan, Xiao, Huan, Zhu, Yumeng, Bu, Faqian, Wang, Aoxue, Sun, Qiu, Wang, Guan, and Ouyang, Liang

Subjects

*PARKINSON'S disease, *CHEMICAL inhibitors, *SMALL molecules, *PROTEIN kinases, *DRUG design

Abstract

c‐Jun N‐terminal kinases (JNKs) including JNK1/2/3 are key members of mitogen‐activated protein kinase family. Wherein JNK3 is specifically expressed in brain and emerges as therapeutic target, especially for neurodegenerative diseases. However, developing JNK3 selective inhibitors as chemical probes to investigate its therapeutic potential in diseases remains challenging. Here, we adopted the covalent strategy for identifying JNK3‐selective covalent inhibitor JC16I, with high inhibitory activity against JNK3. Despite targeting a conserved cysteine in the vicinity of ATP pocket in JNK family, JC16I exerted a greater than 160‐fold selectivity for JNK3 over JNK1/2. Importantly, even at low concentration, JC16I showed enhanced and long‐lasting inhibition against cellular JNK3. In addition, its alkyne‐containing probe JC‐P1 could label JNK3 in SH‐SY5Y cell lysate and living cells, with good proteome‐wide selectivity. JC16I selectively suppressed the abnormal activation of JNK3 signaling and sufficiently exhibited neuroprotective effect in Parkinson's diseases (PD) models. Overall, our findings highlight the potential of developing isoform‐selective and cell‐active JNK3 inhibitors by covalent drug design strategy targeting a conserved cysteine. This work not only provides a valuable chemical probe for JNK3‐targeted investigations in vitro and in vivo but also opens new avenues for the treatment of PD. [ABSTRACT FROM AUTHOR]

Published

2024

13. Predictive model of IVF outcomes for polycystic ovarian morphology and polycystic ovary syndrome in GnRH antagonist protocol using AMH‐MoM and ovarian sensitivity index.

Author

Ko, Yoo Ra, Yu, Eun Jeong, Park, Jae Eun, Park, Jae Kyun, Eum, Jin Hee, Kim, Tae Hyung, Lee, Woo Sik, and Lee, Hee Jun

Subjects

*POLYCYSTIC ovary syndrome treatment, *OVARIAN hyperstimulation syndrome, *SEX hormones, *OVUM, *PREDICTION models, *RESEARCH funding, *BODY mass index, *TREATMENT effectiveness, *RETROSPECTIVE studies, *DESCRIPTIVE statistics, *FERTILIZATION in vitro, *GONADOTROPIN releasing hormone, *OVARIAN reserve, *COMPARATIVE studies, *CONFIDENCE intervals, *ABORTION, *CHEMICAL inhibitors

Abstract

Aim: To evaluate the relationship between AMH and ovarian response to controlled ovarian hyperstimulation in women with PCOM and PCOS. Methods: A retrospective study was conducted on 559 patients who underwent the IVF‐ET cycle between January 2018 and December 2022 at Gangnam Cha Hospital. Patients were divided into 3 groups matched for age and BMI: the PCOS group (n = 54), based on the new 2023 PCOS guideline; the PCOM group (n = 53); and the control group (n = 452) with normal ovaries. Serum AMH levels were converted to multiples of the median (MoM) for each corresponding age. The ovarian sensitivity index (OSI) was calculated as the number of retrieved oocytes divided by the total dose of recombinant FSH administered (per 1000 IU). Results: There were significant differences in AMH‐MoM value among women with PCOS [2.7 ± 1.3 (95% CI 2.3–3.0)], those with PCOM [2.0 ± 1.0 (95% CI 1.7–2.3)], and controls [0.8 ± 0.7 (95% CI 0.8–0.9)] (p < 0.001). The abortion rates in the normoovulatory, PCOM, and PCOS groups were 18.2%, 21.1%, and 25.0%, respectively. OSI and live birth rate were positively correlated with the AMH‐MoM value in normoovulatory women (r = 0.389, p < 0.05, r = 0.122, p < 0.05), while no such correlation was observed in women with PCOM and PCOS. Conclusions: Ovarian response and live birth rate are possibly correlated with the AMH‐MoM value in normoovulatory women, but not in women with PCOM and PCOS. [ABSTRACT FROM AUTHOR]

Published

2024

14. Guiding Dyslipidemia Treatment: A Population Pharmacokinetic–Pharmacodynamic Framework for Obicetrapib.

Author

Dunn, Allison, Ditmarsch, Marc, Kastelein, John J. P., Kling, Douglas, Neild, Annie, Davidson, Michael H., and Gobburu, Joga

Subjects

*DRUG therapy for hyperlipidemia, *HIGH density lipoproteins, *ANTILIPEMIC agents, *CARDIOVASCULAR diseases, *RESEARCH funding, *STRUCTURAL models, *BODY weight, *GLYCOPROTEINS, *DESCRIPTIVE statistics, *DECISION making, *BIOTRANSFORMATION (Metabolism), *LOW density lipoproteins, *DRUG development, *ALLOMETRY, *PHARMACODYNAMICS, *CHEMICAL inhibitors, RESEARCH evaluation

Abstract

Obicetrapib is a selective inhibitor of cholesteryl ester transfer protein that is currently in phase 3 of development for the treatment of dyslipidemia as adjunct therapy. The purpose of this study was to comprehensively characterize the pharmacokinetic (PK) and pharmacodynamic (PD) disposition of obicetrapib. Data from 7 clinical trials conducted in healthy adults and those with varying degrees of dyslipidemia were included for model development. The structural model that best described obicetrapib PK was a 3‐compartment model with 4‐compartment transit absorption and first‐order elimination. Body weight was the only covariate found to significantly explain observed variability and was therefore included using allometric scaling on all disposition parameters. For a typical patient weighing 75 kg, the estimated apparent total body clearance and apparent volume of distribution of the central compartment was 0.81 L/h and 36.1 L, respectively. The final PK model parameters were estimated with good precision and were ultimately leveraged to sequentially inform 2 turnover models that describe obicetrapib's effect on low‐density lipoprotein cholesterol (LDL‐C) and high‐density lipoprotein cholesterol (HDL‐C) concentrations. The maximum stimulatory effect of obicetrapib on LDL‐C loss was estimated to be 1.046, while the maximum inhibitory effect of obicetrapib on HDL‐C loss was 0.691. This corresponds to a predicted typical maximum percent change from baseline LDL‐C and HDL‐C of 51.1% and 224%, respectively. The final sequential model described obicetrapib PKPD well and was ultimately able to both demonstrate evidence of internal consistency and support decision‐making throughout the development lifecycle. [ABSTRACT FROM AUTHOR]

Published

2024

15. Quantitative Assessment of Drug Efficacy and Emergence of Resistance in Patients with Metastatic Renal Cell Carcinoma Using a Longitudinal Exposure‐Tumor Growth Inhibition Model: Apitolisib (Dual PI3K/mTORC1/2 Inhibitor) Versus Everolimus (mTORC1 Inhibitor)

Author

Moein, Anita, Jin, Jin Y., Wright, Matthew R., and Wong, Harvey

Subjects

*THERAPEUTIC use of antineoplastic agents, *DRUG resistance in cancer cells, *RESEARCH funding, *CANCER relapse, *ENZYME inhibitors, *ANTINEOPLASTIC agents, *CELL physiology, *CELL proliferation, *CELLULAR signal transduction, *CANCER patients, *DESCRIPTIVE statistics, *METASTASIS, *CELL lines, *MATHEMATICAL models, *DRUG efficacy, *RENAL cell carcinoma, *THEORY, *EVEROLIMUS, *PHOSPHOTRANSFERASES, *COMPARATIVE studies, *SIGNAL peptides, *EVALUATION, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Cancer remains a significant global health challenge, and despite remarkable advancements in therapeutic strategies, poor tolerability of drugs (causing dose reduction/interruptions) and/or the emergence of drug resistance are major obstacles to successful treatment outcomes. Metastatic renal cell carcinoma (mRCC) accounts for 2% of global cancer diagnoses and deaths. Despite the initial success of targeted therapies in mRCC, challenges remain to overcome drug resistance that limits the long‐term efficacy of these treatments. Our analysis aim was to develop a semi‐mechanistic longitudinal exposure‐tumor growth inhibition model for patients with mRCC to characterize and compare everolimus (mTORC1) and apitolisib's (dual PI3K/mTORC1/2) ability to inhibit tumor growth, and quantitate each drug's efficacy decay caused by emergence of tumor resistance over time. Model‐estimated on‐treatment tumor growth rate constant was 1.7‐fold higher for apitolisib compared to everolimus. Estimated half‐life for loss of treatment effect over time for everolimus was 16.1 weeks compared to 7.72 weeks for apitolisib, suggesting a faster rate of tumor re‐growth for apitolisib patients likely due to the emergence of resistance. Goodness‐of‐fit plots including visual predictive check indicated a good model fit and the model was able to capture individual tumor size–time profiles. Based on our knowledge, this is the first clinical report to quantitatively assess everolimus (mTORC1) and apitolisib (PI3K/mTORC1/2) efficacy decay in patients with mRCC. These results highlight the difference in overall efficacy of 2 drugs due to the quantified efficacy decay caused by emergence of resistance, and emphasize the importance of model‐informed drug development for targeted cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

16. TNNT1 accelerates migration, invasion and EMT progression in lung cancer cells.

Author

Ge, Xiaobin, Du, Guangzhong, Zhou, Qingchen, Yan, Bing, and Yue, Gonglei

Subjects

*TROPONIN, *EPITHELIAL cells, *EPITHELIAL-mesenchymal transition, *CANCER invasiveness, *QUALITATIVE research, *LITHIUM compounds, *CELL motility, *REVERSE transcriptase polymerase chain reaction, *CELLULAR signal transduction, *CELL lines, *METASTASIS, *GENE expression, *LUNG tumors, *GENE expression profiling, *WESTERN immunoblotting, *LUNG cancer, *BIOMARKERS, *SEQUENCE analysis, *WNT proteins, *CHEMICAL inhibitors

Abstract

Background: Clinically, most patients with lung cancer (LC) die from tumor spread and metastasis. Specific metastasis‐related molecules can provide reference for clinical prediction of efficacy, evaluation of prognosis, and search for the best treatment plan. Troponin T1 (TNNT1) is highly expressed in various cancer tissues, which affects malignant behavior of tumor cells and is related to patients' survival and prognosis. However, the role and molecular mechanism of TNNT1 in LC invasion and metastasis have not yet been investigated. Methods: Gene expression profiling interactive analysis (GEPIA) online analysis was used to analyze TNNT1 expression in LC tissues. Quantitative real‐time‐polymerase chain reaction (qRT‐PCR) or western blot were performed to measure TNNT1 or epithelial‐to‐mesenchymal transition (EMT)‐related and Wnt/β‐catenin pathway‐related protein expression in LC cells. After TNNT1 knockdown, cell scratch healing and transwell assays were introduced to assess cell migration and invasion, respectively. Results: TNNT1 expression in LC tissues and cells was increased. TNNT1 knockdown notably impaired LC cell migration, invasion and EMT. TNNT1 knockdown inhibited Wnt/β‐catenin pathway of LC cells. Lithium chloride (LiCl) addition partially restored the inhibition of TNNT1 knockdown on migration, invasion, EMT and Wnt/β‐catenin of LC cells. Conclusion: TNNT1 knockdown attenuated LC migration, invasion and EMT, possibly through Wnt/β‐catenin signaling. [ABSTRACT FROM AUTHOR]

Published

2024

17. Impact of gender in patients with device‐related thrombosis after left atrial appendage closure – A sub‐analysis from the multicenter EUROC‐DRT‐registry.

Author

Saw, Jacqueline, Vij, Vivian, Galea, Roberto, Piayda, Kerstin, Nelles, Dominik, Vogt, Lara, Gloekler, Steffen, Fürholz, Monika, Meier, Bernhard, Räber, Lorenz, O'Hara, Gilles, Arzamendi, Dabit, Agudelo, Victor, Asmarats, Lluis, Freixa, Xavier, Flores‐Umanzor, Eduardo, De Backer, Ole, Sondergaard, Lars, Nombela‐Franco, Luis, and Salinas, Pablo

Subjects

*THROMBOSIS risk factors, *RISK assessment, *PROSTHETICS, *ANTICOAGULANTS, *SEX distribution, *ARTIFICIAL implants, *DESCRIPTIVE statistics, *REPORTING of diseases, *VITAMIN K, *SURGICAL complications, *KAPLAN-Meier estimator, *ATRIAL fibrillation, *LEFT atrial appendage closure, *ADVERSE health care events, *CONFIDENCE intervals, *STROKE, *COMORBIDITY, *CHEMICAL inhibitors

Abstract

Background: Device‐related thrombosis (DRT) is a common finding after left atrial appendage closure (LAAC) and is associated with worse outcomes. As women are underrepresented in clinical studies, further understanding of sex differences in DRT patients is warranted. Methods and Results: This sub‐analysis from the EUROC‐DRT‐registry compromises 176 patients with diagnosis of DRT after LAAC. Women, who accounted for 34.7% (61/176) of patients, were older (78.0 ± 6.7 vs. 74.9 ± 9.1 years, p =.06) with lower rates of comorbidities. While DRT was detected significantly later in women (173 ± 267 vs. 127 ± 192 days, p =.01), anticoagulation therapy was escalated similarly, mainly with initiation of novel oral anticoagulant (NOAC), vitamin K antagonist (VKA) or heparin. DRT resolution was achieved in 67.5% (27/40) of women and in 75.0% (54/72) of men (p =.40). In the remaining cases, an intensification/switch of anticoagulation was conducted in 50.% (9/18) of men and in 41.7% (5/12) of women. Final resolution was achieved in 72.5% (29/40) cases in women, and in 81.9% (59/72) cases in men (p =.24). Women were followed‐up for a similar time as men (779 ± 520 vs. 908 ± 687 days, p =.51). Kaplan–Meier analysis revealed no difference in mortality rates in women (Hazard Ratio [HR]: 1.73, 95%‐Confidence interval [95%‐CI]:.68–4.37, p =.25) and no differences in stroke (HR:.83, 95%‐CI:.30–2.32, p =.72) within 2 years after LAAC. Conclusion: Evaluation of risk factors and outcome revealed no differences between men and women, with DRT in women being diagnosed significantly later. Women should be monitored closely to assess for DRT formation/resolution. Treatment strategies appear to be equally effective. [ABSTRACT FROM AUTHOR]

Published

2024

18. Effect of Secukinumab Versus Adalimumab Biosimilar on Radiographic Progression in Patients With Radiographic Axial Spondyloarthritis: Results From a Head‐to‐Head Randomized Phase IIIb Study.

Author

Baraliakos, Xenofon, Østergaard, Mikkel, Poddubnyy, Denis, van der Heijde, Désirée, Deodhar, Atul, Machado, Pedro M., Navarro‐Compán, Victoria, Hermann, Kay Geert A., Kishimoto, Mitsumasa, Lee, Eun Young, Gensler, Lianne S., Kiltz, Uta, Eigenmann, Marco F., Pertel, Patricia, Readie, Aimee, Richards, Hanno B., Porter, Brian, and Braun, Juergen

Subjects

*COMBINATION drug therapy, *ANTI-inflammatory agents, *RESEARCH funding, *PATIENT safety, *ANKYLOSIS, *EDEMA, *LOGISTIC regression analysis, *QUESTIONNAIRES, *DESCRIPTIVE statistics, *MAGNETIC resonance imaging, *ANALYSIS of covariance, *CHI-squared test, *MONOCLONAL antibodies, *ADALIMUMAB, *DRUG efficacy, *INTRACLASS correlation, *BIOSIMILARS, *SPONDYLOARTHROPATHIES, *HEALTH outcome assessment, *CONFIDENCE intervals, *DATA analysis software, *DISEASE progression, *INTERLEUKINS, *C-reactive protein, *DRUG tolerance, *SUBCUTANEOUS injections, *DRUG dosage, *DRUG administration, *CHEMICAL inhibitors

Abstract

Objective: Spinal radiographic progression is an important outcome in radiographic axial spondyloarthritis (SpA). The objective of the phase IIIb SURPASS study was to compare spinal radiographic progression in patients with radiographic axial SpA treated with secukinumab (interleukin‐17A inhibitor) versus adalimumab biosimilar (Sandoz adalimumab [SDZ‐ADL]; tumor necrosis factor inhibitor). Methods: Biologic‐naive patients with active radiographic axial SpA, at high risk of radiographic progression (high‐sensitivity C‐reactive protein [hsCRP] ≥5 mg/L and/or ≥1 syndesmophyte[s] on spinal radiographs), were randomized (1:1:1) to secukinumab (150/300 mg) or SDZ‐ADL (40 mg). The proportion of patients with no radiographic progression (change from baseline [CFB] in modified Stoke Ankylosing Spondylitis Spinal Score [mSASSS] ≤0.5) on secukinumab versus SDZ‐ADL at week 104 (primary endpoint), mean CFB‐mSASSS, proportion of patients with ≥1 syndesmophyte(s) at baseline with no new syndesmophyte(s), and safety were evaluated. Results: Overall, 859 patients (78.5% male, mSASSS 16.6, Bath Ankylosing Spondylitis Disease Activity Index 7.1, hsCRP 20.4 mg/L, and 73.0% with ≥1 syndesmophyte[s]) received secukinumab 150 mg (n = 287), secukinumab 300 mg (n = 286), or SDZ‐ADL (n = 286). At week 104, the proportion of patients with no radiographic progression was 66.1%, 66.9%, and 65.6% (P = not significant, both secukinumab doses) and mean CFB‐mSASSS was 0.54, 0.55, and 0.72 in secukinumab 150 mg, secukinumab 300 mg, and SDZ‐ADL arms, respectively. Overall, 56.9%, 53.8%, and 53.3% of patients on secukinumab 150 mg, secukinumab 300 mg, and SDZ‐ADL, respectively, with ≥1 syndesmophyte(s) at baseline did not develop new syndesmophyte(s) by week 104. There were no unexpected safety findings. Conclusion: Spinal radiographic progression over two years was low with no significant difference between secukinumab and SDZ‐ADL arms. The safety of both treatments was consistent with previous reports. [ABSTRACT FROM AUTHOR]

Published

2024

19. Characterizing the Nonlinear Pharmacokinetics and Pharmacodynamics of BI 187004, an 11β‐Hydroxysteroid Dehydrogenase Type 1 Inhibitor, in Humans by a Target‐Mediated Drug Disposition Model.

Author

Yuan, Xuanzhen and An, Guohua

Subjects

*PROTEIN kinase inhibitors, *BIOLOGICAL models, *CHAOS theory, *STRUCTURAL models, *ENZYME inhibitors, *SAMPLE size (Statistics), *DESCRIPTIVE statistics, *SMALL molecules, *OXIDOREDUCTASES, *RESEARCH, *BLOOD plasma, *LIVER, *DRUG development, *DATA analysis software, *COMPARATIVE studies, *CONFIDENCE intervals, *ABSORPTION, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

BI 187004, a selective small‐molecule inhibitor of 11β‐hydroxysteroid dehydrogenase‐1 (11β‐HSD1), displayed complex nonlinear pharmacokinetics (PK) in humans. Following nine single oral doses, BI 187004 exhibited nonlinear PK at low doses and linear PK at higher doses. Notably, substantial hepatic 11β‐HSD1 inhibition (50%) was detected in a very low‐dose group, achieving a consistent 70% hepatic enzyme inhibition in subsequent ascending doses without any dose‐dependent effects. The unusual PK and PD profiles of BI 187004 suggest the presence of pharmacological target‐mediated drug disposition (TMDD), arising from the saturable binding of BI 187004 compound to its high‐affinity and low‐capacity target 11β‐HSD1. The non‐intuitive dose, exposure, and response relationship for BI 187004 pose a significant challenge in rational dose selection. This study aimed to construct a TMDD model to explain the complex nonlinear PK behavior and underscore the importance of recognizing TMDD in this small‐molecule compound. Among the various models explored, the best model was a two‐compartment TMDD model with three transit absorption components. The final model provides insights into 11β‐HSD1 binding‐related parameters for BI 187004, including the total amount of 11β‐HSD1 in the liver (estimated to be 8000 nmol), the second order association rate constant (estimated to be 0.102 nM−1h−1), and the first‐order dissociation rate constant (estimated to be 0.11 h−1). Our final population PK model successfully characterized the intricate nonlinear PK of BI 187004 across a wide dose range. This modeling work serves as a valuable reference for the rational selection of the dose regimens for BI 187004's future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2024

20. The importance of stratum corneum ω‐linoleoyloxyacylceramides in human skin barrier health: their biochemistry, processing enzymes and metabolites involved in corneocyte lipid envelope maturation.

Author

Rawlings, Anthony V., Lane, Majella E., and Voegeli, Rainer

Subjects

*STAINS & staining (Microscopy), *CHEMICAL inhibitors, *METABOLITES, *CERAMIDES, *STRUCTURAL models

Abstract

Over the past 50 years there have been great strides made in the discovery of the composition and relevance of the total stratum corneum (SC) ceramide matrix. However, the focus of this review is on the free intercellular class of ω‐linoleoyloxyacylceramides, corneocyte‐bound ceramides and associated lipids known as the corneocyte lipid envelope (CLE) together with their processing enzymes involved in aiding ceramide attachment the corneocyte protein envelope (CPE). Two structural models and partially shared biosynthetic pathways have been proposed for the attachment of CPE‐bound O‐ceramides (ω‐hydroxyceramides attached to glutamate residues of proteins in the (CPE) using the 12R‐lipoxygenase (12R‐LOX)/epidermal lipoxygenase‐3 (eLOX3)/epoxide hydrolase‐3 (EPHX3)/unknown esterase/ transglutaminase‐1 (TG1) attachment pathway) and CPE‐bound EO‐ceramides (epoxy‐enone ceramides attached to cysteine residues of proteins in the CPE using the 12R‐LOX/eLOX3/short chain dehydrogenase/reductase family 9C member 7 (SDR9C7)/non‐enzymatic attachment pathway), i.e. there is a bifurcation step beyond epidermal eLOX3. Their formation and structures will be discussed as well as their relevance in compromised skin barrier conditions together with our own work on SC maturation examined by proteomics, lipidomics, enzyme immunolocalization studies, mechanical fragility assays and Nile red staining of corneocyte envelopes (CE). Reduced levels of 12R‐LOX, eLOX3, SDR9C7 and TG1 were observed in photodamaged skin of the cheeks that were associated with reduced SC maturation as evidenced by Nile red staining and increased CE fragility. In the severely photodamaged cheeks of Albino African SC we also observed increased levels of acylceramides. Concomitantly by reducing the activity of 12R‐LOX by antibody inhibition and TG1 inhibition with a known chemical inhibitor, we demonstrated in a humidity‐based ex vivo SC maturation model that these enzymes contributed to increased CE hydrophobicity and mechanical integrity. We hypothesize that at least the CPE‐bound O‐ceramide pathway is operational in the SC. Nevertheless, our understanding of the full complexity of ω‐linoleoyloxyacylceramides and the composition of the CLE is limited particularly on cosmetically relevant body sites such as the face. [ABSTRACT FROM AUTHOR]

Published

2024

21. Outcome of tailored therapy in rheumatic heart disease with persistent atrial fibrillation (RHD‐AF).

Author

Saggu, Daljeet Kaur, Subramaniam, Muthiah, Korabathina, Radhika, Raju, B. Soma, Atreya, Auras R., Reddy, Prasad, Kumar, D. N., Menon, Rajeev, Yalagudri, Sachin, Kapadiya, Anuj, Chennapragada, Sridevi, and Narasimhan, Calambur

Subjects

*DISEASE risk factors, *ATRIAL fibrillation treatment, *RISK assessment, *ELECTRIC countershock, *ANTICOAGULANTS, *TRANSESOPHAGEAL echocardiography, *T-test (Statistics), *LEFT heart atrium, *VENTRICULAR ejection fraction, *HOSPITAL care, *FISHER exact test, *PULMONARY artery, *TREATMENT effectiveness, *PEPTIDE hormones, *HEART failure, *HEART valve diseases, *VITAMIN K, *MANN Whitney U Test, *CHI-squared test, *ORAL drug administration, *CALCIUM antagonists, *DESCRIPTIVE statistics, *HEART conduction system, *LONGITUDINAL method, *THROMBOEMBOLISM, *CATHETER ablation, *DISEASE relapse, *CARDIAC pacing, *COMPARATIVE studies, *DATA analysis software, *SYSTOLIC blood pressure, *RHEUMATIC heart disease, *MYOCARDIAL depressants, *LEFT ventricular dysfunction, *DISEASE complications, *CHEMICAL inhibitors

Abstract

Introduction: Rheumatic heart disease with persistent atrial fibrillation (RHD‐AF) is associated with increased morbidity. However, there is no standardized approach for the maintenance of sinus rhythm (SR) in them. We aimed to determine the utility of a stepwise approach to achieve SR in RHD‐AF. Methods: Consecutive patients with RHD‐AF from July 2021 to August 2023 formed the study cohort. The stepwise approach included pharmacological rhythm control and/or electrical cardioversion (Central illustration). In patients with recurrence, additional options included AF ablation or pace and ablate strategy with conduction system pacing or biventricular pacing. Clinical improvement, NT‐proBNP, 6‐Minute Walk Test (6MWT), heart failure (HF) hospitalizations, and thromboembolic complications were documented during follow‐up. Results: Eighty‐three patients with RHD‐AF (mean age 56.13 ± 9.51 years, women 72.28%) were included. Utilizing this approach, 43 (51.81%) achieved and maintained SR during the study period of 11.04 ± 7.14 months. These patients had improved functional class, lower NT‐proBNP, better distance covered for 6MWT, and reduced HF hospitalizations. The duration of AF was shorter in patients who achieved SR, compared to those who remained in AF (3.15 ± 1.29 vs 6.93 ± 5.23, p = 0.041). Thirty‐five percent (29) maintained SR after a single cardioversion over the study period. Only one underwent AF ablation. Of the 24 who underwent pace and ablate strategy, atrial lead was implanted in 22 (hybrid approach), and 50% of these achieved and maintained SR. Among these 24, none had HF hospitalizations, but patients who maintained SR had further improvement in clinical and functional parameters. Conclusions: RHD‐AF patients who could achieve SR with a stepwise approach, had better clinical outcomes and lower HF hospitalizations. [ABSTRACT FROM AUTHOR]

Published

2024

22. An extremely wide QRS complex tachycardia induced by anamorelin.

Author

Shimojo, Kazuki, Kanzaki, Yasunori, Miyazawa, Hiroyuki, and Morishima, Itsuro

Subjects

LOSS of consciousness, FATIGUE (Physiology), DIZZINESS, SUPRAVENTRICULAR tachycardia, APPETITE, DISCHARGE planning, ELECTROCARDIOGRAPHY, VENTRICULAR tachycardia, RECTUM tumors, METASTASIS, GHRELIN, TACHYCARDIA, CACHEXIA, LIVER, MYOCARDIAL depressants, CHEMICAL inhibitors, DISEASE complications

Published

2024

23. BBR affects macrophage polarization via inhibition of NF‐κB pathway to protect against T2DM‐associated periodontitis.

Author

Xia, Siying, Jing, Rui, Shi, Mingyan, Yang, Yanan, Feng, Meiting, Deng, Li, and Luo, Lijun

Subjects

INFLAMMATION prevention, NF-kappa B, BONE resorption, MACROPHAGES, ALKALOIDS, RESEARCH funding, INFLAMMATORY mediators, POLYMERASE chain reaction, COMPUTED tomography, GINGIVA, CELLULAR signal transduction, MICE, MESSENGER RNA, GENE expression, EXPERIMENTAL design, TYPE 2 diabetes, ANIMAL experimentation, WESTERN immunoblotting, CYTOKINES, PERIODONTITIS, CHEMICAL inhibitors, DISEASE complications

Abstract

Background and Objective: Periodontitis is intimately associated with the development of various systemic diseases, among which type 2 diabetes mellitus (T2DM) has a bidirectional relationship with the pathogenesis of periodontitis. The objective of the present work was to investigate the role of berberine (BBR) in periodontitis with T2DM and related mechanisms. Methods: The mRNA expression of macrophage polarization‐related factors in the microenvironment of periodontal inflammation was detected using real‐time quantitative PCR (RT‐qPCR). The experimental periodontitis model was constructed in wild‐type (WT) and T2DM (db/db) mice, which were administered BBR after 7 days of modeling. Alveolar bone loss (ABL) in each group of mice was measured utilizing micro‐computed tomography images. RT‐qPCR was performed to analyze the levels of macrophage polarization‐related factors in mouse gingiva. Lastly, using western blotting and RT‐qPCR, the signaling pathway of BBR affecting macrophage polarization in the microenvironment of periodontitis was explored. Results: BBR inhibited M1 polarization and stimulated M2 polarization in the periodontitis microenvironment. BBR decreased ABL in the WT and T2DM periodontitis models. And BBR reduced the production of proinflammatory cytokines and increased anti‐inflammatory cytokine expression in the gingiva of WT and T2DM model mice. Ultimately, BBR mediates its anti‐inflammatory effects on periodontitis through inhibition of the NF‐κB pathway. Conclusions: BBR had a therapeutic effect on T2DM‐associated periodontitis via inhibiting the NF‐κB pathway to affect macrophage polarization, which may have implications for the new pharmacological treatment of T2DM‐associated periodontitis. [ABSTRACT FROM AUTHOR]

Published

2024

24. De‐nitrosylation Coordinates Appressorium Function for Infection of the Rice Blast Fungus.

Author

Hu, Hong, He, Wenhui, Qu, Zhiguang, Dong, Xiang, Ren, Zhiyong, Qin, Mengyuan, Liu, Hao, Zheng, Lu, Huang, Junbin, and Chen, Xiao‐Lin

Subjects

*RICE blast disease, *PYRICULARIA oryzae, *CHEMICAL inhibitors, *PROTEIN structure, *MYCOSES

Abstract

As a signaling molecule, nitric oxide (NO) regulates the development and stress response in different organisms. The major biological activity of NO is protein S‐nitrosylation, whose function in fungi remains largely unclear. Here, it is found in the rice blast fungus Magnaporthe oryzae, de‐nitrosylation process is essential for functional appressorium formation during infection. Nitrosative stress caused by excessive accumulation of NO is harmful for fungal infection. While the S‐nitrosoglutathione reductase GSNOR‐mediated de‐nitrosylation removes excess NO toxicity during appressorium formation to promote infection. Through an indoTMT switch labeling proteomics technique, 741 S‐nitrosylation sites in 483 proteins are identified. Key appressorial proteins, such as Mgb1, MagB, Sps1, Cdc42, and septins, are activated by GSNOR through de‐nitrosylation. Removing S‐nitrosylation sites of above proteins is essential for proper protein structure and appressorial function. Therefore, GSNOR‐mediated de‐nitrosylation is an essential regulator for appressorium formation. It is also shown that breaking NO homeostasis by NO donors, NO scavengers, as well as chemical inhibitor of GSNOR, shall be effective methods for fungal disease control. [ABSTRACT FROM AUTHOR]

Published

2024

25. Integrating Full Bayesian Inference and Student's t‐Distribution Method for Enhanced Outlier Handling in Caffeine Population Pharmacokinetics: Assessing Drug–Drug Interactions with Enasidenib in Relapsed or Refractory AML and MDS Patients.

Author

Cheng, Yiming, Du, Shengnan, Hu, Hongxiang, Wang, Xiaomin, Carayannopoulos, Leon, and Li, Yan

Subjects

*CAFFEINE, *MYELODYSPLASTIC syndromes, *MEMBRANE transport proteins, *CANCER relapse, *RESEARCH funding, *ENZYME inhibitors, *ANTINEOPLASTIC agents, *PROBABILITY theory, *UNCERTAINTY, *OXIDOREDUCTASES, *DRUG interactions, *CYTOCHROME P-450, *GENETIC mutation, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

As the first‐in‐class, selective, and potent inhibitor of the isocitrate dehydrogenase‐2 (IDH2) mutant protein, enasidenib was approved by the US Food and Drug Administration (FDA) in 2017 for the treatment of adult patients with relapsed or refractory acute myeloid leukemia (AML) with an IDH2 mutation. Known for its interactions with various cytochrome P450 (CYP) enzymes and transporters in vitro, a clinical pharmacokinetics (PK) trial was initiated to assess the impact of multiple doses of enasidenib on the single‐dose PK of sensitive probe substrates of several cytochrome P450 enzymes and transporters. In this study, a population pharmacokinetic analysis approach was employed to address challenges posed by high, nonzero baseline caffeine concentrations. Moreover, we integrated full Bayesian inference into this approach innovatively for a more detailed understanding of parameter uncertainty and greater modeling flexibility, alongside Student's t‐distribution for robust error modeling in handling the abnormal outlier caffeine concentration data observed in this trial. Our analyses demonstrated that multiple doses of enasidenib altered caffeine clearance to a clinically meaningful extent, as evidenced by an approximate 8‐fold decrease. This finding led to a specific recommendation in the package insert to avoid the concurrent use of certain CYP1A2 substrates with enasidenib, unless directed otherwise in the prescribing information. Furthermore, this research underlines the technical benefits of integrating full Bayesian inference and incorporating Student's t‐distribution for residual error modeling in the PK field. [ABSTRACT FROM AUTHOR]

Published

2024

26. A Real‐World Pharmacovigilance Study of Ceftazidime/Avibactam: Data Mining of the Food and Drug Administration Adverse Event Reporting System Database.

Author

Yao, Haiping, Wang, Yanyan, Peng, Yan, Huang, Zhixiong, Gan, Guoping, and Wang, Zhu

Subjects

*COMMUNICABLE diseases, *COMBINATION drug therapy, *PHARMACOLOGY, *DRUG toxicity, *RISK assessment, *DATABASES, *POISSON distribution, *DRUG side effects, *DATA mining, *GASTROINTESTINAL hemorrhage, *PURPURA (Pathology), *RETROSPECTIVE studies, *ODDS ratio, *ARTIFICIAL neural networks, *DELIRIUM, *CEFTAZIDIME, *BETA lactamases, *HEMORRHAGIC shock, *ALGORITHMS, *TIME, *RECTUM, *HYPERNATREMIA, *CONSCIOUSNESS disorders, *CEREBRAL edema, *CHEMICAL inhibitors

Abstract

Ceftazidime/avibactam (CAZ/AVI) is a combination of a well‐known third‐generation, broad‐spectrum cephalosporin with a new beta‐lactamase inhibitor that has been approved for the treatment of various infectious diseases (especially multidrug‐resistant Gram‐negative bacterial infections) by the Food and Drug Administration (FDA). The current study extensively assessed CAZ/AVI‐related adverse events (AEs) in the real world through data mining of the FDA Adverse Event Reporting System (FAERS) database to better understand toxicities. The signals of CAZ/AVI‐related AEs were quantified using disproportionality analyses, including the reporting odds ratio, the proportional reporting ratio, the Bayesian confidence propagation neural network, and the multi‐item gamma Poisson shrinker algorithms. Out of 10,114,815 records retrieved from the FAERS database, 628 cases were identified, where CAZ/AVI was implicated as the primary suspect drug. A total of 61 preferred terms with significant disproportionality that simultaneously met the criteria of all four algorithms were retained. Several unexpected safety signals may also occur, including melena, hypernatremia, depressed level of consciousness, brain edema, petechiae, delirium, and shock hemorrhagic. The median onset time for AEs associated with CAZ/AVI was 4 days, with most cases occurring within 3 days after CAZ/AVI initiation. [ABSTRACT FROM AUTHOR]

Published

2024

27. Evaluating the efficacy of the selective orexin 1 receptor antagonist nivasorexant in an animal model of binge‐eating disorder.

Author

Steiner, Michel Alexander, Botticelli, Luca, Bergamini, Giorgio, Micioni Di Bonaventura, Emanuela, Gatfield, John, Williams, Jodi T., Treiber, Alexander, Vaillant, Catherine, Cifani, Carlo, and Micioni Di Bonaventura, Maria Vittoria

Subjects

*BIOLOGICAL models, *RESEARCH funding, *BINGE-eating disorder, *NEURONS, *FLUORESCENT antibody technique, *CYTOCHEMISTRY, *DIETARY fats, *RATS, *GENE expression, *NEUROPEPTIDES, *DRUG efficacy, *ANIMAL experimentation, *PHENOTYPES, *EVALUATION, *CHEMICAL inhibitors

Abstract

Objective: Test the efficacy of the selective orexin 1 receptor (OX1R) antagonist (SO1RA) nivasorexant in an animal model of binge‐eating disorder (BED) and study its dose–response relationship considering free brain concentrations and calculated OX1R occupancy. Compare nivasorexant's profile to that of other, structurally diverse SO1RAs. Gain understanding of potential changes in orexin‐A (OXA) neuropeptide and deltaFosB (ΔFosB) protein expression possibly underlying the development of the binge‐eating phenotype in the rat model used. Method: Binge‐like eating of highly palatable food (HPF) in rats was induced through priming by intermittent, repeated periods of dieting and access to HPF, followed by an additional challenge with acute stress. Effects of nivasorexant were compared to the SO1RAs ACT‐335827 and IDOR‐1104‐2408. OXA expression in neurons and neuronal fibers as well as ΔFosB and OXA‐ΔFosB co‐expression was studied in relevant brain regions using immuno‐ or immunofluorescent histochemistry. Results: All SO1RAs dose‐dependently reduced binge‐like eating with effect sizes comparable to the positive control topiramate, at unbound drug concentrations selectively blocking brain OX1Rs. Nivasorexant's efficacy was maintained upon chronic dosing and under conditions involving more frequent stress exposure. Priming for binge‐like eating or nivasorexant treatment resulted in only minor changes in OXA or ΔFosB expression in few brain areas. Discussion: Selective OX1R blockade reduced binge‐like eating in rats. Neither ΔFosB nor OXA expression proved to be a useful classifier for their binge‐eating phenotype. The current results formed the basis for a clinical phase II trial in BED, in which nivasorexant was unfortunately not efficacious compared with placebo. Public Significance: Nivasorexant is a new investigational drug for the treatment of binge‐eating disorder (BED). It underwent clinical testing in a phase II proof of concept trial in humans but was not efficacious compared with placebo. The current manuscript investigated the drug's efficacy in reducing binge‐like eating behavior of a highly palatable sweet and fat diet in a rat model of BED, which initially laid the foundation for the clinical trial. [ABSTRACT FROM AUTHOR]

Published

2024

28. Situational prevention: Pharmacotherapy during periods of increased risk for migraine attacks.

Author

Lipton, Richard B., Ailani, Jessica, Mullin, Kathleen, Pavlovic, Jelena M., Tepper, Stewart J., Dodick, David W., and Blumenfeld, Andrew M.

Subjects

*MIGRAINE prevention, *PATIENT safety, *CALCITONIN, *NEUROPEPTIDES, *DRUG efficacy, *MIGRAINE, *PREVENTIVE health services, *DRUG tolerance, *DISEASE risk factors, *CHEMICAL inhibitors

Abstract

The small molecule calcitonin gene–related peptide receptor antagonists (gepants) are the only drug class with medicines indicated for both the acute and preventive treatment of migraine. Given this dual capacity to both treat and prevent, along with their favorable tolerability profiles and lack of an association with medication‐overuse headache, headache specialists have begun to use gepants in ways that transcend the traditional categories of acute and preventive treatment. One approach, called situational prevention, directs patients to treat during the interictal phase, before symptoms develop, in situations of increased risk for migraine attacks. Herein, we present three patients to illustrate scenarios of gepant use for situational prevention. In each case, a gepant was started in anticipation of a period of increased headache probability (vulnerability) and continued for a duration of 1 day to 5 consecutive days. Although this approach may expose patients to medication when headache may not have developed, the tolerability and safety profile and preventive effect of gepants may represent a feasible approach for some patients. Situational prevention is an emerging strategy for managing migraine before symptoms develop in individuals who can identify periods when the probability of headache is high. This paper is intended to increase awareness of this strategy and stimulate future randomized, placebo‐controlled trials to rigorously assess this strategy. Plain Language Summary: A new class of migraine medicines, the gepants, does not cause medication‐overuse headache; these drugs can be taken in periods of increased headache risk, even before symptoms begin, to keep headaches from coming on. This new way of treating migraine is called "situational prevention." Experience in clinical practice suggests that treating migraine patients without current symptoms during times of increased headache risk, for example in connection with the menstrual cycle, travel, stress, or relaxation after stress, may be good times for situational prevention, but studies are needed to confirm when this strategy is most likely to be beneficial. [ABSTRACT FROM AUTHOR]

Published

2024

29. Protein kinase C epsilon‐mediated modulation of T‐type calcium channels underlies alcohol withdrawal hyperexcitability in the midline thalamus.

Author

Shan, Hong Qu, Smith, Thuy, Klorig, David C., and Godwin, Dwayne W.

Subjects

*PROTEIN kinases, *RESEARCH funding, *T-test (Statistics), *CALCIUM channels, *NEURONS, *DESCRIPTIVE statistics, *THALAMUS, *MICE, *ALCOHOL withdrawal syndrome, *ANIMAL experimentation, *ONE-way analysis of variance, *ALCOHOL drinking, *ALCOHOLISM, *BIOLOGICAL assay, *DATA analysis software, *CONFIDENCE intervals, *COMPARATIVE studies, *ELECTROPHYSIOLOGY, *CHEMICAL inhibitors

Abstract

Background: Millions of people struggle with alcohol use disorder (AUD). Abrupt abstinence after a period of chronic alcohol use can precipitate the alcohol withdrawal syndrome (AWS), which includes hyperexcitability and, potentially, seizures. We have shown that T‐type Ca2+ channels are novel, sensitive targets of alcohol, an effect that is dependent upon protein kinase C (PKC). The purpose of this study was to (1) understand midline thalamic neuronal hyperexcitability during alcohol withdrawal and its dependence on PKC; (2) characterize T channel functional changes using both current clamp and voltage clamp methods; and (3) determine which PKC isoform may be responsible for alcohol withdrawal (WD) effects. Methods: Whole‐cell patch clamp recordings were performed in midline thalamic neurons in brain slices prepared from C57bl/6 mice that underwent chronic intermittent alcohol exposure in a standard vapor chamber model. The recordings were compared to those from air‐exposed controls. T‐channel inactivation curves and burst responses were acquired through voltage‐clamp and current‐clamp recordings, respectively. Results: Whole‐cell voltage clamp recordings of native T‐type current exhibited a depolarizing shift in the voltage‐dependency of inactivation during alcohol withdrawal compared to air‐exposed controls. A PKCε translocation inhibitor peptide mitigated this change. Current clamp recordings demonstrated more spikes per burst during alcohol withdrawal. Consistent with voltage clamp findings, the PKCɛ translocation inhibitor peptide reduced the number of spikes per burst after WD. Conclusion: We found that alcohol WD produces T channel‐mediated hyperexcitability in the midline thalamus, produced in part by a shift in the inactivation curve consistent with greater availability of T current. WD effects on T current inactivation were reduced to control levels by blocking PKCε translocation. Our results demonstrate that PKCε translocation plays an important role in the regulation of alcohol withdrawal‐induced hyperexcitability in midline thalamic circuitry. [ABSTRACT FROM AUTHOR]

Published

2024

30. LRP4 mutations, dental anomalies, and oral exostoses.

Author

Kantaputra, Piranit, Panichkul, Weena, Sillapasorn, Parisri, Adisornkanj, Ploy, Kitsadayurach, Panita, Kaewgaya, Massupa, Intachai, Worrachet, Olsen, Bjorn, Ngamphiw, Chumpol, Leethanakul, Chidchanok, Jatooratthawichot, Peeranat, Ketudat Cairns, James R., and Tongsima, Sissades

Subjects

TEETH abnormality genetics, TEETH abnormalities, HYPODONTIA, CELLULAR signal transduction, LOW density lipoproteins, PEDIATRIC dentistry, INCISORS, EXOSTOSIS, GENETIC mutation, WNT proteins, CHEMICAL inhibitors

Abstract

Background: In order to generate a normal set of teeth, fine‐tuning of Wnt/β‐catenin signaling is required, in which WNT ligands bind to their inhibitors or WNT inhibitors bind to their co‐receptors. Lrp4 regulates the number of teeth and their morphology by modulating Wnt/β‐catenin signaling as a Wnt/β‐catenin activator or inhibitor, depending on its interactions with the partner proteins, such as Sostdc1 and Dkk1. Aim: To investigate genetic etiologies of dental anomalies involving LRP4 in a Thai cohort of 250 children and adults with dental anomalies. Design: Oral and radiographic examinations and whole exome sequencing were performed for every patient. Results: Two novel (p.Leu1356Arg and p.Ala1702Gly) and three recurrent (p.Arg263His, p.Gly1314Ser, and p.Asn1385Ser) rare variants in low‐density lipoprotein receptor‐related protein 4 (LRP4: MIM 604270) were identified in 11 patients. Oral exostoses were observed in five patients. Conclusion: Antagonism of Bmp signaling by Sostdc1 requires the presence of Lrp4. Mice lacking Lrp4 have been demonstrated to have alteration of Wnt–Bmp–Shh signaling and an abnormal number of incisors. Therefore, the LRP4 mutations found in our patients may disrupt Wnt–Bmp–Shh signaling, thereby resulting in dental anomalies and oral exostoses. Root maldevelopment in the patients suggests an important role of LRP4 in root morphogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

31. Hypoxia differently regulates the proportion of ALDHhi cells in lung squamous carcinoma H520 and adenocarcinoma A549 cells via the Wnt/β‐catenin pathway.

Author

Liu, Ni, Zheng, Qi, Zhang, Yuqing, Wang, Huimin, Zhang, Zhihui, He, Long, Wei, Chenxi, Xia, Handai, Liu, Yanguo, and Wang, Xiuwen

Subjects

*SQUAMOUS cell carcinoma, *ADENOCARCINOMA, *SMALL interfering RNA, *RESEARCH funding, *EPITHELIAL-mesenchymal transition, *DRUG resistance in cancer cells, *CALCIUM-binding proteins, *PLASMIDS, *POLYMERASE chain reaction, *CELL proliferation, *ALDEHYDE dehydrogenase, *CYTOSKELETAL proteins, *CELLULAR signal transduction, *CELL lines, *GENE expression, *MESSENGER RNA, *LUNG tumors, *WESTERN immunoblotting, *LUNG cancer, *STEM cells, *CELL differentiation, *HYPOXEMIA, *WNT proteins, *DISEASE progression, *CHEMICAL inhibitors

Abstract

Background: Cancer stem cells (CSCs) are a specific subpopulation of cancer cells with the ability of self‐renewal, infinite proliferation, multidifferentiation and tumorigenicity, and play critical roles in cancer progression and treatment resistance. CSCs are tightly regulated by the tumor microenvironment, such as hypoxia; however, how hypoxia regulates CSCs in non‐small cell lung cancer (NSCLC) remains unclear. Methods: The proportion of ALDHhi cells was examined using the Aldefluor assay. Tankyrase inhibitor XAV939 and siRNA were used to inhibit β‐catenin while pcDNA3‐β‐catenin (S33Y) plasmid enhanced the expression of β‐catenin. Western blot was administered for protein detection. The mRNA expression was measured by quantitative real‐time PCR. Results: We found that hypoxia led to an increase in the proportion of ALDHhi cells in lung squamous carcinoma (LUSC) H520 cells, while causing a decrease in the ALDHhi cell proportion in lung adenocarcinoma (LUAD) A549 cells. Similarly, β‐catenin expression was upregulated in H520 cells but downregulated in A549 cells upon exposure to hypoxia. Mechanically, the proportion of ALDHhi cells in both cell lines was decreased by β‐catenin inhibitor or siRNA knockdown, whereas increased after β‐catenin overexpression. Furthermore, hypoxia treatment suppressed E‐cadherin expression in H520 cells and enhanced N‐cadherin and β‐catenin expression, while this effect was completely opposite in A549 cells. Conclusion: The hypoxia‐EMT‐β‐catenin axis functions as an important regulator for the proportion of CSCs in NSCLC and could potentially be explored as therapeutic targets in the future. [ABSTRACT FROM AUTHOR]

Published

2024

32. Enhanced systemic antitumor efficacy of PD‐1/PD‐L1 blockade with immunological response induced by photodynamic therapy.

Author

Sonokawa, Takumi, Fujiwara, Yukio, Pan, Cheng, Komohara, Yoshihiro, and Usuda, Jitsuo

Subjects

*THERAPEUTIC use of monoclonal antibodies, *IN vitro studies, *RESEARCH funding, *KILLER cells, *CHEMICAL reagents, *PROGRAMMED death-ligand 1, *STATISTICAL sampling, *TREATMENT effectiveness, *COLON tumors, *MICE, *IMMUNOHISTOCHEMISTRY, *CYTOTOXINS, *COMBINED modality therapy, *ANIMAL experimentation, *PROGRAMMED cell death 1 receptors, *DRUG efficacy, *PHOTODYNAMIC therapy, *CELL survival, *IMMUNE checkpoint proteins, *IMMUNITY, *CHEMICAL inhibitors

Abstract

Background: Photodynamic therapy (PDT) is an antitumor therapy and has traditionally been regarded as a localized therapy in itself. However, recent reports have shown that it not only exerts a direct cytotoxic effect on cancer cells but also enhances body's tumor immunity. We hypothesized that the immunological response induced by PDT could potentially enhance the efficacy of programmed death‐1 (PD‐1) / programmed death‐ligand 1 (PD‐L1) blockade. Methods: The cytotoxic effects of PDT on colon 26 cells were investigated in vitro using the WST assay. We investigated whether the antitumor effect of anti‐PD‐1 antibodies could be amplified by the addition of PDT. We performed combination therapy by randomly allocating tumor‐bearing mice to four treatment groups: control, anti‐PD‐1 antibodies, PDT, and a combination of anti‐PD‐1 antibodies and PDT. To analyze the tumor microenvironment after treatment, the tumors were resected and pathologically evaluated. Results: The viability rate of colon 26 cells decreased proportionally with the laser dose. In vivo experiments for combined PDT and anti‐PD‐1 antibody treatment, combination therapy showed an enhanced antitumor effect compared with the control. Immunohistochemical findings of the tumor microenvironment 10 days after PDT indicated that the number of CD8+ cells, the area of Iba‐1+ cells and the area expressing PD‐L1 were significantly higher in tumors treated with combination therapy than in tumors treated with anti‐PD‐1 antibody alone, PDT alone, or the control. Conclusions: PDT increased immune cell infiltration into the tumor microenvironment. The immunological response induced by PDT may enhance the efficacy of PD‐1/PD‐L1 blockade. [ABSTRACT FROM AUTHOR]

Published

2024

33. Lack of effect from genetic deletion of Hdac6 in a humanized mouse model of CMT2D.

Author

Tadenev, Abigail L. D., Hatton, Courtney L., and Burgess, Robert W.

Subjects

*RNA metabolism, *BIOLOGICAL models, *SCIATIC nerve, *RESEARCH funding, *GENETIC engineering, *GENES, *MICE, *NERVE tissue proteins, *ANIMAL experimentation, *GENETIC mutation, *CHARCOT-Marie-Tooth disease, *ALLELES, *CHEMICAL inhibitors

Abstract

Background: Inhibition of HDAC6 has been proposed as a broadly applicable therapeutic strategy for Charcot–Marie–Tooth disease (CMT). Inhibition of HDAC6 increases the acetylation of proteins important in axonal trafficking, such as α‐tubulin and Miro, and has been shown to be efficacious in several preclinical studies using mouse models of CMT. Aims: Here, we sought to expand on previous preclinical studies by testing the effect of genetic deletion of Hdac6 on mice carrying a humanized knockin allele of Gars1, a model of CMT‐type 2D. Methods: Gars1ΔETAQ mice were bred to an Hdac6 knockout strain, and the resulting offspring were evaluated for clinically relevant outcomes. Results: The genetic deletion of Hdac6 increased α‐tubulin acetylation in the sciatic nerves of both wild‐type and Gars1ΔETAQ mice. However, when tested at 5 weeks of age, the Gars1ΔETAQ mice lacking Hdac6 showed no changes in body weight, muscle atrophy, grip strength or endurance, sciatic motor nerve conduction velocity, compound muscle action potential amplitude, or peripheral nerve histopathology compared to Gars1ΔETAQ mice with intact Hdac6. Interpretation: Our results differ from those of two previous studies that demonstrated the benefit of the HDAC6 inhibitor tubastatin A in mouse models of CMT2D. While we cannot fully explain the different outcomes, our results offer a counterexample to the benefit of inhibiting HDAC6 in CMT2D, suggesting additional research is necessary. [ABSTRACT FROM AUTHOR]

Published

2024

34. Clinical Characteristics of Cryopyrin‐Associated Periodic Syndrome and Long‐Term Real‐World Efficacy and Tolerability of Canakinumab in Japan: Results of a Nationwide Survey.

Author

Miyamoto, Takayuki, Izawa, Kazushi, Masui, Sho, Yamazaki, Atsue, Yamasaki, Yuichi, Matsubayashi, Tadashi, Shiraki, Mayuka, Ohnishi, Hidenori, Yasumura, Junko, Kawabe, Tomohiro, Miyamae, Takako, Matsubara, Tomoyo, Arakawa, Naoya, Ishige, Takashi, Takizawa, Takumi, Shimbo, Asami, Shimizu, Masaki, Kimura, Naoki, Maeda, Yuichi, and Maruyama, Yuta

Subjects

*PATIENT safety, *RESEARCH funding, *CRYOPYRIN-associated periodic syndromes, *SYMPTOMS, *DESCRIPTIVE statistics, *CAUSES of death, *AUTOINFLAMMATORY diseases, *DISEASE remission, *INVENTORY shortages, *RETROSPECTIVE studies, *DRUG efficacy, *GENETIC mutation, *SERODIAGNOSIS, *DRUGS, *INTERLEUKINS, *DISEASE progression, *EVALUATION, *CHEMICAL inhibitors

Abstract

Objective: We assess the clinical characteristics of patients with cryopyrin‐associated periodic syndrome (CAPS) in Japan and evaluate the real‐world efficacy and safety of interleukin‐1 (IL‐1) inhibitors, primarily canakinumab. Methods: Clinical information was collected retrospectively, and serum concentrations of canakinumab and cytokines were analyzed. Results: A total of 101 patients were included, with 86 and 15 carrying heterozygous germline and somatic mosaic mutations, respectively. We identified 39 mutation types, and the common CAPS‐associated symptoms corresponded with those in previous reports. Six patients (5.9% of all patients) died, with four of the deaths caused by CAPS‐associated symptoms. Notably, 73.7% of patients (100%, 79.6%, and 44.4% of familial cold autoinflammatory syndrome, Muckle–Wells syndrome, and chronic infantile neurological cutaneous articular syndrome/neonatal onset multisystem inflammatory disease, respectively) achieved complete remission with canakinumab, and early therapeutic intervention was associated with better auditory outcomes. In some patients, canakinumab treatment stabilized the progression of epiphysial overgrowth and improved height gain, visual acuity, and renal function. However, 23.7% of patients did not achieve inflammatory remission with crucial deterioration of organ damage, with two dying while receiving high‐dose canakinumab treatment. Serological analysis of canakinumab and cytokine concentrations revealed that the poor response was not related to canakinumab shortage. Four inflammatory nonremitters developed inflammatory bowel disease (IBD)—unclassified during canakinumab treatment. Dual biologic therapy with canakinumab and anti–tumor necrosis factor‐α agents was effective for IBD– and CAPS‐associated symptoms not resolved by canakinumab monotherapy. Conclusion: This study provides one of the largest epidemiologic data sets for CAPS. Although early initiation of anti–IL‐1 treatment with canakinumab is beneficial for improving disease prognosis, some patients do not achieve remission despite a high serum concentration of canakinumab. Moreover, IBD may develop in CAPS after canakinumab treatment. [ABSTRACT FROM AUTHOR]

Published

2024

35. Modulation of Interleukin‐23 Signaling With Guselkumab in Biologic‐Naive Patients Versus Tumor Necrosis Factor Inhibitor–Inadequate Responders With Active Psoriatic Arthritis.

Author

Siebert, Stefan, Coates, Laura C., Schett, Georg, Raychaudhuri, Siba P., Chen, Warner, Gao, Sheng, Seridi, Loqmane, Chakravarty, Soumya D., Shawi, May, Lavie, Frederic, Sharaf, Mohamed, Zimmermann, Miriam, Kollmeier, Alexa P., Xu, Xie L., Rahman, Proton, Mease, Philip J., and Deodhar, Atul

Subjects

*THERAPEUTIC use of monoclonal antibodies, *ANTI-inflammatory agents, *PSORIATIC arthritis, *PLACEBOS, *STATISTICAL sampling, *BLIND experiment, *CELLULAR signal transduction, *TREATMENT effectiveness, *RANDOMIZED controlled trials, *ANTIRHEUMATIC agents, *ACUTE phase proteins, *NURSING, *BIOLOGICAL products, *DESCRIPTIVE statistics, *RESEARCH, *RHEUMATOLOGY, *COMPARATIVE studies, *INTERLEUKINS, *TUMOR necrosis factors, *BIOMARKERS, *C-reactive protein, *CHEMICAL inhibitors

Abstract

Objective: We assessed and compared immunologic differences and associations with clinical response to guselkumab, a fully human interleukin (IL)–23p19 subunit inhibitor, in participants with active psoriatic arthritis (PsA) who were biologic‐naive or had inadequate response to tumor necrosis factor inhibitors (TNFi‐IR). Methods: Serum biomarker levels at baseline and after treatment with guselkumab 100 mg every 8 weeks were compared between biologic‐naive (n = 251) and TNFi‐IR (n = 93) subgroups identified in the pooled DISCOVER‐1/DISCOVER‐2/COSMOS data set. Baseline biomarker levels determined by achievement of week 24 clinical responses (≥75%/90% improvement in Psoriasis Area and Severity Index [PASI 75/90], Investigator's Global Assessment [IGA] of psoriasis score 0/1 and ≥2‐point improvement], ≥20% improvement in American College of Rheumatology criteria [ACR20]) were compared between prior treatment subgroups. Results: Baseline IL‐22, TNFα, and beta defensin‐2 (BD‐2) levels were significantly lower in biologic‐naive than in TNFi‐IR participants. With guselkumab, week 24 IL‐17A, IL‐17F, IL‐22, serum amyloid A, C‐reactive protein, IL‐6, and BD‐2 levels were significantly reduced from baseline in biologic‐naive and TNFi‐IR participants (≥1.4‐fold difference, nominal P < 0.05). Clinical responders to guselkumab exhibited significantly higher baseline levels of several biomarkers than nonresponders (IL‐17A, IL‐17F, BD‐2 in biologic‐naive PASI 90 responders; IL‐17A, BD‐2 in TNFi‐IR IGA 0/1 responders; IL‐22, BD‐2 in TNFi‐IR PASI 90 responders [nominal P < 0.05]) and trended higher in TNFi‐IR ACR20 responders. Conclusion: Guselkumab modulates IL‐23 signaling and provides consistent pharmacodynamic effects in both biologic‐naive and TNFi‐IR PsA patients. Significantly elevated baseline IL‐22, TNFα, and BD‐2 levels and associations between baseline IL‐22, IL‐17A, and BD‐2 levels and skin responses to guselkumab suggest greater dysregulation of IL‐23/Th17 signaling in patients with TNFi‐IR. [ABSTRACT FROM AUTHOR]

Published

2024

36. Honokiol regulates ovarian cancer cell malignant behavior through YAP/TAZ pathway modulation.

Author

Liu, Fang, Zhang, Yufang, Xia, Xinyi, Han, Jing, and Cao, Linyan

Subjects

*YAP signaling proteins, *RESEARCH funding, *OVARIAN tumors, *ANTINEOPLASTIC agents, *CELL proliferation, *APOPTOSIS, *CELLULAR signal transduction, *CELL motility, *PLANT extracts, *CELL lines, *GENE expression, *PHENOLS, *WESTERN immunoblotting, *CELL survival, *SIGNAL peptides, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Background: Ovarian cancer (OVCA) stands as one of the most fatal gynecological malignancies. Honokiol (HNK) has been substantiated by numerous studies for its anti‐tumor activity against malignancies including OVCA. Consequently, this work was designed to elucidate the impact of HNK‐mediated modulation of the YAP/TAZ pathway on the biological functions of OVCA cells. Methods: OVCA cells were subjected to treatment with varying concentrations (0, 25, 50, 75, and 100 μM) of HNK, concomitant with the administration of YAP agonist (XMU). Assessment of cellular viability was executed employing the CCK‐8 assay, while quantification of cellular proliferation transpired via colony formation assays. Apoptosis was ascertained using flow cytometry, and expression of apoptosis‐related proteins (caspase‐3, Bcl‐2, Bax), EMT‐related proteins (E‐cadherin, N‐cadherin), migration‐associated proteins (MMP‐2, MMP‐9), and YAP/TAZ pathway‐related proteins was evaluated by western blot. Transwell experiments were conducted to assess cellular migratory and invasive propensities. Xenograft tumor models were built to observe tumor growth (volume and weight), apoptosis was assessed by TUNEL staining, and Ki67 expression was evaluated through IHC. Results: HNK exerted inhibitory effects on the viability and proliferative capacity of OVCA cells, elicited apoptotic responses, curtailed the migratory and invasive tendencies of cells, and downregulated the YAP/TAZ pathway. Stimulation with YAP agonist (XMU‐MP‐1) partially attenuated the impacts of HNK on OVCA cell biology. Experiments in vivo confirmed that HNK inhibited OVCA tumor growth. Conclusion: The outcomes of this investigation conclusively established that HNK orchestrated the modulation of the YAP/TAZ pathway, thereby exerting control over the malignant phenotypic manifestations of OVCA cells. The ascertained function of HNK in restraining cellular proliferation and tumor progression provided novel evidence of its anti‐proliferative activity within OVCA cells. [ABSTRACT FROM AUTHOR]

Published

2024

37. Influence of fungicide selection and application timing on take‐all root rot management under field and greenhouse conditions.

Author

Stephens, Cameron M., Gannon, Travis W., Cubeta, Marc A., and Kerns, James P.

Subjects

BERMUDA grass, ROOT rots, FUNGICIDES, GREENHOUSES, CHEMICAL inhibitors, GRASS growing

Abstract

Take‐all root rot (TARR) is a detrimental disease of ultradwarf bermudagrass (Cynodon dactylon × Cynodon transvaalensis; UDB) putting greens frequently diagnosed where warm‐season grasses are grown. Since this disease is largely aggregated and variable under field conditions, field research is difficult and often yields inconsistent results. Multiple pathogens have only recently been associated with this disease, so practical management solutions such as fungicide efficacy and fungicide application timing have not been thoroughly investigated. Therefore, the objectives of this research were to determine the influence of fungicide selection and fungicide application timing on take‐all root rot management under field and greenhouse conditions. In general, fungicides from the quinone outside inhibitor and/or demethylation inhibitor chemical classes provided the greatest reduction in take‐all root rot severity. Fungicide applications that were made when soil temperatures were between 77–86°F provided the greatest disease suppression. The in vivo greenhouse method developed in this research proved to be an efficient and consistent method to evaluate management practices such as fungicide efficacy on take‐all root rot. This research improves our understanding of fungicide efficacy and fungicide application timing for take‐all root rot management on ultradwarf bermudagrass. Core Ideas: Fungicides from the QoI and/or DMI chemical class provided the greatest reduction in take‐all root rot severity.Apply fungicides when the 5‐day average soil temperature at a 2‐inch depth is approximately 80°F for TARR management.The in vivo screening method developed here is an efficient way to evaluate TARR management parameters. [ABSTRACT FROM AUTHOR]

Published

2024

38. ZNF862 induces cytostasis and apoptosis via the p21‐RB1 and Bcl‐xL‐Caspase 3 signaling pathways in human gingival fibroblasts.

Author

Zhu, Yaoyao, Zhao, Tian, Wu, Yongkang, Xie, Sijing, Sun, Weibin, and Wu, Juan

Subjects

IN vitro studies, RESEARCH funding, GINGIVA, CELL proliferation, APOPTOSIS, CELLULAR signal transduction, FLUORESCENT antibody technique, CELL motility, CELL cycle, REVERSE transcriptase polymerase chain reaction, GENE expression, FIBROBLASTS, IMMUNOHISTOCHEMISTRY, RETINOBLASTOMA, WESTERN immunoblotting, GENE expression profiling, CYTOPLASM, STAINS & staining (Microscopy), CASPASES, CYCLIN-dependent kinases, B cell lymphoma, CHEMICAL inhibitors

Abstract

Objective: This study investigates the effects of ZNF862 on the proliferation and apoptosis of human gingival fibroblasts and their related mechanisms. Background: As a major transcription factor family, zinc finger proteins (ZFPs) regulate cell differentiation, growth, and apoptosis through their conserved zinc finger motifs, which allow high flexibility and specificity in gene regulation. In our previous study, ZNF862 mutation was associated with hereditary gingival fibromatosis. Nevertheless, little is known about the biological function of ZNF862. Therefore, this study was aimed to reveal intracellular localization of ZNF862, the influence of ZNF862 on the growth and apoptosis of human gingival fibroblasts (HGFs) and its potential related mechanisms. Methods: Immunohistochemistry, immunofluorescence staining, and western blotting were performed to determine the intracellular localization of ZNF862 in HGFs. HGFs were divided into three groups: ZNF862 overexpression group, ZNF862 interference group, and the empty vector control group. Then, the effects of ZNF862 on cell proliferation, migration, cell cycle, and apoptosis were evaluated. qRT‐PCR and western blotting were performed to further explore the mechanism related to the proliferation and apoptosis of HGFs. Results: ZNF862 was found to be localized in the cytoplasm of HGFs. In vitro experiments revealed that ZNF862 overexpression inhibited HGFs proliferation and migration, induced cell cycle arrest at the G0/G1‐phase and apoptosis. Whereas, ZNF862 knockdown promoted HGFs proliferation and migration, accelerated the transition from the G0/G1 phase into the S and G2/M phase and inhibited cell apoptosis. Mechanistically, the effects of ZNF862 on HGFs proliferation and apoptosis were noted to be dependent on inhibiting the cyclin‐dependent kinase inhibitor 1A (p21)‐retinoblastoma 1 (RB1) signaling pathway and enhancing the B‐cell lymphoma‐extra‐large (Bcl‐xL)‐Caspase 3 signaling pathway. Conclusion: Our results for the first time reveal that ZNF862 is localized in the cytoplasm of HGFs. ZNF862 can inhibit the proliferation of HGFs by inhibiting the p21‐RB1 signaling pathway, and it also promotes the apoptosis of HGFs by enhancing the Bcl‐xL‐Caspase 3 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2024

39. Melatonin attenuates dental pulp stem cells senescence due to vitro expansion via inhibiting MMP3.

Author

Zhang, Zeying, Bao, Yandong, Wei, Penggong, Yan, Xiaoyuan, Qiu, Qiujing, and Qiu, Lihong

Subjects

*IN vitro studies, *ANTI-inflammatory agents, *DENTAL pulp, *RESEARCH funding, *CELLULAR aging, *MELATONIN, *REVERSE transcriptase polymerase chain reaction, *TREATMENT effectiveness, *CELLULAR signal transduction, *TRANSCRIPTION factors, *GENES, *BIOINFORMATICS, *JANUS kinases, *MATRIX metalloproteinases, *WESTERN immunoblotting, *RESEARCH, *STEM cells, *STAINS & staining (Microscopy), *NEUROTRANSMITTER uptake inhibitors, *INTERLEUKINS, *CHEMICAL inhibitors

Abstract

Objective: We aimed to identify the crucial genes involved in dental pulp stem cell (DPSC) senescence and evaluate the impact of melatonin on DPSC senescence. Methods: Western blotting, SA‐β‐Gal staining and ALP staining were used to evaluate the senescence and differentiation potential of DPSCs. The optimal concentration of melatonin was determined using the CCK‐8 assay. Differentially expressed genes (DEGs) involved in DPSC senescence were obtained via bioinformatics analysis, followed by RT–qPCR. Gain‐ and loss‐of‐function studies were conducted to explore the role of MMP3 in DPSC in vitro expansion and in response to melatonin. GSEA was employed to analyse MMP3‐related pathways in cellular senescence. Results: Treatment with 0.1 μM melatonin attenuated cellular senescence and differentiation potential suppression in DPSCs due to long‐term in vitro expansion. MMP3 was a crucial gene in senescence, as confirmed by bioinformatics analysis, RT–qPCR and Western blotting. Furthermore, gain‐ and loss‐of‐function studies revealed that MMP3 played a regulatory role in cellular senescence. Rescue assays showed that overexpression of MMP3 reversed the effect of melatonin on senescence. GSEA revealed that the MMP3‐dependent anti‐senescence effect of melatonin was associated with the IL6‐JAK‐STAT3, TNF‐α‐Signalling‐VIA‐NF‐κB, COMPLEMENT, NOTCH Signalling and PI3K‐AKT‐mTOR pathways. Conclusion: Melatonin attenuated DPSC senescence caused by long‐term expansion by inhibiting MMP3. [ABSTRACT FROM AUTHOR]

Published

2024

40. Nonspecific oral medications versus anti–calcitonin gene‐related peptide monoclonal antibodies for migraine: A systematic review and meta‐analysis of randomized controlled trials.

Author

Robblee, Jennifer, Hakim, Sameh M., Reynolds, John M., Monteith, Teshamae S., Zhang, Niushen, and Barad, Meredith

Subjects

*THERAPEUTIC use of monoclonal antibodies, *MEDICAL information storage & retrieval systems, *EFFECT sizes (Statistics), *GREY literature, *TOPIRAMATE, *HEALTH insurance reimbursement, *RESEARCH funding, *HEADACHE, *CALCITONIN, *ORAL drug administration, *TREATMENT effectiveness, *META-analysis, *GENES, *PEPTIDES, *SYSTEMATIC reviews, *MEDLINE, *MEDICAL databases, *VALPROIC acid, *COMPARATIVE studies, *MIGRAINE, *PSYCHOLOGY information storage & retrieval systems, *SEQUENCE analysis, *EVALUATION, *CHEMICAL inhibitors

Abstract

Objective: To compare calcitonin gene–related peptide monoclonal antibodies (CGRP mAbs) versus nonspecific oral migraine preventives (NOEPs). Background: Insurers mandate step therapy with NOEPs before approving CGRP mAbs. Methods: Databases were searched for class I or II randomized controlled trials (RCTs) comparing CGRP mAbs or NOEPs versus placebo for migraine prevention in adults. The primary outcome measure was monthly migraine days (MMD) or moderate to severe headache days. Results: Twelve RCTs for CGRP mAbs, 5 RCTs for topiramate, and 3 RCTs for divalproex were included in the meta‐analysis. There was high certainty that CGRP mAbs are more effective than placebo, with weighted mean difference (WMD; 95% confidence interval) of −1.64 (−1.99 to −1.28) MMD, which is compatible with small effect size (Cohen's d −0.25 [−0.34 to −0.16]). Certainty of evidence that topiramate or divalproex is more effective than placebo was very low and low, respectively (WMD −1.45 [−1.52 to −1.38] and −1.65 [−2.30 to −1.00], respectively; Cohen's d −1.25 [−2.47 to −0.03] and −0.48 [−0.67 to −0.29], respectively). Trial sequential analysis showed that information size was adequate and that CGRP mAbs had clear benefit versus placebo. Network meta‐analysis showed no statistically significant difference between CGRP mAbs and topiramate (WMD −0.19 [−0.56 to 0.17]) or divalproex (0.01 [−0.73 to 0.75]). No significant difference was seen between topiramate or divalproex (0.21 [−0.45 to 0.86]). Conclusions: There is high certainty that CGRP mAbs are more effective than placebo, but the effect size is small. When feasible, CGRP mAbs may be prescribed as first‐line preventives; topiramate or divalproex could be as effective but are less well tolerated. The findings of this study support the recently published 2024 position of the American Headache Society on the use of CGRP mAbs as the first‐line treatment. Plain Language Summary: Insurance companies often do not approve calcitonin gene–related peptide monoclonal antibodies (CGRP mAbs) for the treatment of migraine until patients have tried other medicines first. We reviewed and summarized data from studies that reported how well different migraine medications worked, including CGRP mAbs, and found evidence that CGRP mAbs are more effective than placebo and just as effective as other migraine drugs. This suggests that CGRP mAbs should be offered as a first‐line preventive therapy at the discretion of the clinician and the individual patient. Answer questions and earn CME credit: https://wileyhealthlearning.com/#/online‐courses/d524dd0e‐d6b3‐4fd3‐b298‐230b74599848 [ABSTRACT FROM AUTHOR]

Published

2024

41. Corrosion Inhibition of Carbon Steel by Some Schiff Base Compounds in HCl and H2SO4 Solutions.

Author

Iranpour, Maryam, Babaei, Ali, and Bagherzadeh, Mojtaba

Subjects

*CARBON steel corrosion, *SCHIFF bases, *CARBON steel, *ADSORPTION isotherms, *CHEMICAL inhibitors

Abstract

The inhibition power of two Schiff bases on carbon steel corrosion in 1 M HCl and 0.5 M H2SO4 solutions has been investigated using weight loss, Tafel polarization, and electrochemical impedance spectroscopy techniques. The results revealed that increasing the concentration of inhibitors in acidic solutions led to a higher inhibition efficiency. The polarization curves indicated that the Schiff bases acted as mixed inhibitors, affecting both the cathodic and anodic reactions. The adsorption of the inhibitors on the carbon steel surface followed the Langmuir adsorption isotherm, and various adsorption isotherm parameters such as Kads, ΔGads, ΔHads, and ΔSads were determined at room temperature. Furthermore, the effect of temperature on the inhibitors′ performance was examined within the range of 25–45 °C. The corrosion‐related activation energy, pre‐exponential factor (k), activation enthalpy, and entropy were calculated to assess the inhibitors′ behavior. Scanning electron microscopy (SEM) was employed to examine some carbon steel samples, revealing differences in inhibition efficiency attributed to the inhibitors′ chemical structure. The results highlighted the highest inhibition efficiency in H2SO4 medium at 93.4 %, with a corresponding free energy of 39.51 KJ/mol indicating physical‐chemical adsorption of inhibitor molecules. Furthermore, an enthalpy value of −40.6 KJ/mol suggested an exothermic inhibitor absorption process. The findings are presented and discussed in detail. [ABSTRACT FROM AUTHOR]

Published

2024

42. Sex Differences in the Effectiveness of First‐Line Tumor Necrosis Factor Inhibitors in Psoriatic Arthritis: Results From the European Spondyloarthritis Research Collaboration Network.

Author

Hellamand, Pasoon, van de Sande, Marleen G. H., Ørnbjerg, Lykke M., Klausch, Thomas, Eklund, Kari K., Relas, Heikki, Santos, Maria J., Vieira‐Sousa, Elsa, Loft, Anne G., Glintborg, Bente, Østergaard, Mikkel, Lindström, Ulf, Wallman, Johan K., Michelsen, Brigitte, Fagerli, Karen M., Castrejón, Isabel, Gudbjornsson, Bjorn, Love, Thorvardur J., Vencovský, Jiří, and Nekvindová, Lucie

Subjects

*PATIENT compliance, *PSORIATIC arthritis, *SEX distribution, *LOGISTIC regression analysis, *HUMAN research subjects, *TREATMENT effectiveness, *ANTIRHEUMATIC agents, *DESCRIPTIVE statistics, *RELATIVE medical risk, *KAPLAN-Meier estimator, *DRUG efficacy, *SYNTHETIC drugs, *CONFIDENCE intervals, *TUMOR necrosis factors, *C-reactive protein, *PATIENT participation, *EVALUATION, *CHEMICAL inhibitors

Abstract

Objective: Women with psoriatic arthritis (PsA) may have reduced tumor necrosis factor inhibitor (TNFi) effectiveness compared to men. We examined sex differences in treatment response and retention rates during 24 months of follow‐up among patients with PsA initiating their first TNFi. Methods: Data from patients with PsA across 13 European Spondyloarthritis Research Collaboration Network registries starting their first TNFi were pooled. Logistic regression was used to analyze the association between sex and treatment response using low disease activity (LDA) according to the Disease Activity Score in 28 joints using the C‐reactive protein level (DAS28‐CRP) (<3.2) at six months as the primary outcome. Analyses were adjusted for age, country, conventional synthetic disease‐modifying antirheumatic drug treatment, and TNFi start year. Retention rates were explored using the Kaplan–Meier estimator. Results: We analyzed the treatment response of 7,679 patients with PsA (50% women) with available data on LDA at six months. At baseline, women and men had similar characteristics, including mean DAS28‐CRP (women vs men, 4.4 [SD 1.2] vs 4.2 [SD 1.2]), though patient‐reported outcome measures were worse in women. At six months, 64% of women and 78% of men had LDA (relative risk [RR] 0.82; 95% confidence interval [CI] 0.80–0.84). This difference was similar after adjustment (RR 0.83; 95% CI 0.81–0.85). TNFi retention rates were evaluated in 17,842 patients with PsA. Women had significantly lower retention rates than men at all time points (women 79%, 64%, and 50% vs men 88%, 77%, and 64% at 6, 12, and 24 months, respectively). Conclusion: Despite comparable disease characteristics at baseline, women with PsA have reduced treatment response and retention rates to their first TNFi, highlighting the need to consider sex differences in PsA research and management. [ABSTRACT FROM AUTHOR]

Published

2024

43. Determinants of Achieving Serum Urate Goal with Treat‐to‐Target Urate‐Lowering Therapy in Gout.

Author

Helget, Lindsay N., O'Dell, James R., Newcomb, Jeff A., Androsenko, Maria, Brophy, Mary T., Davis‐Karim, Anne, England, Bryant R., Ferguson, Ryan, Pillinger, Michael H., Neogi, Tuhina, Palevsky, Paul M., Wu, Hongsheng, Kramer, Bridget, and Mikuls, Ted R.

Subjects

*PATIENT compliance, *SOCIAL determinants of health, *BODY mass index, *RESEARCH funding, *PREDICTION models, *ENZYME inhibitors, *MULTIPLE regression analysis, *GOAL (Psychology), *RANDOMIZED controlled trials, *DIURETICS, *MULTIVARIATE analysis, *DESCRIPTIVE statistics, *GOUT suppressants, *ODDS ratio, *RACE, *GOUT, *ALLOPURINOL, *OXIDOREDUCTASES, *URIC acid, *QUALITY of life, *COMPARATIVE studies, *SOCIODEMOGRAPHIC factors, *DRUGS, *INDIVIDUALIZED medicine, *COMORBIDITY, *EDUCATIONAL attainment, *CHEMICAL inhibitors

Abstract

Objective: Using trial data comparing treat‐to‐target allopurinol and febuxostat in gout, we examined participant characteristics associated with serum urate (SU) goal achievement. Methods: Participants with gout and SU ≥6.8 mg/dL were randomized to allopurinol or febuxostat, titrated during weeks 0 to 24, and maintained weeks 25 to 48. Participants were considered to achieve SU goal if the mean SU from weeks 36, 42, and 48 was <6.0 mg/dL or <5 mg/dL if tophi were present. Possible determinants of treatment response were preselected and included sociodemographics, comorbidities, diuretic use, health‐related quality of life (HRQoL), body mass index, and gout measures. Determinants of SU response were assessed using multivariable logistic regression with additional analyses to account for treatment adherence. Results: Of 764 study participants completing week 48, 618 (81%) achieved SU goal. After multivariable adjustment, factors associated with a greater likelihood of SU goal achievement included older age (adjusted odds ratio [aOR] 1.40 per 10 years), higher education (aOR 2.02), and better HRQoL (aOR 1.17 per 0.1 unit). Factors associated with a lower odds of SU goal achievement included non‐White race (aORs 0.32–0.47), higher baseline SU (aOR 0.83 per 1 mg/dL), presence of tophi (aOR 0.29), and the use of diuretics (aOR 0.52). Comorbidities including chronic kidney disease, hypertension, diabetes, and cardiovascular disease were not associated with SU goal achievement. Results were not meaningfully changed in analyses accounting for adherence. Conclusions: Several patient‐level factors were predictive of SU goal achievement among patients with gout who received treat‐to‐target urate‐lowering therapy (ULT). Approaches that accurately predict individual responses to treat‐to‐target ULT hold promise in facilitating personalized management and improving outcomes in patients with gout. [ABSTRACT FROM AUTHOR]

Published

2024

44. Targeting TGF beta receptor 1 in head and neck squamous cell carcinoma.

Author

Jank, Bernhard J., Schnoell, Julia, Kladnik, Katharina, Sparr, Carmen, Haas, Markus, Gurnhofer, Elisabeth, Lein, Alexander L., Brunner, Markus, Kenner, Lukas, Kadletz‐Wanke, Lorenz, and Heiduschka, Gregor

Subjects

*THERAPEUTIC use of antineoplastic agents, *SQUAMOUS cell carcinoma, *HETEROCYCLIC compounds, *RISK assessment, *PROTEIN kinases, *CANCER, *HEAD & neck cancer, *CELL physiology, *MULTIVARIATE analysis, *DESCRIPTIVE statistics, *GENE expression, *RADIATION-sensitizing agents, *LONGITUDINAL method, *FIBROBLASTS, *CELL lines, *MESSENGER RNA, *IMMUNOHISTOCHEMISTRY, *AMINES, *CANCER patient psychology, *TRANSFORMING growth factors-beta, *CELL receptors, *OVERALL survival, *CHEMICAL inhibitors, MORTALITY risk factors

Abstract

Objectives: The transforming growth factor‐Beta (TGF‐ß) pathway may be involved in the radioresistance of head and neck squamous cell carcinoma (HNSCC). This study analyzed TGF‐ß receptor 1 (TGFBR1) expression in HNSCC patients and evaluated the antineoplastic and radiosensitizing effects of vactosertib, a novel TGFBR1 inhibitor, in vitro. Materials and Methods: TGFBR1 expression was examined in HNSCC patients at the mRNA level in silico and the protein level by immunohistochemistry, including surgical specimens of primary tumors, matched lymph node metastasis, and recurrent disease. Furthermore, a novel small molecule TGFBR1 inhibitor was evaluated in HNSCC cell lines. Finally, an indirect coculture model using patient‐derived cancer‐associated fibroblasts was applied to mimic the tumor microenvironment. Results: Patients with high TGFBR1 mRNA levels showed significantly worse overall survival in silico (OS, p = 0.024). At the protein level, an association between TGFBR1+ tumor and OS was observed for the subgroup with TGFBR1‐stroma (p = 0.001). Those results prevailed in multivariable analysis. Inhibition of TGFBR1 showed antineoplastic effects in vitro. In combination with radiation, vactosertib showed synergistic effects. Conclusion: Our results indicate a high risk of death in tumorTGFBR1+|stromaTGFBR1‐ expressing patients. In vitro data suggest a potential radiosensitizing effect of TGFBR1 inhibition by vactosertib. [ABSTRACT FROM AUTHOR]

Published

2024

45. Notch activation promotes bone metastasis via SPARC inhibition in adenoid cystic carcinoma.

Author

Zhang, Ye, Liu, Xiaoxiao, Zhu, Lijing, Zhou, Zheng, Cui, Yajuan, Zhou, Chuan‐Xiang, and Li, Tie‐jun

Subjects

*BONE resorption, *CELL migration, *PEARSON correlation (Statistics), *IN vitro studies, *OSTEOBLASTS, *ACADEMIC medical centers, *MOUTH tumors, *SURVIVAL rate, *RESEARCH funding, *HEAD & neck cancer, *CELL proliferation, *BONE growth, *FISHER exact test, *TUMOR markers, *GLYCOPROTEINS, *CELLULAR signal transduction, *CANCER patients, *RETROSPECTIVE studies, *REVERSE transcriptase polymerase chain reaction, *NEOVASCULARIZATION inhibitors, *CHI-squared test, *SALIVARY gland tumors, *DESCRIPTIVE statistics, *BONE metastasis, *ADENOID cystic carcinoma, *IMMUNOHISTOCHEMISTRY, *CELL lines, *MESSENGER RNA, *KAPLAN-Meier estimator, *LOG-rank test, *FACE diseases, *WESTERN immunoblotting, *GENE expression profiling, *MICROBIOLOGICAL assay, *GENETIC mutation, *CELL differentiation, *FACTOR analysis, *MICROSCOPY, *STAINS & staining (Microscopy), *TUMORS, *DATA analysis software, *CONFIDENCE intervals, *SEQUENCE analysis, *OVERALL survival, *CHEMICAL inhibitors, PAROTID gland tumors

Abstract

Objectives: We aimed to investigate bone metastasis induced by Notch signalling pathway dysregulation and to demonstrate that SPARC is a potential therapeutic target in adenoid cystic carcinoma (AdCC) with Notch dysregulation. Materials and Methods: This retrospective study enrolled 144 AdCC patients. RNA‐sequencing and enrichment analyses were performed using 32 AdCC samples. Osteonectin/SPARC and the Notch activation indicator Notch intracellular domain (NICD) were detected using immunohistochemistry. Cell proliferation and migration assays were conducted using stably NICD over‐expressing cells. The effect of SPARC on osteoclast differentiation in NICD cells was investigated using western blotting, quantitative reverse transcription PCR, tartrate‐resistant acid phosphatase staining and resorption assays. Results: RNA‐sequencing analysis showed that genes down‐regulated in Notch‐mutant AdCCs, such as SPARC, were enriched in ossification and osteoblast differentiation. Most (75/110, 68.2%) Notch1‐wild‐type AdCCs showed SPARC over‐expression, whereas 30 out of 34 (88.2%) Notch1‐mutant tumours showed low SPARC expression. SPARC over‐expression was then found negatively to be correlated with NICD expression in 144 AdCCs. NICD over‐expression promoted cell growth, migration and osteoclast differentiation, which could be partly reversed by exogenous SPARC. Conclusions: Notch activation in AdCC contributes to bone metastasis through SPARC inhibition. The study results suggest that SPARC may represent a prognostic biomarker and potential therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2024

46. Calcitonin gene‐related peptide‐targeting therapies are a first‐line option for the prevention of migraine: An American Headache Society position statement update.

Author

Charles, Andrew C., Digre, Kathleen B., Goadsby, Peter J., Robbins, Matthew S., Hershey, Andrew, Schwedt, Todd J., Ailani, Jessica, Tepper, Stewart J., Halker Singh, Rashmi B., Harriott, Andrea M., Lay, Christine, Nahas, Stephanie J., Powers, Scott W., Rosen, Noah, Starling, Amaal J., and Wells, Rebecca

Subjects

*MIGRAINE prevention, *THERAPEUTIC use of monoclonal antibodies, *PATIENT compliance, *PATIENT safety, *DATA analysis, *DRUG side effects, *HEADACHE, *DISEASE management, *SCIENTIFIC observation, *CALCITONIN, *RETROSPECTIVE studies, *LONGITUDINAL method, *DRUG efficacy, *STATISTICS, *MEDICAL records, *ACQUISITION of data, *PEPTIDE antibiotics, *DRUGS, *MIGRAINE, *DRUG tolerance, *PREVENTIVE health services, *EVALUATION, *CHEMICAL inhibitors

Abstract

Objective: To provide a position statement update from The American Headache Society specifically regarding therapies targeting calcitonin gene‐related peptide (CGRP) for the prevention of migraine. Background: All migraine preventive therapies previously considered to be first‐line treatments were developed for other indications and adopted later for migraine. Adherence to these therapies is often poor due to issues with efficacy and tolerability. Multiple new migraine‐specific therapies have been developed based on a broad foundation of pre‐clinical and clinical evidence showing that CGRP plays a key role in the pathogenesis of migraine. These CGRP‐targeting therapies have had a transformational impact on the management of migraine but are still not widely considered to be first‐line approaches. Methods: Evidence regarding migraine preventive therapies including primary and secondary endpoints from randomized placebo‐controlled clinical trials, post hoc analyses and open‐label extensions of these trials, and prospective and retrospective observational studies were collected from a variety of sources including PubMed, Google Scholar, and ClinicalTrials.gov. The results and conclusions based upon these results were reviewed and discussed by the Board of Directors of The American Headache Society to confirm consistency with clinical experience and to achieve consensus. Results: The evidence for the efficacy, tolerability, and safety of CGRP‐targeting migraine preventive therapies (the monoclonal antibodies: erenumab, fremanezumab, galcanezumab, and eptinezumab, and the gepants: rimegepant and atogepant) is substantial, and vastly exceeds that for any other preventive treatment approach. The evidence remains consistent across different individual CGRP‐targeting treatments and is corroborated by extensive "real‐world" clinical experience. The data indicates that the efficacy and tolerability of CGRP‐targeting therapies are equal to or greater than those of previous first‐line therapies and that serious adverse events associated with CGRP‐targeting therapies are rare. Conclusion: The CGRP‐targeting therapies should be considered as a first‐line approach for migraine prevention along with previous first‐line treatments without a requirement for prior failure of other classes of migraine preventive treatment. [ABSTRACT FROM AUTHOR]

Published

2024

47. High glucose impairs human periodontal ligament cells migration through lowered microRNAs 221 and 222.

Author

Monteiro, Mariana Marin, Gomes, Cibele Crastequini, Cruz, Mario Costa, Horliana, Anna Carolina R. Tempestini, Hamassaki, Dânia Emi, Lima, Cilene Rebouças, and Santos, Marinilce F.

Subjects

CELL analysis, PERIODONTIUM, GLUCOSE, RESEARCH funding, MICRORNA, APOPTOSIS, CELL motility, CYTOSKELETAL proteins, REVERSE transcriptase polymerase chain reaction, BLOOD sugar, CELL culture, FIBRONECTINS, OLIGONUCLEOTIDES, GENE expression, BICUSPIDS, PERIODONTAL ligament, DIABETES, CHEMICAL inhibitors

Abstract

Objective: To investigate the effects of miR‐221 and miR‐222 and high glucose on human periodontal ligament (PL) cells morphology, cytoskeleton, adhesion, and migration. Background: Chronic hyperglycemia is common in uncontrolled diabetes mellitus (DM) and plays a central role in long‐term DM complications, such as impaired periodontal healing. We have previously shown that high glucose increases apoptosis of human PL cells by inhibiting miR‐221 and miR‐222 and consequently augmenting their target caspase‐3. However, other effects of miR‐221/222 downregulation on PL cells are still unknown. Methods: Cells from young humans' premolar teeth were cultured for 7 days under 5 or 30 mM glucose. Directional and spontaneous migration on fibronectin were studied using transwell and time‐lapse assays, respectively. F‐actin staining was employed to study cell morphology and the actin cytoskeleton. MiR‐221 and miR‐222 were inhibited using antagomiRs, and their expressions were evaluated by real‐time RT‐PCR. Results: High glucose inhibited PL cells early adhesion, spreading, and migration on fibronectin. Cells exposed to high glucose showed reduced polarization, velocity, and directionality. They formed several simultaneous unstable and short‐lived protrusions, suggesting impairment of adhesion maturation. MiR‐221 and miR‐222 inhibition also reduced migration, decreasing cell directionality but not significantly cell velocity. After miR‐221 and miR‐222 downregulation cells showed morphological resemblance with cells exposed to high glucose. Conclusion: High glucose impairs human PL cells migration potentially through a mechanism involving reduction of microRNA‐221 and microRNA‐222 expression. These effects may contribute to the impairment of periodontal healing, especially after surgery and during guided regeneration therapies. [ABSTRACT FROM AUTHOR]

Published

2024

48. Do P‐glycoprotein Medications Alter the Risk of Ventriculoperitoneal Shunt in Adults with Hydrocephalus?

Author

Grullon, Jason R., Koutsouras, George W., Onwumere, Nneka F., Lehmann, David F., and Krishnamurthy, Satish

Subjects

*HYDROCEPHALUS, *RETROSPECTIVE studies, *ACQUISITION of data, *MEMBRANE glycoproteins, *CEREBROSPINAL fluid shunts, *TREATMENT effectiveness, *COMPARATIVE studies, *MEDICAL records, *PATIENT safety, *CHEMICAL inhibitors, *ADULTS

Abstract

Hydrocephalus is a disorder caused by excess fluid accumulation in the brain and results in brain damage with consequent cognitive and physical problems. This condition has no cure; the only treatment is brain surgery. Experimental data indicate that P‐glycoprotein (P‐gp) plays a crucial role in the pathogenesis of hydrocephalus due to its function in clearing macromolecules from the brain. Numerous medications frequently used are classified as P‐gp inducers or inhibitors, and comprehending their effects may aid in attaining improved patient outcomes. Therefore, in this single‐center retrospective study, we examined the risk of the need for ventriculoperitoneal shunt placement over 10 years among 4588 adult patients with hydrocephalus not exposed to any P‐gp inhibitors/inducers or exclusively exposed to either P‐gp inhibitors or inducers. Our analysis shows that patients exposed to P‐gp inhibitors had a 3.2 times higher risk of requiring ventriculoperitoneal shunt surgery (P <.0001). In contrast, the relative risk was not significantly affected (P =.07) among those exposed to P‐gp inducers. Our findings indicate the need for caution when prescribing P‐gp inhibitors to patients with hydrocephalus. Additional studies using larger cohorts are required to confirm whether P‐gp inducers in patients with hydrocephalus can mitigate the risk of ventriculoperitoneal shunt. [ABSTRACT FROM AUTHOR]

Published

2024

49. PDZ‐binding kinase inhibitor OTS514 suppresses the proliferation of oral squamous carcinoma cells.

Author

Kato, Mikako, Ota, Akinobu, Ono, Takayuki, Karnan, Sivasundaram, Hyodo, Toshinori, Rahman, Md Lutfur, Hasan, Muhammad Nazmul, Onda, Maho, Kondo, Sayuri, Ito, Kunihiro, Furuhashi, Akifumi, Hayashi, Tomio, Konishi, Hiroyuki, Tsuzuki, Shinobu, Hosokawa, Yoshitaka, and Kazaoka, Yoshiaki

Subjects

*MOUTH tumors, *DNA, *PROTEIN kinase inhibitors, *ANIMAL experimentation, *HEAD & neck cancer, *APOPTOSIS, *ANTINEOPLASTIC agents, *MICROARRAY technology, *SIGNAL peptides, *CELL survival, *GENE expression, *CELL proliferation, *GENE expression profiling, *RESEARCH funding, *CELL lines, *MOLECULAR structure, *TRANSCRIPTION factors, *SQUAMOUS cell carcinoma, *MICE, *CARRIER proteins, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Objective: PDZ‐binding kinase (PBK) has been reported as a poor prognostic factor and is a promising molecular target for anticancer therapeutics. Here, we aimed to investigate the effect of specific PBK inhibitor OTS514 on the survival of OSCC cells. Methods: Four OSCC cell lines (HSC‐2, HSC‐3, SAS, and OSC‐19) were used to examine the effect of OTS514 on cell survival and apoptosis. DNA microarray analysis was conducted to investigate the effect of OTS514 on gene expression in OSCC cells. Gene set enrichment analysis was performed to identify molecular signatures related to the antiproliferative effect of OTS514. Results: OTS514 decreased the cell survival of OSCC cells dose‐dependently, and administration of OTS514 readily suppressed the HSC‐2‐derived tumor growth in immunodeficient mice. Treatment with OTS514 significantly increased the number of apoptotic cells and caspase‐3/7 activity. Importantly, OTS514 suppressed the expression of E2F target genes with a marked decrease in protein levels of E2F1, a transcriptional factor. Moreover, TP53 knockdown attenuated OTS514‐induced apoptosis. Conclusion: OTS514 suppressed the proliferation of OSCC cells by downregulating the expression of E2F target genes and induced apoptosis by mediating the p53 signaling pathway. These results highlight the clinical application of PBK inhibitors in the development of molecular‐targeted therapeutics against OSCC. [ABSTRACT FROM AUTHOR]

Published

2024

50. Histone deacetylase inhibitor decreases hyperalgesia in a mouse model of alcohol withdrawal‐induced hyperalgesia.

Author

Aguilar, Jhoan, De Carvalho, Luana Martins, Chen, Hu, Condon, Ryan, Lasek, Amy W., and Pradhan, Amynah A.

Subjects

*BIOLOGICAL models, *T-test (Statistics), *RESEARCH funding, *ETHANOL, *EPIGENOMICS, *BINGE drinking, *PAIN threshold, *DESCRIPTIVE statistics, *HYPERALGESIA, *MICE, *ALCOHOL withdrawal syndrome, *ANIMAL experimentation, *ANALYSIS of variance, *ALCOHOL drinking, *ALCOHOLS (Chemical class), *HISTONE deacetylase, *DIET therapy, *ALLODYNIA, *CHEMICAL inhibitors

Abstract

Background: Alcohol withdrawal‐induced hyperalgesia (AWH) is characterized as an increased pain sensitivity observed after cessation of chronic alcohol use. Alcohol withdrawal‐induced hyperalgesia can contribute to the negative affective state associated with abstinence and can increase susceptibility to relapse. We aimed to characterize pain sensitivity in mice during withdrawal from two different models of alcohol exposure: chronic drinking in the dark (DID) and the Lieber–DeCarli liquid diet. We also investigated whether treatment with a histone deacetylase (HDAC) inhibitor, suberoylanilide hydroxamic acid (SAHA), could ameliorate AWH in mice treated with the Lieber–DeCarli diet. Methods: Male and female C57BL/6J mice were used for these studies. In the DID model, mice received bottles of 20% ethanol or water during the dark cycle for 4 h per day on four consecutive days per week for 6 weeks. Peripheral mechanical sensitivity was measured weekly the morning of Day 5 using von Frey filaments. In the Lieber–DeCarli model, mice received ethanol (5% v/v) or control liquid diet for 10 days, along with a single binge ethanol gavage (5 g/kg) or control gavage, respectively, on Day 10. Peripheral mechanical sensitivity was measured during the liquid diet administration and at 24 and 72 h into ethanol withdrawal. An independent group of mice that received the Lieber–DeCarli diet were administered SAHA (50 mg/kg, i.p.) during withdrawal. Results: Male mice exhibited mechanical hypersensitivity after consuming ethanol for 5 weeks in the DID procedure. In the Lieber–DeCarli model, ethanol withdrawal led to hyperalgesia in both sexes. Suberoylanilide hydroxamic acid treatment during withdrawal from the ethanol liquid diet alleviated AWH. Conclusions: These results demonstrate AWH in mice after chronic binge drinking in males and after Lieber–DeCarli liquid diet administration in both sexes. Like previous findings in rats, HDAC inhibition reduced AWH in mice, suggesting that epigenetic mechanisms are involved in AWH. [ABSTRACT FROM AUTHOR]

Published

2024