Your search keyword '"ANTI-inflammatory agents"' showing total 798 results

1. High‐Content Image‐Based Screening and Deep Learning for the Detection of Anti‐Inflammatory Drug Leads

Author

Lau, Tannia A, Lau, Tannia A, Mair, Elmar, Rabbitts, Beverley M, Lohith, Akshar, Lokey, R Scott, Lau, Tannia A, Lau, Tannia A, Mair, Elmar, Rabbitts, Beverley M, Lohith, Akshar, and Lokey, R Scott

Abstract

We developed a high-content image-based screen that utilizes the pro-inflammatory stimulus lipopolysaccharide (LPS) and murine macrophages (RAW264.7) with the goal of enabling the identification of novel anti-inflammatory lead compounds. We screened 2,259 bioactive compounds with annotated mechanisms of action (MOA) to identify compounds that block the LPS-induced phenotype in macrophages. We utilized a set of seven fluorescence microscopy probes to generate images that were used to train and optimize a deep neural network classifier to distinguish between unstimulated and LPS-stimulated macrophages. The top hits from the deep learning classifier were validated using a linear classifier trained on individual cells and subsequently investigated in a multiplexed cytokine secretion assay. All 12 hits significantly modulated the expression of at least one cytokine upon LPS stimulation. Seven of these were allosteric inhibitors of the mitogen-activated protein kinase kinase (MEK1/2) and showed similar effects on cytokine expression. This deep learning morphological assay identified compounds that modulate the innate immune response to LPS and may aid in identifying new anti-inflammatory drug leads.

Published

2024

2. Maintenance of Investigators Static Global Assessment Response with Once-Daily Crisaborole in Participants with Mild to Moderate Atopic Dermatitis.

Author

Eichenfield, Lawrence, Eichenfield, Lawrence, Stein Gold, Linda, Lynde, Charles, Guenther, Lyn, Greenberger, Shoshana, Chu, Chia-Yu, Ghodsi, Zara, Vlahos, Bonnie, Sanders, Paul, Cha, Amy, Canosa, Juliana, Eichenfield, Lawrence, Eichenfield, Lawrence, Stein Gold, Linda, Lynde, Charles, Guenther, Lyn, Greenberger, Shoshana, Chu, Chia-Yu, Ghodsi, Zara, Vlahos, Bonnie, Sanders, Paul, Cha, Amy, and Canosa, Juliana

Abstract

INTRODUCTION: Treatments for atopic dermatitis (AD) often fail to achieve lasting disease control. In the CrisADe CONTROL phase III study (ClinicalTrials.gov: NCT04040192), participants aged ≥ 3 months with mild to moderate AD treated with once-daily (QD) crisaborole, following initial treatment success with crisaborole twice daily (BID), had longer periods of flare-free maintenance, a higher number of flare-free days, and a lower number of flares compared with those who received vehicle. The study was an exploratory analysis of data on the maintenance of response per Investigators Static Global Assessment (ISGA; ISGA score of 0 [clear] or 1 [almost clear]) during the CrisADe CONTROL study through week 52. METHODS: Exploratory endpoints were the time to ISGA response during the open-label run-in period, and the maintenance of ISGA response and the severity and duration of flares during the double-blind maintenance period. Outcomes were stratified by age (participants aged 3 months to < 12 years and ≥ 12 years) and duration of crisaborole BID treatment (< 4 weeks or ≥ 4 weeks) during the open-label run-in period. RESULTS: During the open-label run-in period, the median time to ISGA response was 41.5 days. From week 4 to week 52 of the double-blind maintenance period, the proportion of participants who maintained ISGA response was greater with crisaborole versus vehicle, and this difference was statistically significant up to week 36 (P < 0.05). Duration of flare periods during the maintenance period were 54.1 and 54.0 days for the vehicle and crisaborole-treated groups, respectively. Numerically fewer crisaborole-treated participants experienced a flare with an ISGA score of ≥ 2 compared with vehicle-treated participants (64.8% vs. 74.4%, respectively). Findings were comparable across most subgroups. CONCLUSIONS: Adult and pediatric participants with mild to moderate AD at baseline who had achieved responder criteria (

Published

2024

3. Cardiovascular/anti-inflammatory drugs repurposed for treating or preventing cancer: A systematic review and meta-analysis of randomized trials.

Author

Benjamin, David, Benjamin, David, Haslam, Alyson, Prasad, Vinay, Benjamin, David, Benjamin, David, Haslam, Alyson, and Prasad, Vinay

Abstract

BACKGROUND: Due to encouraging pre-clinical data and supportive observational studies, there has been growing interest in applying cardiovascular drugs (including aspirin, angiotensin-converting enzyme [ACE] inhibitors, statins, and metformin) approved to treat diseases such as hypertension, hyperlipidemia, and diabetes mellitus to the field of oncology. Moreover, given growing costs with cancer care, these medications have offered a potentially more affordable avenue to treat or prevent recurrence of cancer. We sought to investigate the anti-cancer effects of drugs repurposed from cardiology or anti-inflammatories to treat cancer. We specifically evaluated the following drug classes: HMG-CoA reductase inhibitors (statins), cyclo-oxygenase inhibitors, aspirin, metformin, and both angiotensin receptor blockers (ARBs) and angiotensin-converting enzyme inhibitors. We also included non-steroidal anti-inflammatory drugs (NSAIDs) because they exert a similar mechanism to aspirin by blocking prostaglandins and reducing inflammation that is thought to promote the development of cancer. METHODS: We performed a systematic literature review using PubMed and Web of Science with search terms including aspirin, NSAID, statin (including specific statin drug names), metformin, ACE inhibitors, and ARBs (including specific anti-hypertensive drug names) in combination with cancer. Searches were limited to human studies published between 2000 and 2023. MAIN OUTCOMES AND MEASURES: The number and percentage of studies reported positive results and pooled estimates of overall survival, progression-free survival, response, and disease-free survival. RESULTS: We reviewed 3094 titles and included 67 randomized clinical trials. The most common drugs that were tested were metformin (n = 21; 30.9%), celecoxib (n = 20; 29.4%), and simvastatin (n = 8; 11.8%). There was only one study that tested cardiac glycosides and none that studied ACE inhibitors. The most common tumor types were non-small-ce

Published

2024

4. Sustained Focal Vascular Inflammation Accelerates Atherosclerosis in Remote Arteries

Author

Lavín Plaza, Begoña, Phinikaridou, Alkystis, Andia, Marcelo E., Potter, Myles, Lorrio, Silvia, Rashid, Imran, Botnar, Rene M., Lavín Plaza, Begoña, Phinikaridou, Alkystis, Andia, Marcelo E., Potter, Myles, Lorrio, Silvia, Rashid, Imran, and Botnar, Rene M.

Abstract

OBJECTIVE: Evidence from preclinical and clinical studies has demonstrated that myocardial infarction promotes atherosclerosis progression. The impact of focal vascular inflammation on the progression and phenotype of remote atherosclerosis remains unknown. APPROACH AND RESULTS: We used a novel ApoE−/− knockout mouse model of sustained arterial inflammation, initiated by mechanical injury in the abdominal aorta. Using serial in vivo molecular MRI and ex vivo histology and flow cytometry, we demonstrate that focal arterial inflammation triggered by aortic injury, accelerates atherosclerosis in the remote brachiocephalic artery. The brachiocephalic artery atheroma had distinct histological features including increased plaque size, plaque permeability, necrotic core to collagen ratio, infiltration of more inflammatory monocyte subsets, and reduced collagen content. We also found that arterial inflammation following focal vascular injury evoked a prolonged systemic inflammatory response manifested as a persistent increase in serum IL-6 (interleukin 6). Finally, we demonstrate that 2 therapeutic interventions—pravastatin and minocycline—had distinct anti-inflammatory effects at the plaque and systemic level. CONCLUSIONS: We show for the first time that focal arterial inflammation in response to vascular injury enhances systemic vascular inflammation, accelerates remote atheroma progression and induces plaques more inflamed, lipid-rich, and collagenpoor in the absence of ischemic myocardial injury. This inflammatory cascade is modulated by pravastatin and minocycline treatments, which have anti-inflammatory effects at both plaque and systemic levels that mitigate atheroma progression., Engineering and Physical Sciences Research Council (EPSRC), British Heart Foundation (BHF), King’s BHF Centre for Research Excellence, EPSRC Centre for Medical Engineering, Depto. de Bioquímica y Biología Molecular, Fac. de Ciencias Químicas, TRUE, pub

Published

2024

5. Isolation and characterisation of hTNF-alpha neutralising VNARs from an immunised nurse shark, Ginglymostoma cirratum, using phage display

Author

Ubah, Obinna Chukwuemeka

Subjects

616.07, Ginglymostoma, Monoclonal antibodies, Anti-inflammatory agents

Abstract

TNF-α is a pleiotropic cytokine with an established role in the pathogenesis of immune-mediated inflammatory diseases, such as rheumatoid arthritis (RA), inflammatory bowel disease (IBD), psoriasis and non-infective uveitis. Anti-TNF-α monoclonal antibodies continue to demonstrate clinical efficacy in the management of some of these inflammatory conditions. However there are limitations associated with these commercially available monoclonal antibodies, and they include but are not limited to their large molecular size, safety profile and affordability. As a result of these limitations, there has been efforts to reduce the size of the antigen-binding fragment via antibody engineering. Interestingly, nature has already provided two reductionist solutions as the serum of camelids and cartilaginous fish possess antibody-like molecules of heavy chain-only homodimeric immunoglobulins. Their antigen binding regions are formed by an independent single variable domain referred to as the VHH in camelid and VNAR in sharks. Here we demonstrated the isolation of high affinity, and specific TNF-α binding VNAR domains through the immunisation of nurse shark, Ginglymostoma cirratum, and antigen-driven selection of anti-TNF-α VNAR phage display library. These isolated lead VNAR domains neutralised TNF-α mediated cytotoxicity in actinomycin-D treated L929 cells. These IgNAR V regions allow multiple reformatting and molecular fusion because of their single chain molecular architecture. As a result of this unique advantage, we were able to construct multivalent anti-TNF-α VNARs, and demonstrated significantly improved functional affinity to hTNF-α, and enhanced in vitro efficacy in cell based models of hTNF-α induced cytotoxicity and intestinal epithelial barrier dysfunctions. These multivalent domains showed no compromise in stability compared to their stable parent monomeric domains. Together these demonstrated characteristics of the isolated anti-hTNF-α IgNAR V region constructs suggest the development of lead domains with real potential for site-delivered efficacy in inflammatory disease.

Published

2016

6. Inflammatory biomarkers of colorectal neoplasia and their manipulation by an anti-inflammatory diet

Author

Basavaraju, Umesh

Subjects

616.99434, Colon (Anatomy), Rectum, Biochemical markers, Anti-inflammatory agents

Abstract

Colorectal neoplasia (CRN) continues to be a leading cause of morbidity and mortality in the developed world and with westernisation, similar trends are now emerging in the developing world. Although secondary prevention through screening programmes has reduced mortality, uptake remains poor due to the invasive nature of colonoscopy, which also exerts increased costs to the health care system. Primary prevention remains the ultimate aim to reduce the morbidity and mortality associated with CRN. In this regard, chemoprevention strategies through regular use of aspirin and other NSAIDS have showed great promise but the associated significant side-effects of these drugs has prevented their routine clinical application for this purpose. Hence there is an urgent need for the identification of safer alternatives for primary prevention of CRN. In parallel to this search, better understanding of the molecular pathogenesis of CRN to identify biomarkers that aid in stratification of at risk individuals would also help. In this regard, the role of chronic inflammation and the influence of host genetics in the pathogenesis of CRN has been the focus of extensive research in recent years. However there is a lack of studies which have investigated these associations in an exclusively screened population, which confers some advantages for this type of investigation. Firstly, most of the screened subjects are relatively healthy, asymptomatic and with no significant co-morbidities, the factors which could otherwise influence the levels of inflammatory markers. Secondly, the screened population is in the 50 to74 year age group which represents the group with a high prevalence of CRN and hence increasing the possibility of finding associations which would be more relevant and generalisable. Thirdly, the selected controls match the cases in all important respects, apart from having CRN, thus increasing the validity of the findings in this population. The Grampian region was one of the first in the UK to participate in the National Colorectal Cancer Screening Programme and this resource gave the ideal opportunity to conduct research involving an exclusively screened population. Utilising this cohort, the current thesis addressed three important aspects of the association between inflammation and CRN. Firstly the investigation of the association of inflammatory genotype, inflammatory phenotype and CRN risk. Secondly the impact of environmental factors, specifically dietary antiinflammatory salicylic acid intakes on CRN risk. And finally assessing if inflammation, and hence in the long term risk of CRN, could be attenuated through a comprehensive anti-inflammatory dietary supplementation in the form of a randomised dietary intervention clinical trial. The study of the association of polymorphisms in key inflammatory genes (IL1B- 31, IL8-251, IL6-174, TNFα-308, IL10-1082, IL10-592, PTGS2-765, and IL1RN VNTR) and CRN risk showed some significant findings. A novel finding was that the homozygous IL1B-31C*C genotype was associated with statistically significant increased risk of CRN, OR 1.63 (95% CI 1.06-2.50) whilst the IL8-251 A*A genotype increased the propensity of having high risk lesions by two-fold (OR 2.04; 95% CI 1.02-4.07). The study of circulating inflammatory marker levels in subjects in whom the CRN was in-situ showed that increased CRP levels were associated with increased risk of CRN, OR 1.55 (95% CI 1.00-2.39). Increased levels of IL8 were associated with increased risk of having a high risk lesion, OR 2.57 (95% CI 1.03-6.44). In a sub group of subjects, it was observed that levels IL8 and CRP decreased following polypectomy (mean IL8 20.3 pg/ml to 14.9 pg/ml, p=0.05 and mean CRP 5.99 mg/l to 3.82 mg/l, p=0.07) raising an important question regarding the sequence of the inflammation-neoplasia cascade, “Is inflammation the cause or the effect of neoplasia?” The study of the association of dietary salicylic acid (SA) and CRN using the newly constructed SA database showed that high levels of total SA (aspirin and dietary SA) intakes were associated with a 75% and moderate levels with a 67% decreased risk of CRN. But dietary SA on its own showed no significant effect on CRN risk probably because of low intake levels in the current cohort. Applying the SA database to populations with higher dietary SA intake would help to further explore its association with CRN risk. The randomised clinical trial examining the effect of a combined antiinflammatory dietary supplement (curcumin, omega-3 PUFA and polyphenols rich fruit smoothie) on markers of inflammation in subjects who had adenomatous colorectal polyps removed showed that the inflammatory marker levels in the control group who just continued their habitual diet remained stable without any statistically significant changes at 6 weeks compared to the baseline. Whereas following 6 weeks of dietary intervention, there was marginally significant increase in IL8 and IL1B levels. One of the possible mechanisms for increase in pro-inflammatory marker levels in the intervention group was the weight gain seen in the intervention group. In the intervention group, the post-intervention mean weight (86.80kgs) was significantly higher than the pre-intervention mean weight (85.38 kgs). In summary, the findings from these investigations suggest that a proinflammatory genotype (IL1B-31C*C and IL8-251 A*A) and elevated circulating inflammatory marker levels (CRP and IL8) are associated with increased risk of CRN. And along with the findings that regular NSAID use and total dietary SA are associated with decreased risk of CRN, our data point to inflammation as an underlying pathogenetic mechanism in CRN. The pilot clinical trial has demonstrated that a clinical trial with combined dietary supplementation is feasible, but challenging. The anti-inflammatory dietary intervention strategy employed to reduce the inflammatory markers did not achieve the desired effect and hence more research is required to establish the ideal delivery strategy of the anti-inflammatory dietary agents. Once this is established, dietary chemoprevention of CRN as a safe alternative should be a realistic achievable goal in the future.

Published

2011

7. A Pharmacokinetic and Analgesic Efficacy Study of Carprofen in Female CD1 Mice.

Author

McKenna, Brandon, McKenna, Brandon, Weaver, Hannah, Kim, Jeffrey, Bowman, Madelyn, Kendall, Lon, Knych, Heather, McKenna, Brandon, McKenna, Brandon, Weaver, Hannah, Kim, Jeffrey, Bowman, Madelyn, Kendall, Lon, and Knych, Heather

Abstract

The minimization of pain in research animals is a scientific and ethical necessity. Carprofen is commonly used for pain management in mice; however, some data suggest that the standard dosage of 5 mg/kg may not provide adequate analgesia after surgery. We hypothesized that a higher dose of carprofen in mice would reduce pain-associated behaviors and improve analgesia without toxic effects. A pharmacokinetic study was performed in mice given carprofen subcutaneously at 10 or 20 mg/kg. Plasma concentrations were measured at 0.25, 0.5, 1, 2, 4, 8, 12, 24, and 48 h after dosing (n = 3 per time point and treatment). At these doses, plasma levels were above the purported therapeutic level for at least 12 and 24 h, respectively, with respective half-lives of 14.9 and 10.2 h. For the efficacy study, 10 mice per group received anesthesia with or without an ovariectomy. Mice were then given 5 or 10 mg/kg of carprofen, or saline subcutaneously every 12 h. Orbital tightening, arched posture, wound licking, rearing, grooming, nesting behavior, and activity were assessed before surgery and at 4, 8, 12, 24, and 48 h after surgery. The von Frey responses were assessed before and at 4, 12, 24, and 48 h after surgery. The efficacy study showed that all surgery groups had significantly higher scores for orbital tightening, arched posture, and wound licking than did the anesthesia-only groups at 4, 8, 12, and 24-h time points. At the 8 h time point, the surgery groups treated with carprofen had significantly lower arched posture scores than did the surgery group treated with saline only. No significant differences were found between carprofen treatment groups for rearing, grooming, von Frey, activity, or nesting behavior at any time point. These results indicate that subcutaneous carprofen administered at these doses does not provide sufficient analgesia to alleviate postoperative pain in female CD1 mice.

Published

2023

8. A behavioral intervention to promote use of multimodal pain medication for hospitalized patients: A randomized controlled trial.

Author

Bongiovanni, Tasce, Bongiovanni, Tasce, Pletcher, Mark, Lau, Catherine, Robinson, Andrew, Lancaster, Elizabeth, Zhang, Li, Behrends, Matthias, Wick, Elizabeth, Auerbach, Andrew, Bongiovanni, Tasce, Bongiovanni, Tasce, Pletcher, Mark, Lau, Catherine, Robinson, Andrew, Lancaster, Elizabeth, Zhang, Li, Behrends, Matthias, Wick, Elizabeth, and Auerbach, Andrew

Abstract

BACKGROUND: The use of nonsteroidal anti-inflammatory drugs (NSAIDs) can reduce pain and has become a core strategy to decrease opioid use, but there is a lack of data to describe encouraging use when admitting patients using electronic health record systems. OBJECTIVE: Assess an electronic health record system to increase ordering of NSAIDs for hospitalized adults. DESIGNS, SETTINGS AND PARTICIPANTS: We performed a cluster randomized controlled trial of clinicians admitting adult patients to a health system over a 9-month period. Clinicians were randomized to use a standard admission order set. INTERVENTION: Clinicians in the intervention arm were required to actively order or decline NSAIDs; the control arm was shown the same order but without a required response. MAIN OUTCOME AND MEASURES: The primary outcome was NSAIDs ordered and administered by the first full hospital day. Secondary outcomes included pain scores and opioid prescribing. RESULTS: A total of 20,085 hospitalizations were included. Among these hospitalizations, patients had a mean age of 58 years, and a Charlson comorbidity score of 2.97, while 50% and 56% were female and White, respectively. Overall, 52% were admitted by a clinician randomized to the intervention arm. NSAIDs were ordered in 2267 (22%) interventions and 2093 (22%) control admissions (p = .10). Similarly, there were no statistical differences in NSAID administration, pain scores, or opioid prescribing. Average pain scores (0-5 scale) were 3.36 in the control group and 3.39 in the intervention group (p = .46). There were no differences in clinical harms. CONCLUSIONS AND RELEVANCE: Requiring an active decision to order an NSAID at admission had no demonstrable impact on NSAID ordering. Multicomponent interventions, perhaps with stronger decision support, may be necessary to encourage NSAID ordering.

Published

2023

9. Chronic Diclofenac Exposure Increases Mitochondrial Oxidative Stress, Inflammatory Mediators, and Cardiac Dysfunction.

Author

Thai, Phung N, Thai, Phung N, Ren, Lu, Xu, Wilson, Overton, James, Timofeyev, Valeriy, Nader, Carol E, Haddad, Michael, Yang, Jun, Gomes, Aldrin V, Hammock, Bruce D, Chiamvimonvat, Nipavan, Sirish, Padmini, Thai, Phung N, Thai, Phung N, Ren, Lu, Xu, Wilson, Overton, James, Timofeyev, Valeriy, Nader, Carol E, Haddad, Michael, Yang, Jun, Gomes, Aldrin V, Hammock, Bruce D, Chiamvimonvat, Nipavan, and Sirish, Padmini

Abstract

PurposeNonsteroidal anti-inflammatory drugs (NSAIDs) are among one of the most commonly prescribed medications for pain and inflammation. Diclofenac (DIC) is a commonly prescribed NSAID that is known to increase the risk of cardiovascular diseases. However, the mechanisms underlying its cardiotoxic effects remain largely unknown. In this study, we tested the hypothesis that chronic exposure to DIC increases oxidative stress, which ultimately impairs cardiovascular function.Methods and resultsMice were treated with DIC for 4 weeks and subsequently subjected to in vivo and in vitro functional assessments. Chronic DIC exposure resulted in not only systolic but also diastolic dysfunction. DIC treatment, however, did not alter blood pressure or electrocardiographic recordings. Importantly, treatment with DIC significantly increased inflammatory cytokines and chemokines as well as cardiac fibroblast activation and proliferation. There was increased reactive oxygen species (ROS) production in cardiomyocytes from DIC-treated mice, which may contribute to the more depolarized mitochondrial membrane potential and reduced energy production, leading to a significant decrease in sarcoplasmic reticulum (SR) Ca2+ load, Ca2+ transients, and sarcomere shortening. Using unbiased metabolomic analyses, we demonstrated significant alterations in oxylipin profiles towards inflammatory features in chronic DIC treatment.ConclusionsTogether, chronic treatment with DIC resulted in severe cardiotoxicity, which was mediated, in part, by an increase in mitochondrial oxidative stress.

Published

2023

10. Results and insights from a phase I clinical trial of Lomecel-B for Alzheimer's disease.

Author

Brody, Mark, Brody, Mark, Agronin, Marc, Herskowitz, Brad J, Bookheimer, Susan Y, Small, Gary W, Hitchinson, Benjamin, Ramdas, Kevin, Wishard, Tyler, McInerney, Katalina Fernández, Vellas, Bruno, Sierra, Felipe, Jiang, Zhijie, Mcclain-Moss, Lisa, Perez, Carmen, Fuquay, Ana, Rodriguez, Savannah, Hare, Joshua M, Oliva, Anthony A, Baumel, Bernard, Brody, Mark, Brody, Mark, Agronin, Marc, Herskowitz, Brad J, Bookheimer, Susan Y, Small, Gary W, Hitchinson, Benjamin, Ramdas, Kevin, Wishard, Tyler, McInerney, Katalina Fernández, Vellas, Bruno, Sierra, Felipe, Jiang, Zhijie, Mcclain-Moss, Lisa, Perez, Carmen, Fuquay, Ana, Rodriguez, Savannah, Hare, Joshua M, Oliva, Anthony A, and Baumel, Bernard

Abstract

HypothesisWe hypothesized that Lomecel-B, an allogeneic medicinal signaling cell (MSC) therapeutic candidate for Alzheimer's disease (AD), is safe and potentially disease-modifying via pleiotropic mechanisms of action.Key predictionsWe prospectively tested the predictions that Lomecel-B administration to mild AD patients is safe (primary endpoint) and would provide multiple exploratory indications of potential efficacy in clinical and biomarker domains (prespecified secondary/exploratory endpoints).Strategy and key resultsMild AD patient received a single infusion of low- or high-dose Lomecel-B, or placebo, in a double-blind, randomized, phase I trial. The primary safety endpoint was met. Fluid-based and imaging biomarkers indicated significant improvement in the Lomecel-B arms versus placebo. The low-dose Lomecel-B arm showed significant improvements versus placebo on neurocognitive and other assessments.InterpretationOur results support the safety of Lomecel-B for AD, suggest clinical potential, and provide mechanistic insights. This early-stage study provides important exploratory information for larger efficacy-powered clinical trials.

Published

2023

11. High-dose Meloxicam Provides Improved Analgesia in Female CD1 Mice: A Pharmacokinetic and Efficacy Study.

Author

Kim, Jeffrey, Kim, Jeffrey, Cannon, Brinley A, Freeman, Layne E, Tan, Sarah, Knych, Heather K, Kendall, Lon V, Kim, Jeffrey, Kim, Jeffrey, Cannon, Brinley A, Freeman, Layne E, Tan, Sarah, Knych, Heather K, and Kendall, Lon V

Abstract

Meloxicam is a nonsteroidal anti-inflammatory analgesic drug that is often used in mice. However, doses of 1 to 5 mg/kg given twice daily were recently reported to provide inadequate analgesia. Some studies suggest that doses of up to 20 mg/kg may be necessary for adequate pain management. We investigated the analgesia provided by a high-dose of meloxicam in female CD1 mice. Pharmacokinetic analyses demonstrated that a subcutaneous injection of 10 mg/kg or 20 mg/kg of meloxicam produced therapeutic plasma concentrations for at least 12 h. Ovariectomies via ventral laparotomy were performed to assess analgesic efficacy. Mice were treated immediately before surgery with a high-dose of 10 mg/kg, a low-dose of 2.5 mg/kg, or saline, followed by every 12 h for 36 h. At 3, 6, 12, 24, and 48 h after surgery, mice were assessed for pain based on the following behaviors: distance traveled, time mobile, grooming, rearing, hunched posture, orbital tightening, and von Frey. Initially, some mice received a 20-mg/kg loading dose followed by 10 mg/kg every 12 h. This regimen caused severe morbidity and mortality in 2 mice. Subsequently, this regimen was abandoned, and mice assigned to the high-dose group received 10 mg/kg every 12 h. Mice that received the 10-mg/kg dose after surgery showed less orbital tightening between 3 to 6 h and reduced frequency of hunched posture for 48 h compared with mice that received either the low-dose or saline. However, mice were significantly less mobile for 6 to 12 h after surgery regardless of treatment. These data indicate that a meloxicam dose of 10 mg/kg every 12 h provides better analgesia than a 2.5-mg/kg dose but does not completely alleviate pain.

Published

2023

12. Clinical and endoscopic remission in patients with inflamatory bowel disease using aminosalicilates, systemic corticoesteroids and immunomodulators

Author

García, María, Armanie, Emma, García, María, and Armanie, Emma

Abstract

A cross-sectional transversal research was conducted with the aim of determining clinical and endoscopic remission of inflammatory bowel disease (IBD) with the use of aminosalicylates, systemic corticosteroids and immunomodulators in patients attended at the Servicio de Gastroenterologia of the Hospital Central Universitario Dr. Antonio María Pineda, Barquisimeto, Lara state, during the period 2012-2020, using the Montreal, Mayo, CDEIS, Harvey-Bradshaw and Harvey-Bradshaw indices. The population consisted of 87 records from the clinical histories of patients who met the established criteria. The prevalence age was between 41 and 62 years; 65.5% were females. 44.9% of patients with ulcerative colitis (UC) showed left colitis and 34.6% pancolitis. In Crohn’s disease (CD), 88.9% of patients showed an inflammatory pattern. Clinical activity of UC at diagnosis was mild (47.7%) and moderate (44.9%). After induction, 87% of patients who did not achieve clinical remission were found to have mild activity. In CD at diagnosis, mild clinical activity prevailed (77.8%). Endoscopic activity at UC diagnosis was moderate (56.4%) and severe (32.1%) and at control colonoscopy during maintenance therapy, the percentage of patients in mild/ moderate activity was 40% in both groups. In UC, prednisone (47.4%) or mesalazine (24.3%) was used for induction and for maintenance, azathioprine + mesalazine or sulfasalazine (35.9% and 25.6%), respectively. In CD, prednisone (88.9%) was used for induction and for maintenance, aminosalicylates (77.8%) and aminosalicylates + azathioprine (22.2). In UC, 70.5% presented clinical remission and 29.5% endoscopic remission. In CD, 88.9% showed clinical remission and 33.3% endoscopic remission., Se realizó una investigación descriptiva transversal con el objetivo de determinar la remisión clínica y endoscópica de la enfermedad inflamatoria intestinal (EII) con el uso de aminosalicilatos, corticoides sistémicos e inmunomoduladores en pacientes atendidos en el Servicio de Gastroenterología del Hospital Central Universitario Dr. Antonio María Pineda de Barquisimeto, estado Lara, durante el período 2012-2020 usando los índices de Montreal, Mayo, CDEIS y Harvey-Bradshaw. La población estuvo conformada por 87 registros de historias clínicas de pacientes que cumplieron con los criterios establecidos. La edad de prevalencia fue entre 41 y 62 años; 65.5% del sexo femenino. 44.9% de pacientes con colitis ulcerosa (CU) presentaban colitis izquierda y 34.6% pancolitis. En enfermedad de Crohn (EC), 88.9% de los pacientes presentó patrón inflamatorio. La actividad clínica de la CU al diagnóstico fue leve (47.7%) y moderada (44.9%). Después de la inducción, 87% de pacientes que no lograron remisión clínica se encontraron en actividad leve. Al momento del diagnóstico de la EC, prevaleció la actividad clínica leve (77.8%). La actividad endoscópica en el diagnóstico de CU fue moderada (56.4%) y severa (32.1%) y en la colonoscopia control durante la terapia de mantenimiento, el porcentaje de pacientes en actividad leve y moderada fue de 40% en ambos grupos. En CU, se utilizó prednisona (47.4%) o mesalazina (24.3%) para inducción y mantenimiento, azatioprina más mesalazina o sulfasalazina (35.9% y 25.6%), respectivamente. En EC, se utilizó prednisona (88.9%) para inducción y para mantenimiento, aminosalicilatos (77.8%) y aminosalicilatos más azatioprina (22.2). En CU, 70.5% presentó remisión clínica y 29.5% remisión endoscópica. En EC, el 88.9% presentó remisión clínica y 33.3% endoscópica.

Published

2023

13. Modeling Early Heterogeneous Rates of Progression in Boys with Duchenne Muscular Dystrophy.

Author

Fang, Yuan, Fang, Yuan, Clemens, Paula, Gordish, Heather-Dressman, Illei, Kate, Hoffman, Eric, Dang, Utkarsh, McDonald, Craig, Fang, Yuan, Fang, Yuan, Clemens, Paula, Gordish, Heather-Dressman, Illei, Kate, Hoffman, Eric, Dang, Utkarsh, and McDonald, Craig

Abstract

BACKGROUND: Duchenne muscular dystrophy (DMD) exhibits substantial variability in rates of disease progression and response to treatment. This has hindered treatment development and complicated interpretation of drug effects in clinical trials. OBJECTIVE: We hypothesized that a multivariate combination of early-age clinical outcome measurements can explain differential disease progression. METHODS: Data on boys with DMD (ages 4-<10 years), both treated with steroidal anti-inflammatories and untreated, were obtained from CINRG Duchenne Natural History Study (n = 209) and vamorolone VBP15-002/003/LTE (n = 46) studies. Velocities from three timed function tests (TFTs; stand from supine, run/walk 10 meters, and climb 4 stairs) were simultaneously modeled in a longitudinal latent class analysis. RESULTS: Three classes of differentially progressing early age DMD motor trajectories were identified. Quicker decline/progression was associated with lower baseline TFT velocities, earlier loss of ability to finish a TFT, and lower predicted velocities. Earlier substantial steroid exposure was associated with greater TFT velocities while the moderate progression class was observed to have the largest difference in performance between boys treated early with steroids vs. not. Sample size calculations with the class showing the largest treatment response showed a large reduction in required sample size as compared to using summaries from all participants. Gene mutations were also investigated in post-hoc analyses, with mutations near the beginning of the DMD gene (Dp427 absent and Dp140/Dp71 present) found to be enriched in the slowest progressing class. CONCLUSIONS: This study provides insight into the variation in DMD progression through a latent class analysis. Our findings show class-related trajectories of motor outcomes and pharmacological response to corticosteroids, and suggest that enrichment strategies and/or subgroup analyses could be considered further in design of

Published

2023

14. Current Medical Therapy and Revascularization in Peripheral Artery Disease of the Lower Limbs: Impacts on Subclinical Chronic Inflammation

Author

Cecchini, Andrea Leonardo, Biscetti, Federico, Manzato, Matteo, Lo Sasso, Lorenzo, Rando, Maria Margherita, Nicolazzi, Maria Anna, Rossini, Enrica, Eraso, Luis, DiMuzio, Paul, Massetti, Massimo, Gasbarrini, Antonio, Flex, Andrea, Cecchini, Andrea Leonardo, Biscetti, Federico, Manzato, Matteo, Lo Sasso, Lorenzo, Rando, Maria Margherita, Nicolazzi, Maria Anna, Rossini, Enrica, Eraso, Luis, DiMuzio, Paul, Massetti, Massimo, Gasbarrini, Antonio, and Flex, Andrea

Abstract

Peripheral artery disease (PAD), coronary artery disease (CAD), and cerebrovascular disease (CeVD) are characterized by atherosclerosis and inflammation as their underlying mechanisms. This paper aims to conduct a literature review on pharmacotherapy for PAD, specifically focusing on how different drug classes target pro-inflammatory pathways. The goal is to enhance the choice of therapeutic plans by considering their impact on the chronic subclinical inflammation that is associated with PAD development and progression. We conducted a comprehensive review of currently published original articles, narratives, systematic reviews, and meta-analyses. The aim was to explore the relationship between PAD and inflammation and evaluate the influence of current pharmacological and nonpharmacological interventions on the underlying chronic subclinical inflammation. Our findings indicate that the existing treatments have added anti-inflammatory properties that can potentially delay or prevent PAD progression and improve outcomes, independent of their effects on traditional risk factors. Although inflammation-targeted therapy in PAD shows promising potential, its benefits have not been definitively proven yet. However, it is crucial not to overlook the pleiotropic properties of the currently available treatments, as they may provide valuable insights for therapeutic strategies. Further studies focusing on the anti-inflammatory and immunomodulatory effects of these treatments could enhance our understanding of the mechanisms contributing to the residual risk in PAD and pave the way for the development of novel therapies.

Published

2023

15. The role of interleukin-4 and interleukin-13 in the prevention of cartilage breakdown

Author

Cleaver, Catherine Sarah

Subjects

610, Arthritis, Anti-inflammatory agents

Published

2000

16. The development of natural murine osteoarthritis : a quantitative cytochemical study

Author

Chambers, Mark Geoffrey

Subjects

610, Anti-inflammatory agents

Published

1991

17. Aspirin's effect on kinetic parameters of cells contributes to its role in reducing incidence of advanced colorectal adenomas, shown by a multiscale computational study.

Author

Wang, Yifan, Wang, Yifan, Boland, C Richard, Goel, Ajay, Wodarz, Dominik, Komarova, Natalia L, Wang, Yifan, Wang, Yifan, Boland, C Richard, Goel, Ajay, Wodarz, Dominik, and Komarova, Natalia L

Abstract

Aspirin intake has been shown to lead to significant protection against colorectal cancer, for example with an up to twofold reduction in colorectal adenoma incidence rates at higher doses. The mechanisms contributing to protection are not yet fully understood. While aspirin is an anti-inflammatory drug and can thus influence the tumor microenvironment, in vitro and in vivo experiments have recently shown that aspirin can also have a direct effect on cellular kinetics and fitness. It reduces the rate of tumor cell division and increases the rate of cell death. The question arises whether such changes in cellular fitness are sufficient to significantly contribute to the epidemiologically observed protection. To investigate this, we constructed a class of mathematical models of in vivo evolution of advanced adenomas, parameterized it with available estimates, and calculated population level incidence. Fitting the predictions to age incidence data revealed that only a model that included colonic crypt competition can account for the observed age-incidence curve. This model was then used to predict modified incidence patterns if cellular kinetics were altered as a result of aspirin treatment. We found that changes in cellular fitness that were within the experimentally observed ranges could reduce advanced adenoma incidence by a sufficient amount to account for age incidence data in aspirin-treated patient cohorts. While the mechanisms that contribute to the protective effect of aspirin are likely complex and multi-factorial, our study demonstrates that direct aspirin-induced changes of tumor cell fitness can significantly contribute to epidemiologically observed reduced incidence patterns.

Published

2022

18. Intra-articular Administration of Triamcinolone Acetonide in a Murine Cartilage Defect Model Reduces Inflammation but Inhibits Endogenous Cartilage Repair

Author

Wesdorp, Marinus A. (author), Capar, Serdar (author), Bastiaansen-Jenniskens, Yvonne M. (author), Kops, Nicole (author), Creemers, Laura B. (author), Verhaar, Jan A.N. (author), van Osch, G.J.V.M. (author), Wei, Wu (author), Wesdorp, Marinus A. (author), Capar, Serdar (author), Bastiaansen-Jenniskens, Yvonne M. (author), Kops, Nicole (author), Creemers, Laura B. (author), Verhaar, Jan A.N. (author), van Osch, G.J.V.M. (author), and Wei, Wu (author)

Abstract

Background: Cartilage defects result in joint inflammation. The presence of proinflammatory factors has been described to negatively affect cartilage formation. Purpose: To evaluate the effect and timing of administration of triamcinolone acetonide (TAA), an anti-inflammatory drug, on cartilage repair using a mouse model. Study Design: Controlled laboratory study. Methods: A full-thickness cartilage defect was created in the trochlear groove of 10-week-old male DBA/1 mice (N = 80). Mice received an intra-articular injection of TAA or saline on day 1 or 7 after induction of the defect. Mice were euthanized on days 10 and 28 for histological evaluation of cartilage defect repair, synovial inflammation, and synovial membrane thickness. Results: Mice injected with TAA had significantly less synovial inflammation at day 10 than saline-injected mice independent of the time of administration. At day 28, the levels of synovitis dropped toward healthy levels; nevertheless, the synovial membrane was thinner in TAA- than in saline-injected mice, reaching statistical significance in animals injected on day 1 (70.1 ± 31.9 µm vs 111.9 ± 30.9 µm, respectively; P =.01) but not in animals injected on day 7 (68.2 ± 21.86 µm vs 90.2 ± 21.29 µm, respectively; P =.26). A thinner synovial membrane was moderately associated with less filling of the defect after 10 and 28 days (r = 0.42, P =.02; r = 0.47, P =.01, respectively). Whereas 10 days after surgery there was no difference in the area of the defect filled and the cell density in the defect area between saline- and TAA-injected knees, filling of the defect at day 28 was lower in TAA- than in saline-injected knees for both injection time points (day 1 injection, P =.04; day 7 injection, P =.01). Moreover, there was less collagen type 2 staining in the filled defect area in TAA- than in saline-injected knees after 28 days, reaching statistical significance in day 1–injected knees (2.6% vs 18.5%, respectively; P =.01) but not in day, Biomaterials & Tissue Biomechanics

Published

2022

19. Methotrexate Inhibits T Cell Proliferation but Not Inflammatory Cytokine Expression to Modulate Immunity in People Living With HIV.

Author

Freeman, Michael L, Freeman, Michael L, Clagett, Brian M, Moisi, Daniela, Yeh, Eunice, Morris, Charles D, Ryu, Angela, Rodriguez, Benigno, Stein, James H, Deeks, Steven G, Currier, Judith S, Hsue, Priscilla Y, Anthony, Donald D, Calabrese, Leonard H, Ribaudo, Heather J, Lederman, Michael M, Freeman, Michael L, Freeman, Michael L, Clagett, Brian M, Moisi, Daniela, Yeh, Eunice, Morris, Charles D, Ryu, Angela, Rodriguez, Benigno, Stein, James H, Deeks, Steven G, Currier, Judith S, Hsue, Priscilla Y, Anthony, Donald D, Calabrese, Leonard H, Ribaudo, Heather J, and Lederman, Michael M

Abstract

Inflammation associated with increased risk of comorbidities persists in people living with HIV (PWH) on combination antiretroviral therapy (ART). A recent placebo-controlled trial of low-dose methotrexate (MTX) in PWH found that numbers of total CD4 and CD8 T cells decreased in the low-dose MTX arm. In this report we analyzed T cell phenotypes and additional plasma inflammatory indices in samples from the trial. We found that cycling (Ki67+) T cells lacking Bcl-2 were reduced by MTX but plasma inflammatory cytokines were largely unaffected. In a series of in vitro experiments to further investigate the mechanisms of MTX activity, we found that MTX did not inhibit effector cytokine production but inhibited T cell proliferation downstream of mTOR activation, mitochondrial function, and cell cycle entry. This inhibitory effect was reversible with folinic acid, suggesting low-dose MTX exerts anti-inflammatory effects in vivo in PWH largely by blocking T cell proliferation via dihydrofolate reductase inhibition, yet daily administration of folic acid did not rescue this effect in trial participants. Our findings identify the main mechanism of action of this widely used anti-inflammatory medicine in PWH and may provide insight into how MTX works in the setting of other inflammatory conditions.

Published

2022

20. A look at the current management of recurrent aphthous stomatitis

Author

Contreras Escobar, Jorge Andrés, Benítez Suárez, Patricia, Prieto Vélez, Lizette Paola, Orozco Páez, Jennifer, Contreras Escobar, Jorge Andrés, Benítez Suárez, Patricia, Prieto Vélez, Lizette Paola, and Orozco Páez, Jennifer

Abstract

Recurrent Aphthous Stomatitis (RAS) is an idiopathic chronic ulcerative pathology. Although it does not compromise the life of the patients, it can impair their quality of life. It presents a high incidence in the population and a high percentage of recurrence. In view of its importance, the aim of this review is to provide an update on pharmacological and laser therapies that are being implemented for the management of RAS. A bibliographic search of literature that was published between January 2010 and October 2020 was performed in PubMed, Science Direct, EBSCOhost, and LILACS databases, identifying publications in English and Spanish languages. The articles that were included had to be related to aphthous stomatitis and its treatment, focusing on pharmacological or laser management. 4536 bibliographic citations were found and 19 of them were included in this review. Most of the studies were randomized clinical trials in which the target population were adults that reported the use of anti-inflammatory drugs, immunomodulators, monoclonal antibodies, antiseptics, anesthetics, among others for the treatment of recurrent aphthous stomatitis. From the articles analyzed, it was possible to conclude that pharmacological therapy should be established in a particular way according to the patient's symptoms and medical record. The first-choice drugs are of topical use, reserving those of systemic use for moderate or severe cases and for patients with refractory treatment. Likewise, adjuvant recommendations such as nutrition and hygiene can help in the resolution of the disease. Laser therapy emerges as an alternative treatment with low risk and positive results for recurrent aphthous stomatitis., La estomatitis aftosa recurrente (EAR) es una patología ulcerativa crónica idiopática, que, aunque no llega a comprometer la vida de los pacientes, si puede desmejorar su calidad de vida. Presenta una alta incidencia en la población con un alto porcentaje de recurrencia. Atendiendo a su importancia, el objetivo de esta revisión es brindar una actualización respecto a las terapias farmacológicas y con láser para el manejo de la estomatitis aftosa recurrente. Se realizó una búsqueda bibliográfica en las bases de datos PubMed, Science Direct, EBSCO HOST y LILACS desde enero de 2010 a octubre de 2020, identificando publicaciones en inglés y español. Los artículos que fueron incluidos debían estar relacionadas con la estomatitis aftosa y su tratamiento, enfocándose en el manejo farmacológico o con láser. La estrategia de búsqueda arrojó 4536 citas bibliográficas, de las cuales fueron incluidas 19 en esta presente revisión. La mayoría de los estudios fueron ensayos clínicos aleatorizados donde la población objeto fueron adultos que demostraron el uso de antiinflamatorios, inmunomoduladores, anticuerpos monoclonales, antisépticos, anestésicos, entre otros, para el manejo de la estomatitis aftosa recurrente. De los artículos analizados se pudo concluir que la terapia farmacológica debe ser instaurada de manera particular, de acuerdo a la clínica y antecedentes del paciente. Los fármacos de primera elección son de uso tópico, reservando los de uso sistémico para casos moderados o severos y para pacientes con tratamiento refractarios, asimismo, las recomendaciones coadyuvantes como alimentación e higiene pueden ayudar a la resolución de la enfermedad. La terapia láser surge como alternativa de tratamiento con bajo riesgo y buenos resultados para la EAR.

Published

2022

21. NSAID use and clinical outcomes in COVID-19 patients: a 38-center retrospective cohort study.

Author

Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, Robinson, Peter N, Reese, Justin T, Reese, Justin T, Coleman, Ben, Chan, Lauren, Blau, Hannah, Callahan, Tiffany J, Cappelletti, Luca, Fontana, Tommaso, Bradwell, Katie R, Harris, Nomi L, Casiraghi, Elena, Valentini, Giorgio, Karlebach, Guy, Deer, Rachel, McMurry, Julie A, Haendel, Melissa A, Chute, Christopher G, Pfaff, Emily, Moffitt, Richard, Spratt, Heidi, Singh, Jasvinder A, Mungall, Christopher J, Williams, Andrew E, and Robinson, Peter N

Abstract

BackgroundNon-steroidal anti-inflammatory drugs (NSAIDs) are commonly used to reduce pain, fever, and inflammation but have been associated with complications in community-acquired pneumonia. Observations shortly after the start of the COVID-19 pandemic in 2020 suggested that ibuprofen was associated with an increased risk of adverse events in COVID-19 patients, but subsequent observational studies failed to demonstrate increased risk and in one case showed reduced risk associated with NSAID use.MethodsA 38-center retrospective cohort study was performed that leveraged the harmonized, high-granularity electronic health record data of the National COVID Cohort Collaborative. A propensity-matched cohort of 19,746 COVID-19 inpatients was constructed by matching cases (treated with NSAIDs at the time of admission) and 19,746 controls (not treated) from 857,061 patients with COVID-19 available for analysis. The primary outcome of interest was COVID-19 severity in hospitalized patients, which was classified as: moderate, severe, or mortality/hospice. Secondary outcomes were acute kidney injury (AKI), extracorporeal membrane oxygenation (ECMO), invasive ventilation, and all-cause mortality at any time following COVID-19 diagnosis.ResultsLogistic regression showed that NSAID use was not associated with increased COVID-19 severity (OR: 0.57 95% CI: 0.53-0.61). Analysis of secondary outcomes using logistic regression showed that NSAID use was not associated with increased risk of all-cause mortality (OR 0.51 95% CI: 0.47-0.56), invasive ventilation (OR: 0.59 95% CI: 0.55-0.64), AKI (OR: 0.67 95% CI: 0.63-0.72), or ECMO (OR: 0.51 95% CI: 0.36-0.7). In contrast, the odds ratios indicate reduced risk of these outcomes, but our quantitative bias analysis showed E-values of between 1.9 and 3.3 for these associations, indicating that comparatively weak or moderate confounder associations could explain away the observed associations.ConclusionsStudy interpretation is limited by the

Published

2022

22. Neurogenic inflammation as a novel treatment target for chronic pain syndromes.

Author

Seidel, Matthias F, Seidel, Matthias F, Hügle, Thomas, Morlion, Barton, Koltzenburg, Martin, Chapman, Victoria, MaassenVanDenBrink, Antoinette, Lane, Nancy E, Perrot, Serge, Zieglgänsberger, Walter, Seidel, Matthias F, Seidel, Matthias F, Hügle, Thomas, Morlion, Barton, Koltzenburg, Martin, Chapman, Victoria, MaassenVanDenBrink, Antoinette, Lane, Nancy E, Perrot, Serge, and Zieglgänsberger, Walter

Abstract

Chronic pain syndrome is a heterogeneous group of diseases characterized by several pathological mechanisms. One in five adults in Europe may experience chronic pain. In addition to the individual burden, chronic pain has a significant societal impact because of work and school absences, loss of work, early retirement, and high social and healthcare costs. Several anti-inflammatory treatments are available for patients with inflammatory or autoimmune diseases to control their symptoms, including pain. However, patients with degenerative chronic pain conditions, some with 10-fold or more elevated incidence relative to these manageable diseases, have few long-term pharmacological treatment options, limited mainly to non-steroidal anti-inflammatory drugs or opioids. For this review, we performed multiple PubMed searches using keywords such as "pain," "neurogenic inflammation," "NGF," "substance P," "nociception," "BDNF," "inflammation," "CGRP," "osteoarthritis," and "migraine." Many treatments, most with limited scientific evidence of efficacy, are available for the management of chronic pain through a trial-and-error approach. Although basic science and pre-clinical pain research have elucidated many biomolecular mechanisms of pain and identified promising novel targets, little of this work has translated into better clinical management of these conditions. This state-of-the-art review summarizes concepts of chronic pain syndromes and describes potential novel treatment strategies.

Published

2022

23. N-Acylated and N-Alkylated 2-Aminobenzothiazoles Are Novel Agents That Suppress the Generation of Prostaglandin E2.

Author

Theodoropoulou, Maria A, Theodoropoulou, Maria A, Psarra, Anastasia, Erhardt, Martin, Nikolaou, Aikaterini, Gerogiannopoulou, Anna-Dimitra D, Hadjipavlou-Litina, Dimitra, Hayashi, Daiki, Dennis, Edward A, Huwiler, Andrea, Kokotos, George, Theodoropoulou, Maria A, Theodoropoulou, Maria A, Psarra, Anastasia, Erhardt, Martin, Nikolaou, Aikaterini, Gerogiannopoulou, Anna-Dimitra D, Hadjipavlou-Litina, Dimitra, Hayashi, Daiki, Dennis, Edward A, Huwiler, Andrea, and Kokotos, George

Abstract

The quest for novel agents to regulate the generation of prostaglandin E2 (PGE2) is of high importance because this eicosanoid is a key player in inflammatory diseases. We synthesized a series of N-acylated and N-alkylated 2-aminobenzothiazoles and related heterocycles (benzoxazoles and benzimidazoles) and evaluated their ability to suppress the cytokine-stimulated generation of PGE2 in rat mesangial cells. 2-Aminobenzothiazoles, either acylated by the 3-(naphthalen-2-yl)propanoyl moiety (GK510) or N-alkylated by a chain carrying a naphthalene (GK543) or a phenyl moiety (GK562) at a distance of three carbon atoms, stand out in inhibiting PGE2 generation, with EC50 values ranging from 118 nM to 177 nM. Both GK510 and GK543 exhibit in vivo anti-inflammatory activity greater than that of indomethacin. Thus, N-acylated or N-alkylated 2-aminobenzothiazoles are novel leads for the regulation of PGE2 formation.

Published

2022

24. Impact of nutraceuticals on markers of systemic inflammation: Potential relevance to cardiovascular diseases - A position paper from the International Lipid Expert Panel (ILEP).

Author

UCL - (SLuc) Service de pathologie cardiovasculaire, Ruscica, Massimiliano, Penson, Peter E, Ferri, Nicola, Sirtori, Cesare R, Pirro, Matteo, Mancini, G B John, Sattar, Naveed, Toth, Peter P, Sahebkar, Amirhossein, Lavie, Carl J, Wong, Nathan D, Banach, Maciej, International Lipid Expert Panel (ILEP) and International Lipid Expert Panel Experts (alphabetically), Descamps, Olivier, UCL - (SLuc) Service de pathologie cardiovasculaire, Ruscica, Massimiliano, Penson, Peter E, Ferri, Nicola, Sirtori, Cesare R, Pirro, Matteo, Mancini, G B John, Sattar, Naveed, Toth, Peter P, Sahebkar, Amirhossein, Lavie, Carl J, Wong, Nathan D, Banach, Maciej, International Lipid Expert Panel (ILEP) and International Lipid Expert Panel Experts (alphabetically), and Descamps, Olivier

Abstract

Inflammation is a marker of arterial disease stemming from cholesterol-dependent to -independent molecular mechanisms. In recent years, the role of inflammation in atherogenesis has been underpinned by pharmacological approaches targeting systemic inflammation that have led to a significant reduction in cardiovascular disease (CVD) risk. Although the use of nutraceuticals to prevent CVD has largely focused on lipid-lowering (e.g, red-yeast rice and omega-3 fatty acids), there is growing interest and need, especially now in the time of coronavirus pandemic, in the use of nutraceuticals to reduce inflammatory markers, and potentially the inflammatory CVD burden, however, there is still not enough evidence to confirm this. Indeed, diet is an important lifestyle determinant of health and can influence both systemic and vascular inflammation, to varying extents, according to the individual nutraceutical constituents. Thus, the aim of this Position Paper is to provide the first attempt at recommendations on the use of nutraceuticals with effective anti-inflammatory properties.

Published

2022

25. Selectin-targeting glycosaminoglycan-peptide conjugate limits neutrophil-mediated cardiac reperfusion injury.

Author

Dehghani, Tima, Dehghani, Tima, Thai, Phung N, Sodhi, Harkanwalpreet, Ren, Lu, Sirish, Padmini, Nader, Carol E, Timofeyev, Valeriy, Overton, James L, Li, Xiaocen, Lam, Kit S, Chiamvimonvat, Nipavan, Panitch, Alyssa, Dehghani, Tima, Dehghani, Tima, Thai, Phung N, Sodhi, Harkanwalpreet, Ren, Lu, Sirish, Padmini, Nader, Carol E, Timofeyev, Valeriy, Overton, James L, Li, Xiaocen, Lam, Kit S, Chiamvimonvat, Nipavan, and Panitch, Alyssa

Abstract

AimsOne of the hallmarks of myocardial infarction (MI) is excessive inflammation. During an inflammatory insult, damaged endothelial cells shed their glycocalyx, a carbohydrate-rich layer on the cell surface which provides a regulatory interface to immune cell adhesion. Selectin-mediated neutrophilia occurs as a result of endothelial injury and inflammation. We recently designed a novel selectin-targeting glycocalyx mimetic (termed DS-IkL) capable of binding inflamed endothelial cells. This study examines the capacity of DS-IkL to limit neutrophil binding and platelet activation on inflamed endothelial cells, as well as the cardioprotective effects of DS-IkL after acute myocardial infarction.Methods and resultsIn vitro, DS-IkL diminished neutrophil interactions with both recombinant selectin and inflamed endothelial cells, and limited platelet activation on inflamed endothelial cells. Our data demonstrated that DS-IkL localized to regions of vascular inflammation in vivo after 45 min of left anterior descending coronary artery ligation-induced MI. Further, findings from this study show DS-IkL treatment had short- and long-term cardioprotective effects after ischaemia/reperfusion of the left anterior descending coronary artery. Mice treated with DS-IkL immediately after ischaemia/reperfusion and 24 h later exhibited reduced neutrophil extravasation, macrophage accumulation, fibroblast and endothelial cell proliferation, and fibrosis compared to saline controls.ConclusionsOur findings suggest that DS-IkL has great therapeutic potential after MI by limiting reperfusion injury induced by the immune response.

Published

2022

26. Small molecule C381 targets the lysosome to reduce inflammation and ameliorate disease in models of neurodegeneration.

Author

Vest, Ryan T, Vest, Ryan T, Chou, Ching-Chieh, Zhang, Hui, Haney, Michael S, Li, Lulin, Laqtom, Nouf N, Chang, Betty, Shuken, Steven, Nguyen, Andy, Yerra, Lakshmi, Yang, Andrew C, Green, Carol, Tanga, Mary, Abu-Remaileh, Monther, Bassik, Michael C, Frydman, Judith, Luo, Jian, Wyss-Coray, Tony, Vest, Ryan T, Vest, Ryan T, Chou, Ching-Chieh, Zhang, Hui, Haney, Michael S, Li, Lulin, Laqtom, Nouf N, Chang, Betty, Shuken, Steven, Nguyen, Andy, Yerra, Lakshmi, Yang, Andrew C, Green, Carol, Tanga, Mary, Abu-Remaileh, Monther, Bassik, Michael C, Frydman, Judith, Luo, Jian, and Wyss-Coray, Tony

Abstract

SignificanceNeurodegenerative diseases are poorly understood and difficult to treat. One common hallmark is lysosomal dysfunction leading to the accumulation of aggregates and other undegradable materials, which cause damage to brain resident cells. Lysosomes are acidic organelles responsible for breaking down biomolecules and recycling their constitutive parts. In this work, we find that the antiinflammatory and neuroprotective compound, discovered via a phenotypic screen, imparts its beneficial effects by targeting the lysosome and restoring its function. This is established using a genome-wide CRISPRi target identification screen and then confirmed using a variety of lysosome-targeted studies. The resulting small molecule from this study represents a potential treatment for neurodegenerative diseases as well as a research tool for the study of lysosomes in disease.

Published

2022

27. Cannabidiol modulates expression of type I IFN response genes and HIV infection in macrophages.

Author

Tomer, Shallu, Tomer, Shallu, Mu, Wenli, Suryawanshi, Gajendra, Ng, Hwee, Wang, Li, Wennerberg, Wally, Rezek, Valerie, Martin, Heather, Chen, Irvin, Kitchen, Scott, Zhen, Anjie, Tomer, Shallu, Tomer, Shallu, Mu, Wenli, Suryawanshi, Gajendra, Ng, Hwee, Wang, Li, Wennerberg, Wally, Rezek, Valerie, Martin, Heather, Chen, Irvin, Kitchen, Scott, and Zhen, Anjie

Abstract

Cannabis (Cannabis sativa) is a widely used drug in the United States and the frequency of cannabis use is particularly high among people living with HIV (PLWH). One key component of cannabis, the non-psychotropic (-)-cannabidiol (CBD) exerts a wide variety of biological actions, including anticonvulsive, analgesic, and anti-inflammatory effects. However, the exact mechanism of action through which CBD affects the immune cell signaling remains poorly understood. Here we report that CBD modulates type I interferon responses in human macrophages. Transcriptomics analysis shows that CBD treatment significantly attenuates cGAS-STING-mediated activation of type I Interferon response genes (ISGs) in monocytic THP-1 cells. We further showed that CBD treatment effectively attenuates 2'3-cGAMP stimulation of ISGs in both THP-1 cells and primary human macrophages. Interestingly, CBD significantly upregulates expression of autophagy receptor p62/SQSTM1. p62 is critical for autophagy-mediated degradation of stimulated STING. We observed that CBD treated THP-1 cells have elevated autophagy activity. Upon 2'3'-cGAMP stimulation, CBD treated cells have rapid downregulation of phosphorylated-STING, leading to attenuated expression of ISGs. The CBD attenuation of ISGs is reduced in autophagy deficient THP-1 cells, suggesting that the effects of CBD on ISGs is partially mediated by autophagy induction. Lastly, CBD decreases ISGs expression upon HIV infection in THP-1 cells and human primary macrophages, leading to increased HIV RNA expression 24 hours after infection. However, long term culture with CBD in infected primary macrophages reduced HIV viral spread, suggesting potential dichotomous roles of CBD in HIV replication. Our study highlights the immune modulatory effects of CBD and the needs for additional studies on its effect on viral infection and inflammation.

Published

2022

28. The comparative pathology of enterocolitis caused by Clostridium perfringens type C, Clostridioides difficile, Paeniclostridium sordellii, Salmonella enterica subspecies enterica serovar Typhimurium, and nonsteroidal anti-inflammatory drugs in horses.

Author

Mendonça, Fábio S, Mendonça, Fábio S, Navarro, Mauricio A, Uzal, Francisco A, Mendonça, Fábio S, Mendonça, Fábio S, Navarro, Mauricio A, and Uzal, Francisco A

Abstract

To determine if there were significant differences produced by 5 of the most prevalent causes of equine enterocolitis, we studied retrospectively the gross and microscopic pathology of 90 cases of enterocolitis submitted to the San Bernardino laboratory of the California Animal Health and Food Safety Laboratory. Included were cases caused by Clostridium perfringens type C (CP; n = 20), Clostridioides difficile (CD; n = 20), Paeniclostridium sordellii (PS; n = 15), Salmonella enterica subspecies enterica serovar Typhimurium (ST; n = 20), and NSAID intoxication (NS; n = 15). Grossly, necrotizing hemorrhagic typhlocolitis was seen most frequently in cases of CD, ST, and NS disease. Cases of CP and PS had enteritis or colitis in similar percentages. Congestion, hemorrhage, and pleocellular inflammatory infiltrates followed by mucosal and submucosal necrosis were the main lesions found in horses with enteritis or colitis produced by any of the etiologic agents investigated. Severe lesions were more frequent in cases of CD and CP than in cases associated with any of the other 3 etiologies. Pseudomembranes were observed with similar prevalence in the small intestine and colon affected by all agents studied. Thrombosis of the lamina propria and/or submucosa was observed in ~50% of the cases of enteritis and colitis by all etiologies, except for PS, in which the majority of the cases had thrombosis. Gross and microscopic lesions of enterocolitis were not sufficiently specific for any of these etiologic agents to enable these enteritides to be distinguished by gross and/or histologic examination.

Published

2022

29. Soluble epoxide hydrolase inhibition avoid formalin-induced inflammatory hyperalgesia in the temporomandibular joint.

Author

Abdalla, Henrique Ballassini, Abdalla, Henrique Ballassini, Napimoga, Marcelo Henrique, Teixeira, Juliana Maia, Trindade-da-Silva, Carlos Antônio, Pieroni, Victor Luís, Dos Santos Araújo, Fernanda Souto Maior, Hammock, Bruce D, Clemente-Napimoga, Juliana Trindade, Abdalla, Henrique Ballassini, Abdalla, Henrique Ballassini, Napimoga, Marcelo Henrique, Teixeira, Juliana Maia, Trindade-da-Silva, Carlos Antônio, Pieroni, Victor Luís, Dos Santos Araújo, Fernanda Souto Maior, Hammock, Bruce D, and Clemente-Napimoga, Juliana Trindade

Abstract

Epoxyeicosatrienoic acids (EETs) are endogenous molecules that exerts effective antinociceptive and resolutive actions. However, because of their rapid metabolism by the soluble epoxide hydrolase (sEH), EETs are unable to remain bioavailable. Therefore, the aim of this study was to investigate whether local sEH inhibition could prevent inflammatory hyperalgesia in the temporomandibular joint (TMJ) of rats. For that, rats were pre-treated with an intra-TMJ injection of TPPU, followed by the noxious stimulus (1.5% of formalin intra-articular) to evaluate nociceptive behavior. Histological analysis was conducted to explore the inflammatory exudate and mast cell degranulation. Periarticular tissue over the TMJ was used to measure inflammatory lipids and cytokines/chemokine by Enzyme-Linked Immunosorbent Assay (ELISA). We demonstrated that peripheral pretreatment with TPPU prevents formalin-induced inflammatory hyperalgesia in the TMJ, and this effect is strictly local. Moreover, TPPU mitigates the leukocyte exudate in the TMJ, as well as inflammatory lipids mediators. Mast cell number and degranulation were abrogated by TPPU, and the inflammatory cytokine levels were decreased by TPPU. On the other hand, TPPU up-regulated the release of interleukin 10 (IL-10), an anti-inflammatory cytokine. We provide evidence that locally sEH by intra-TMJ injection of TPPU produces an antinociceptive and anti-inflammatory effect on rats' TMJ.

Published

2022

30. Optimizing emollient therapy for skin barrier repair in atopic dermatitis.

Author

Elias, Peter M, Elias, Peter M, Elias, Peter M, and Elias, Peter M

Abstract

ObjectiveWe compared the principal characteristics of over-the-counter moisturizers with physiological lipid-based barrier repair therapy (BRT).Data sourcesAn extended literature reported that moisturizers are considered standard ancillary therapy for anti-inflammatory skin disorders such as atopic dermatitis (AD). Additional studies have found that physiological lipid-based BRT can comprise effective, stand-alone therapy for pediatric AD.ResultsNot all moisturizers are beneficial-some negatively impact skin function, and in doing so, they risk inducing or exacerbating inflammation in patients with AD. The frequent self-reported occurrences of sensitive skin in patients with AD could reflect the potential toxicity of such formulations. A still unanswered question is whether improper formulations could also prove to be counterproductive in other types of sensitive skin, such as rosacea. In contrast, we found how physiological lipid-based BRT (when comprised of the 3 key stratum corneum lipids in sufficient quantities and at an appropriate molar ratio) can correct the barrier abnormality, thereby reducing inflammation in AD and possibly in other inflammatory dermatoses, such as adult eczemas and possibly even psoriasis.ConclusionWe provide guidelines for the appropriate dispensation of moisturizers and physiological lipid-based, BRT for the treatment of AD. Both over-the-counter (Atopalm) and prescription (EpiCeram) products are available in the United States with these characteristics.

Published

2022

31. Inhibition of CtBP-Regulated Proinflammatory Gene Transcription Attenuates Psoriatic Skin Inflammation.

Author

Li, Hong, Li, Hong, Zhang, Caiguo, Bian, Li, Deng, Hui, Blevins, Melanie, Han, Gangwen, Fan, Bin, Yang, Chunxia, Zhao, Rui, High, Whitney, Norris, David, Fujita, Mayumi, Wang, Xiao-Jing, Huang, Mingxia, Li, Hong, Li, Hong, Zhang, Caiguo, Bian, Li, Deng, Hui, Blevins, Melanie, Han, Gangwen, Fan, Bin, Yang, Chunxia, Zhao, Rui, High, Whitney, Norris, David, Fujita, Mayumi, Wang, Xiao-Jing, and Huang, Mingxia

Abstract

Psoriasis is a chronic immune-mediated disease characterized by excessive proliferation of epidermal keratinocytes and increased immune cell infiltration to the skin. Although it is well-known that psoriasis pathogenesis is driven by aberrant production of proinflammatory cytokines, the mechanisms underlying the imbalance between proinflammatory and anti-inflammatory cytokine expression are incompletely understood. In this study, we report that the transcriptional coregulators CtBP1 and 2 can transactivate a common set of proinflammatory genes both in the skin of imiquimod-induced mouse psoriasis model and in human keratinocytes and macrophages stimulated by imiquimod. We find that mice overexpressing CtBP1 in epidermal keratinocytes display severe skin inflammation phenotypes with increased expression of T helper type 1 and T helper type 17 cytokines. We also find that the expression of CtBPs and CtBP-target genes is elevated both in human psoriatic lesions and in the mouse imiquimod psoriasis model. Moreover, we were able to show that topical treatment with a peptidic inhibitor of CtBP effectively suppresses the CtBP-regulated proinflammatory gene expression and thus attenuates psoriatic inflammation in the imiquimod mouse model. Together, our findings suggest to our knowledge previously unreported strategies for therapeutic modulation of the immune response in inflammatory skin diseases.

Published

2022

32. Oxy210, a Semi-Synthetic Oxysterol, Exerts Anti-Inflammatory Effects in Macrophages via Inhibition of Toll-like Receptor (TLR) 4 and TLR2 Signaling and Modulation of Macrophage Polarization.

Author

Wang, Feng, Wang, Feng, Stappenbeck, Frank, Tang, Liu-Ya, Zhang, Ying, Hui, Simon, Lusis, Aldons, Parhami, Farhad, Wang, Feng, Wang, Feng, Stappenbeck, Frank, Tang, Liu-Ya, Zhang, Ying, Hui, Simon, Lusis, Aldons, and Parhami, Farhad

Abstract

Inflammatory responses by the innate and adaptive immune systems protect against infections and are essential to health and survival. Many diseases including atherosclerosis, osteoarthritis, rheumatoid arthritis, psoriasis, and obesity involve persistent chronic inflammation. Currently available anti-inflammatory agents, including non-steroidal anti-inflammatory drugs, steroids, and biologics, are often unsafe for chronic use due to adverse effects. The development of effective non-toxic anti-inflammatory agents for chronic use remains an important research arena. We previously reported that oral administration of Oxy210, a semi-synthetic oxysterol, ameliorates non-alcoholic steatohepatitis (NASH) induced by a high-fat diet in APOE*3-Leiden.CETP humanized mouse model of NASH and inhibits expression of hepatic and circulating levels of inflammatory cytokines. Here, we show that Oxy210 also inhibits diet-induced white adipose tissue inflammation in APOE*3-Leiden.CETP mice, evidenced by the inhibition of adipose tissue expression of IL-6, MCP-1, and CD68 macrophage marker. Oxy210 and related analogs exhibit anti-inflammatory effects in macrophages treated with lipopolysaccharide in vitro, mediated through inhibition of toll-like receptor 4 (TLR4), TLR2, and AP-1 signaling, independent of cyclooxygenase enzymes or steroid receptors. The anti-inflammatory effects of Oxy210 are correlated with the inhibition of macrophage polarization. We propose that Oxy210 and its structural analogs may be attractive candidates for future therapeutic development for targeting inflammatory diseases.

Published

2022

33. Trends in Prescriptions for Non-opioid Pain Medications Among U.S. Adults With Moderate or Severe Pain, 2014-2018.

Author

Gorfinkel, Lauren R, Gorfinkel, Lauren R, Hasin, Deborah, Saxon, Andrew J, Wall, Melanie, Martins, Silvia S, Cerdá, Magdalena, Keyes, Katherine, Fink, David S, Keyhani, Salomeh, Maynard, Charles C, Olfson, Mark, Gorfinkel, Lauren R, Gorfinkel, Lauren R, Hasin, Deborah, Saxon, Andrew J, Wall, Melanie, Martins, Silvia S, Cerdá, Magdalena, Keyes, Katherine, Fink, David S, Keyhani, Salomeh, Maynard, Charles C, and Olfson, Mark

Abstract

As opioid prescribing has declined, it is unclear how the landscape of prescription pain treatment across the U.S. has changed. We used nationally-representative data from the Medical Expenditure Health Survey, 2014 to 2018 to examine trends in prescriptions for opioid and non-opioid pain medications, including acetaminophen, non-steroidal anti-inflammatory drugs, gabapentinoids, and antidepressants among U.S. adults with self-reported pain. Overall, from 2014 to 2018, the percentage of participants receiving a prescription for opioids declined, (38.8% vs 32.8%), remained stable for non-steroidal anti-inflammatory drugs (26.8% vs 27.7%), and increased for acetaminophen (1.6% vs 2.3%), antidepressants (9.6% vs 12.0%) and gabapentinoids (13.2% vs 19.0%). In this period, the adjusted odds of receiving an opioid prescription decreased (aOR = .93, 95% CI = .90-.96), while the adjusted odds of receiving antidepressant, gabapentinoid and acetaminophen prescriptions increased (antidepressants: aOR = 1.08, 95% CI = 1.03-1.13 gabapentinoids: aOR = 1.11, 95% CI = 1.06-1.17; acetaminophen: aOR = 1.10, 95% CI: 1.02-1.20). Secondary analyses stratifiying within the 2014 to 2016 and 2016 to 2018 periods revealed particular increases in prescriptions for gabapentinoids (aOR = 1.13, 95% CI = 1.05-1.21) and antidepressants (aOR = 1.23, 95% CI = 1.12-1.35) since 2016. PERSPECTIVE: These data demonstrate that physicians are increasingly turning to CDC-recommended non-opioid medications for pain management, particularly antidepressants and gabapentinoids. However, evidence for these medications' efficacy in treating numerous common pain conditions, including low back pain, remains limited.

Published

2022

34. No Benefit of Continuing 5-Aminosalicylates in Patients with Crohn's Disease Treated with Anti-metabolite Therapy.

Author

Picetti, Dominic, Picetti, Dominic, Kim, Jihoon, Zhu, Wenhong, Sandborn, William J, Jairath, Vipul, Singh, Siddharth, Picetti, Dominic, Picetti, Dominic, Kim, Jihoon, Zhu, Wenhong, Sandborn, William J, Jairath, Vipul, and Singh, Siddharth

Abstract

Background and aims5-aminosalicylates (5-ASA) are frequently used in the management of Crohn's disease (CD). We used a de-identified administrative claims database to compare patterns and outcomes of continuing versus stopping 5-ASA in patients with CD who escalated to anti-metabolite monotherapy.MethodsPatients with CD on 5-ASA who were new users of anti-metabolite monotherapy and followed for at least 12 months from OptumLabs® Data Warehouse. Three patterns of 5-ASA use were identified: stopped 5-ASA, short-term 5-ASA (use for < 6 months after starting anti-metabolites), or persistent 5-ASA (use for > 6 months after starting anti-metabolites). Outcomes (need for corticosteroids, risk of CD-related hospitalization and/or surgery, treatment escalation to biologic therapy) were compared using Cox proportional hazard analysis adjusting for key covariates, with a 12-month immortal time period.ResultsOf 3036 patients with CD who were new-users of anti-metabolite monotherapy, 667 (21.9%), 626 (20.6%), and 1743 (57.4%) stopped 5-ASA, used 5-ASA transiently or persistently, respectively. Compared to patients who stopped 5-ASA after starting anti-metabolites, persistent 5-ASA use was associated with a higher risk of corticosteroid use (HR, 1.24 [1.08-1.42]), without an increase in risk of CD-related hospitalization (HR, 1.21 [0.98-1.49]), CD-related surgery (HR, 1.28 [0.90-1.80]) or treatment escalation (HR, 0.85 [0.62-1.20]). Sensitivity analyses using a 3-month window after initiation of anti-metabolites to classify patients as continuing vs. stopping 5-ASA showed similar results. Residual confounding by disease severity could not be excluded.Conclusion5-ASAs are frequently continued long-term even after escalation to anti-metabolite therapy in patients with CD but offer no clinical benefit over stopping 5-ASA.

Published

2022

35. Cross-species comparisons reveal resistance of human skeletal stem cells to inhibition by non-steroidal anti-inflammatory drugs.

Author

Goodnough, L Henry, Goodnough, L Henry, Ambrosi, Thomas H, Steininger, Holly M, Butler, M Gohazrua K, Hoover, Malachia Y, Choo, HyeRan, Van Rysselberghe, Noelle L, Bellino, Michael J, Bishop, Julius A, Gardner, Michael J, Chan, Charles KF, Goodnough, L Henry, Goodnough, L Henry, Ambrosi, Thomas H, Steininger, Holly M, Butler, M Gohazrua K, Hoover, Malachia Y, Choo, HyeRan, Van Rysselberghe, Noelle L, Bellino, Michael J, Bishop, Julius A, Gardner, Michael J, and Chan, Charles KF

Abstract

Fracture healing is highly dependent on an early inflammatory response in which prostaglandin production by cyclo-oxygenases (COX) plays a crucial role. Current patient analgesia regimens favor opioids over Non-Steroidal Anti-Inflammatory Drugs (NSAIDs) since the latter have been implicated in delayed fracture healing. While animal studies broadly support a deleterious role of NSAID treatment to bone-regenerative processes, data for human fracture healing remains contradictory. In this study, we prospectively isolated mouse and human skeletal stem cells (SSCs) from fractures and compared the effect of various NSAIDs on their function. We found that osteochondrogenic differentiation of COX2-expressing mouse SSCs was impaired by NSAID treatment. In contrast, human SSCs (hSSC) downregulated COX2 expression during differentiation and showed impaired osteogenic capacity if COX2 was lentivirally overexpressed. Accordingly, short- and long-term treatment of hSSCs with non-selective and selective COX2 inhibitors did not affect colony forming ability, chondrogenic, and osteogenic differentiation potential in vitro. When hSSCs were transplanted ectopically into NSG mice treated with Indomethacin, graft mineralization was unaltered compared to vehicle injected mice. Thus, our results might contribute to understanding species-specific differences in NSAID sensitivity during fracture healing and support emerging clinical data which conflicts with other earlier observations that NSAID administration for post-operative analgesia for treatment of bone fractures are unsafe for patients.

Published

2022

36. Analgesic Use and Circulating Estrogens, Androgens, and Their Metabolites in the Women's Health Initiative Observational Study.

Author

Hurwitz, Lauren M, Hurwitz, Lauren M, Shadyab, Aladdin H, Tabung, Fred K, Anderson, Garnet L, Saquib, Nazmus, Wallace, Robert B, Wild, Robert A, Pfeiffer, Ruth M, Xu, Xia, Trabert, Britton, Hurwitz, Lauren M, Hurwitz, Lauren M, Shadyab, Aladdin H, Tabung, Fred K, Anderson, Garnet L, Saquib, Nazmus, Wallace, Robert B, Wild, Robert A, Pfeiffer, Ruth M, Xu, Xia, and Trabert, Britton

Abstract

Though studies have observed inverse associations between use of analgesics (aspirin, NSAIDs, and acetaminophen) and the risk of several cancers, the potential biological mechanisms underlying these associations are unclear. We investigated the relationship between analgesic use and serum concentrations of estrogens, androgens, and their metabolites among postmenopausal women to provide insights on whether analgesic use might influence endogenous hormone levels, which could in turn influence hormone-related cancer risk. The study included 1,860 postmenopausal women from two case-control studies nested within the Women's Health Initiative Observational Study. Analgesic use was reported at study baseline. Fifteen estrogens and estrogen metabolites and 12 androgens and androgen metabolites were quantified in baseline serum by LC/MS-MS. Linear regression with inverse probability weighting, stratified by menopausal hormone therapy (MHT) use, was used to estimate adjusted geometric mean concentrations of each hormone by analgesic use. Among women not currently using MHT (n = 951), low-dose aspirin (<100 mg) use was associated with a higher serum concentration of estrone, estradiol, and 2, 4, and 16 hydroxylated metabolites. Use of regular-dose aspirin (≥100 mg), non-aspirin NSAIDs, and acetaminophen was not associated with serum concentrations of estrogens, androgens, or their metabolites. This study highlights the importance of examining aspirin use by dose and suggests that low-dose aspirin may influence endogenous estrogen concentrations.Prevention relevanceThis study explores a potential pathway by which analgesic medications such as aspirin may prevent hormone-related cancers. The findings support a positive association between low-dose aspirin use and endogenous estrogens, indicating that further elucidation of the interplay between low-dose aspirin, estrogen concentrations, and cancer risk is needed.

Published

2022

37. Zinc against COVID-19? Symptom surveillance and deficiency risk groups.

Author

Joachimiak, Marcin P, Joachimiak, Marcin P, Joachimiak, Marcin P, and Joachimiak, Marcin P

Abstract

A wide variety of symptoms is associated with Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection, and these symptoms can overlap with other conditions and diseases. Knowing the distribution of symptoms across diseases and individuals can support clinical actions on timelines shorter than those for drug and vaccine development. Here, we focus on zinc deficiency symptoms, symptom overlap with other conditions, as well as zinc effects on immune health and mechanistic zinc deficiency risk groups. There are well-studied beneficial effects of zinc on the immune system including a decreased susceptibility to and improved clinical outcomes for infectious pathogens including multiple viruses. Zinc is also an anti-inflammatory and anti-oxidative stress agent, relevant to some severe Coronavirus Disease 2019 (COVID-19) symptoms. Unfortunately, zinc deficiency is common worldwide and not exclusive to the developing world. Lifestyle choices and preexisting conditions alone can result in zinc deficiency, and we compile zinc risk groups based on a review of the literature. It is also important to distinguish chronic zinc deficiency from deficiency acquired upon viral infection and immune response and their different supplementation strategies. Zinc is being considered as prophylactic or adjunct therapy for COVID-19, with 12 clinical trials underway, highlighting the relevance of this trace element for global pandemics. Using the example of zinc, we show that there is a critical need for a deeper understanding of essential trace elements in human health, and the resulting deficiency symptoms and their overlap with other conditions. This knowledge will directly support human immune health for decreasing susceptibility, shortening illness duration, and preventing progression to severe cases in the current and future pandemics.

Published

2021

38. Immunotherapies for Neurodegenerative Diseases.

Author

Mortada, Ibrahim, Mortada, Ibrahim, Farah, Raymond, Nabha, Sanaa, Ojcius, David M, Fares, Youssef, Almawi, Wassim Y, Sadier, Najwane Said, Mortada, Ibrahim, Mortada, Ibrahim, Farah, Raymond, Nabha, Sanaa, Ojcius, David M, Fares, Youssef, Almawi, Wassim Y, and Sadier, Najwane Said

Abstract

The current treatments for neurodegenerative diseases are mostly symptomatic without affecting the underlying cause of disease. Emerging evidence supports a potential role for immunotherapy in the management of disease progression. Numerous reports raise the exciting prospect that either the immune system or its derivative components could be harnessed to fight the misfolded and aggregated proteins that accumulate in several neurodegenerative diseases. Passive and active vaccinations using monoclonal antibodies and specific antigens that induce adaptive immune responses are currently under evaluation for their potential use in the development of immunotherapies. In this review, we aim to shed light on prominent immunotherapeutic strategies being developed to fight neuroinflammation-induced neurodegeneration, with a focus on innovative immunotherapies such as vaccination therapy.

Published

2021

39. Evaluating efficacy of a novel dentifrice in reducing probing depths in Stage I and II periodontitis maintenance patients: A randomized, double-blind, positive controlled clinical trial.

Author

Kaur, Maninder, Kaur, Maninder, Geurs, Nicolaas C, Cobb, Charles M, Otomo-Corgel, Joan, Takesh, Thair, Lee, June H, Lam, Tracie M, Lin, Kairong, Nguyen, Audrey, Nguyen, Brian L, Wilder-Smith, Petra, Kaur, Maninder, Kaur, Maninder, Geurs, Nicolaas C, Cobb, Charles M, Otomo-Corgel, Joan, Takesh, Thair, Lee, June H, Lam, Tracie M, Lin, Kairong, Nguyen, Audrey, Nguyen, Brian L, and Wilder-Smith, Petra

Abstract

BackgroundCompliance to periodontal maintenance therapy (PMT) is essential for long-term periodontal health. Between PMT visits, patients must maintain good oral hygiene. A dentifrice with demonstrable clinical benefits for use between PMT visits would be highly desirable. The aim of this clinical study was to investigate the effect of a novel dental gel on probing depths (PD) and inflammation when used as a home care dentifrice in Stage I and II periodontitis patients.MethodsThis double-blind clinical study randomized 65 subjects with Stage I and II periodontitis to the novel dental gel containing 2.6% EDTA, and a commercially available anti-gingivitis dentifrice with 0.454% stannous fluoride. Primary endpoint was PD at 6 months for those sites with baseline PD ≥ 4 mm and secondary endpoints included whole mouth mean scores of modified gingival index (MGI), modified sulcus bleeding index (mSBI) and plaque index (PI). No SRP was performed at baseline.ResultsSubjects using the novel dentifrice showed significant PD reductions of 1.18 mm (from 4.27 mm at baseline to 3.09 mm at 6 months) compared to 0.93 mm (from 4.23 mm at baseline to 3.30 mm at 6 months) shown for those using the positive control dentifrice. Difference between treatments at 6 months was 0.21 mm with P-value = 0.0126. Significant improvements in MGI (P = 0.0000), mSBI (P = 0.0000), and PI (P = 0.0102) were also observed in 6 months.ConclusionThe novel dentifrice showed significant reductions in PD and gingival inflammation over 6 months solely as a home care dentifrice without baseline SRP in Stage I and II periodontitis maintenance patients.

Published

2021

40. Mitohormesis reprogrammes macrophage metabolism to enforce tolerance.

Author

Timblin, Greg A, Timblin, Greg A, Tharp, Kevin M, Ford, Breanna, Winchester, Janet M, Wang, Jerome, Zhu, Stella, Khan, Rida I, Louie, Shannon K, Iavarone, Anthony T, Ten Hoeve, Johanna, Nomura, Daniel K, Stahl, Andreas, Saijo, Kaoru, Timblin, Greg A, Timblin, Greg A, Tharp, Kevin M, Ford, Breanna, Winchester, Janet M, Wang, Jerome, Zhu, Stella, Khan, Rida I, Louie, Shannon K, Iavarone, Anthony T, Ten Hoeve, Johanna, Nomura, Daniel K, Stahl, Andreas, and Saijo, Kaoru

Abstract

Macrophages generate mitochondrial reactive oxygen species and mitochondrial reactive electrophilic species as antimicrobials during Toll-like receptor (TLR)-dependent inflammatory responses. Whether mitochondrial stress caused by these molecules impacts macrophage function is unknown. Here, we demonstrate that both pharmacologically driven and lipopolysaccharide (LPS)-driven mitochondrial stress in macrophages triggers a stress response called mitohormesis. LPS-driven mitohormetic stress adaptations occur as macrophages transition from an LPS-responsive to LPS-tolerant state wherein stimulus-induced pro-inflammatory gene transcription is impaired, suggesting tolerance is a product of mitohormesis. Indeed, like LPS, hydroxyoestrogen-triggered mitohormesis suppresses mitochondrial oxidative metabolism and acetyl-CoA production needed for histone acetylation and pro-inflammatory gene transcription, and is sufficient to enforce an LPS-tolerant state. Thus, mitochondrial reactive oxygen species and mitochondrial reactive electrophilic species are TLR-dependent signalling molecules that trigger mitohormesis as a negative feedback mechanism to restrain inflammation via tolerance. Moreover, bypassing TLR signalling and pharmacologically triggering mitohormesis represents a new anti-inflammatory strategy that co-opts this stress response to impair epigenetic support of pro-inflammatory gene transcription by mitochondria.

Published

2021

41. Multisystem Inflammatory Syndrome in Children: Survey of Protocols for Early Hospital Evaluation and Management.

Author

Dove, Matthew L, Dove, Matthew L, Jaggi, Preeti, Kelleman, Michael, Abuali, Mayssa, Ang, Jocelyn Y, Ballan, Wassim, Basu, Sanmit K, Campbell, M Jay, Chikkabyrappa, Sathish M, Choueiter, Nadine F, Clouser, Katharine N, Corwin, Daniel, Edwards, Amy, Gertz, Shira J, Ghassemzadeh, Rod, Jarrah, Rima J, Katz, Sophie E, Knutson, Stacie M, Kuebler, Joseph D, Lighter, Jennifer, Mikesell, Christine, Mongkolrattanothai, Kanokporn, Morton, Ted, Nakra, Natasha A, Olivero, Rosemary, Osborne, Christina M, Panesar, Laurie E, Parsons, Sarah, Patel, Rupal M, Schuette, Jennifer, Thacker, Deepika, Tremoulet, Adriana H, Vidwan, Navjyot K, Oster, Matthew E, Dove, Matthew L, Dove, Matthew L, Jaggi, Preeti, Kelleman, Michael, Abuali, Mayssa, Ang, Jocelyn Y, Ballan, Wassim, Basu, Sanmit K, Campbell, M Jay, Chikkabyrappa, Sathish M, Choueiter, Nadine F, Clouser, Katharine N, Corwin, Daniel, Edwards, Amy, Gertz, Shira J, Ghassemzadeh, Rod, Jarrah, Rima J, Katz, Sophie E, Knutson, Stacie M, Kuebler, Joseph D, Lighter, Jennifer, Mikesell, Christine, Mongkolrattanothai, Kanokporn, Morton, Ted, Nakra, Natasha A, Olivero, Rosemary, Osborne, Christina M, Panesar, Laurie E, Parsons, Sarah, Patel, Rupal M, Schuette, Jennifer, Thacker, Deepika, Tremoulet, Adriana H, Vidwan, Navjyot K, and Oster, Matthew E

Abstract

ObjectiveTo describe the similarities and differences in the evaluation and treatment of multisystem inflammatory syndrome in children (MIS-C) at hospitals in the US.Study designWe conducted a cross-sectional survey from June 16 to July 16, 2020, of US children's hospitals regarding protocols for management of patients with MIS-C. Elements included characteristics of the hospital, clinical definition of MIS-C, evaluation, treatment, and follow-up. We summarized key findings and compared results from centers in which >5 patients had been treated vs those in which ≤5 patients had been treated.ResultsIn all, 40 centers of varying size and experience with MIS-C participated in this protocol survey. Overall, 21 of 40 centers required only 1 day of fever for MIS-C to be considered. In the evaluation of patients, there was often a tiered approach. Intravenous immunoglobulin was the most widely recommended medication to treat MIS-C (98% of centers). Corticosteroids were listed in 93% of protocols primarily for moderate or severe cases. Aspirin was commonly recommended for mild cases, whereas heparin or low molecular weight heparin were to be used primarily in severe cases. In severe cases, anakinra and vasopressors frequently were recommended; 39 of 40 centers recommended follow-up with cardiology. There were similar findings between centers in which >5 patients vs ≤5 patients had been managed. Supplemental materials containing hospital protocols are provided.ConclusionsThere are many similarities yet key differences between hospital protocols for MIS-C. These findings can help healthcare providers learn from others regarding options for managing MIS-C.

Published

2021

42. Colchicine in Patients With Acute Coronary Syndrome: Two-Year Follow-Up of the Australian COPS Randomized Clinical Trial

Author

Tong, DC, Bloom, JE, Quinn, S, Nasis, A, Hiew, Chin, Roberts-Thomson, P, Adams, H, Sriamareswaran, R, Htun, NM, Wilson, W, Stub, D, van Gaal, W, Howes, L, Yeap, A, Yip, B, Wu, S, Perera, P, Collins, N, Yong, A, Bhindi, R, Whitbourn, R, Lee, A, Premaratne, M, Asrress, K, Freeman, M, Amerena, John, Layland, J, Tong, DC, Bloom, JE, Quinn, S, Nasis, A, Hiew, Chin, Roberts-Thomson, P, Adams, H, Sriamareswaran, R, Htun, NM, Wilson, W, Stub, D, van Gaal, W, Howes, L, Yeap, A, Yip, B, Wu, S, Perera, P, Collins, N, Yong, A, Bhindi, R, Whitbourn, R, Lee, A, Premaratne, M, Asrress, K, Freeman, M, Amerena, John, and Layland, J

Published

2021

43. Improvement in Hidradenitis Suppurativa and quality of life in patients treated with adalimumab: Real-world results from the HARMONY Study.

Author

UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de dermatologie, Hafner, A, Ghislain, P D, Kovács, R, Batchelor, R, Katoulis, A C, Kirby, B, Banayan, H, Schonbrun, M, UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de dermatologie, Hafner, A, Ghislain, P D, Kovács, R, Batchelor, R, Katoulis, A C, Kirby, B, Banayan, H, and Schonbrun, M

Abstract

Hidradenitis suppurativa (HS), a chronic, recurrent, debilitating skin disease, is characterized by painful, inflammatory, subcutaneous lesions of the axilla, inguinal and anogenital regions. Overall prevalence of HS is ˜1%, and the impact of disease on patient quality of life (QoL) and healthcare resource utilization (HRU) is high. To estimate the real-world effectiveness of adalimumab (Humira®) treatment in patients with moderate-to-severe HS on disease severity, pain, QoL, work productivity and HRU. HARMONY (Effectiveness of Adalimumab in Moderate to Severe HidrAdenitis SuppuRativa Patients - a Multi-cOuNtry studY in Real Life Setting) is a multicentre, postmarketing observational study in adult patients with moderate-to-severe HS. Disease severity and QoL parameters were evaluated using validated measures at 12-week intervals over 52 weeks of treatment. The primary endpoint was the proportion of patients achieving a Hidradenitis Suppurativa Clinical Response (HiSCR: ≥50% reduction in abscess and inflammatory nodule count, with no increase in abscess and draining fistula counts relative to baseline) at 12 weeks. Secondary endpoints were HiSCR at 24, 36 and 52 weeks and changes in QoL parameters and work productivity assessments. Analyses were conducted using as-observed data. The proportion of patients reaching the primary HiSCR endpoint was 70.2% (n = 132/188 enrolled) and remained ≥70% until study completion. There were statistically significant (P < 0.0001) reductions in worst and average skin pain. All of the QoL measures evaluated improved significantly (P < 0.0001) by 12 weeks of adalimumab treatment, as did work productivity assessments (P < 0.05), and there was a ˜50% decrease in HRU between baseline and week 52. Adalimumab was well tolerated. In this real-world setting, adalimumab treatment of moderate-to-severe HS resulted in decreased disease severity and improvements in QoL and productivity. Response to adalimumab was rapid (within 12 weeks) and susta

Published

2021

44. Cannabis and Inflammation in HIV: A Review of Human and Animal Studies.

Author

Ellis, Ronald J, Ellis, Ronald J, Wilson, Natalie, Peterson, Scott, Ellis, Ronald J, Ellis, Ronald J, Wilson, Natalie, and Peterson, Scott

Abstract

Persistent inflammation occurs in people with HIV (PWH) and has many downstream adverse effects including myocardial infarction, neurocognitive impairment and death. Because the proportion of people with HIV who use cannabis is high and cannabis may be anti-inflammatory, it is important to characterize the impact of cannabis use on inflammation specifically in PWH. We performed a selective, non-exhaustive review of the literature on the effects of cannabis on inflammation in PWH. Research in this area suggests that cannabinoids are anti-inflammatory in the setting of HIV. Anti-inflammatory actions are mediated in many cases through effects on the endocannabinoid system (ECS) in the gut, and through stabilization of gut-blood barrier integrity. Cannabidiol may be particularly important as an anti-inflammatory cannabinoid. Cannabis may provide a beneficial intervention to reduce morbidity related to inflammation in PWH.

Published

2021

45. Pragmatic trials with prespecified subgroups: what oncologists can learn from COVID-19.

Author

Banerjee, Rahul, Banerjee, Rahul, Prasad, Vinay, Banerjee, Rahul, Banerjee, Rahul, and Prasad, Vinay

Abstract

Randomized controlled trials designed to test cancer therapies often fail to clarify effectiveness in real-world settings. Herein, we explore lessons for trial development in oncology that can be learnt from the large-cohort, pragmatic RECOVERY trial involving patients hospitalized with COVID-19.

Published

2021

46. Characterization of individuals with osteoarthritis in the United States and their use of prescription and over-the-counter supplements.

Author

Lane, Nancy E, Lane, Nancy E, Ivanova, Jasmina, Emir, Birol, Mobasheri, Ali, Jensen, Morten Georg, Lane, Nancy E, Lane, Nancy E, Ivanova, Jasmina, Emir, Birol, Mobasheri, Ali, and Jensen, Morten Georg

Abstract

PurposeOsteoarthritis (OA) is a frequently occurring, chronic condition; however, few studies describe the clinical characteristics of individuals with OA and the treatments they use to manage their symptoms. We conducted a study to characterize the OA population in the US and describe the nonsurgical management used by this population based on consumer research data collected through an online survey.MethodsData from the 2017 US National Health and Wellness Survey (NHWS) for adults aged ≥35 years were used to evaluate the relationship between OA and certain study participant characteristics and to identify the most commonly used treatment options. NHWS data were collected through a survey of individuals drawn from the internet panel maintained by Lightspeed Research (Bridgewater, New Jersey) and its panel partners. Weighted estimates were generated using data from the 2016 Current Population Survey (Annual Demographics File) of the US Census Bureau. Comparisons between the general and OA populations were made based on body mass index (BMI), exercise frequency, and comorbid diagnoses of hypertension or diabetes. Among the OA population, the use of dietary supplements, prescription or over-the-counter (OTC) treatments with chondroitin with or without glucosamine (Ch ± Gl), prescription treatment by time since OA diagnosis, and utilization of a physical therapist were also recorded.ResultsThe prevalence of OA in the overall population was 17.6 % and was higher for individuals with a BMI ≥ 25 (21.9 %), patients diagnosed with hypertension or diabetes (36.2 %), and those who did not exercise regularly (19.0 %). Adults without OA were more likely to exercise regularly (12 days per month or more) than adults diagnosed with OA. Ch ± Gl (6.0 %) was the most commonly used OTC dietary supplement in the OA population, followed by omega-3 fatty acids (2.8 %), vitamin D (1.9 %), calcium (1.1 %), and multivitamins (0.7 %). Individuals using Ch ± Gl were more likely to use OTC onl

Published

2021

47. A Phase 2b randomized trial of lorecivivint, a novel intra-articular CLK2/DYRK1A inhibitor and Wnt pathway modulator for knee osteoarthritis.

Author

Yazici, Y, Yazici, Y, McAlindon, TE, Gibofsky, A, Lane, NE, Lattermann, C, Skrepnik, N, Swearingen, CJ, Simsek, I, Ghandehari, H, DiFrancesco, A, Gibbs, J, Tambiah, JRS, Hochberg, MC, Yazici, Y, Yazici, Y, McAlindon, TE, Gibofsky, A, Lane, NE, Lattermann, C, Skrepnik, N, Swearingen, CJ, Simsek, I, Ghandehari, H, DiFrancesco, A, Gibbs, J, Tambiah, JRS, and Hochberg, MC

Abstract

ObjectiveLorecivivint (LOR; SM04690), an investigational Wnt pathway modulator, previously demonstrated patient-reported and radiographic outcome improvements vs placebo in clinically relevant subjects with moderate to severe knee osteoarthritis (OA). This study's objective was to identify effective LOR doses.DesignSubjects in this 24-week, Phase 2b, multicenter, randomized, double-blind, placebo (PBO)-controlled trial received an intra-articular injection of 2 mL LOR (0.03, 0.07, 0.15, or 0.23 mg), PBO, or dry-needle sham. The primary efficacy endpoints were changes in Pain NRS [0-10], WOMAC Pain [0-100], WOMAC Function [0-100], and radiographic mJSW outcomes, which were measured using baseline-adjusted analysis of covariance at Week 24. Multiple Comparison Procedure-Modeling (MCP-Mod) was performed for dose modeling.ResultsIn total, 695/700 subjects were treated. Pain NRS showed significant improvements vs PBO after treatment with 0.07 mg and 0.23 mg LOR at Weeks 12 (-0.96, 95% CI [-1.54, -0.37], P = 0.001; -0.78 [-1.39, -0.17], P = 0.012) and 24 (-0.70 [-1.34, -0.06], P = 0.031; -0.82 [-1.51, -0.12], P = 0.022). Additionally, 0.07 mg LOR significantly improved WOMAC Pain and Function subscores vs PBO at Week 12 (P = 0.04, P = 0.021), and 0.23 mg LOR significantly improved both WOMAC subscores at Week 24 (P = 0.031, P = 0.017). No significant differences from PBO were observed for other doses. No radiographic progression was observed in any group at Week 24. MCP-Mod identified 0.07 mg LOR as the lowest effective dose.ConclusionThis 24-week Phase 2b trial demonstrated the efficacy of LOR on PROs in knee OA subjects. The optimal dose for future studies was identified as 0.07 mg LOR.

Published

2021

48. Naproxen chemoprevention promotes immune activation in Lynch syndrome colorectal mucosa.

Author

Reyes-Uribe, Laura, Reyes-Uribe, Laura, Wu, Wenhui, Gelincik, Ozkan, Bommi, Prashant V, Francisco-Cruz, Alejandro, Solis, Luisa M, Lynch, Patrick M, Lim, Ramona, Stoffel, Elena M, Kanth, Priyanka, Samadder, N Jewel, Mork, Maureen E, Taggart, Melissa W, Milne, Ginger L, Marnett, Lawrence J, Vornik, Lana, Liu, Diane D, Revuelta, Maria, Chang, Kyle, You, Y Nancy, Kopelovich, Levy, Wistuba, Ignacio I, Lee, J Jack, Sei, Shizuko, Shoemaker, Robert H, Szabo, Eva, Richmond, Ellen, Umar, Asad, Perloff, Marjorie, Brown, Powel H, Lipkin, Steven M, Vilar, Eduardo, Reyes-Uribe, Laura, Reyes-Uribe, Laura, Wu, Wenhui, Gelincik, Ozkan, Bommi, Prashant V, Francisco-Cruz, Alejandro, Solis, Luisa M, Lynch, Patrick M, Lim, Ramona, Stoffel, Elena M, Kanth, Priyanka, Samadder, N Jewel, Mork, Maureen E, Taggart, Melissa W, Milne, Ginger L, Marnett, Lawrence J, Vornik, Lana, Liu, Diane D, Revuelta, Maria, Chang, Kyle, You, Y Nancy, Kopelovich, Levy, Wistuba, Ignacio I, Lee, J Jack, Sei, Shizuko, Shoemaker, Robert H, Szabo, Eva, Richmond, Ellen, Umar, Asad, Perloff, Marjorie, Brown, Powel H, Lipkin, Steven M, and Vilar, Eduardo

Abstract

ObjectivePatients with Lynch syndrome (LS) are at markedly increased risk for colorectal cancer. It is being increasingly recognised that the immune system plays an essential role in LS tumour development, thus making an ideal target for cancer prevention. Our objective was to evaluate the safety, assess the activity and discover novel molecular pathways involved in the activity of naproxen as primary and secondary chemoprevention in patients with LS.DesignWe conducted a Phase Ib, placebo-controlled, randomised clinical trial of two dose levels of naproxen sodium (440 and 220 mg) administered daily for 6 months to 80 participants with LS, and a co-clinical trial using a genetically engineered mouse model of LS and patient-derived organoids (PDOs).ResultsOverall, the total number of adverse events was not different across treatment arms with excellent tolerance of the intervention. The level of prostaglandin E2 in the colorectal mucosa was significantly decreased after treatment with naproxen when compared with placebo. Naproxen activated different resident immune cell types without any increase in lymphoid cellularity, and changed the expression patterns of the intestinal crypt towards epithelial differentiation and stem cell regulation. Naproxen demonstrated robust chemopreventive activity in a mouse co-clinical trial and gene expression profiles induced by naproxen in humans showed perfect discrimination of mice specimens with LS and PDOs treated with naproxen and control.ConclusionsNaproxen is a promising strategy for immune interception in LS. We have discovered naproxen-induced gene expression profiles for their potential use as predictive biomarkers of drug activity.Trial registration numbergov Identifier: NCT02052908.

Published

2021

49. Relation of NSAIDs, DMARDs, and TNF Inhibitors for Ankylosing Spondylitis and Psoriatic Arthritis to Risk of Total Hip and Knee Arthroplasty.

Author

Stovall, Rachael, Stovall, Rachael, Peloquin, Christine, Felson, David, Neogi, Tuhina, Dubreuil, Maureen, Stovall, Rachael, Stovall, Rachael, Peloquin, Christine, Felson, David, Neogi, Tuhina, and Dubreuil, Maureen

Abstract

ObjectiveAnkylosing spondylitis (AS) and psoriatic arthritis (PsA) often affect the hip and/or knee. If effective, treatments might reduce risk of total hip or total knee arthroplasty (THA/TKA). We evaluated risk of THA/TKA related to use of medical therapies in AS/PsA.MethodsWe conducted a nested case-control study using 1994-2018 data from the OptumLabs Data Warehouse, which includes deidentified medical and pharmacy claims, laboratory results, and enrollment records for commercial and Medicare Advantage enrollees. Among those with AS/PsA, THA/TKA cases were matched up to 4 controls by sex, age, AS/PsA diagnosis, diagnosis year, insurance type, obesity, and prior THA/TKA. We assessed AS/PsA treatment 6 months prior to THA/TKA, including disease-modifying antirheumatic drugs (DMARDs) and tumor necrosis factor inhibitors (TNFi), alone or in combination, stratified by nonsteroidal antiinflammatory drug (NSAID) use. We evaluated the relation of treatment to risk of THA/TKA using conditional logistical regression with adjustment for confounders.ResultsAmong 16,748 adults with AS, there were 444 THA/TKA cases and 1613 matched controls. Among 34,512 adults with PsA, there were 1003 cases and 3793 controls. Adjusted ORs for treatment category and THA/TKA ranged from 0.60 to 1.92; however, none were statistically significant. Results were similarly null in several sensitivity analyses.ConclusionOdds of THA/TKA were not reduced with any combinations of NSAIDs, DMARDs, or TNFi among persons with AS or PsA. Given current utilization patterns in this population of US adults with AS and PsA, these medical therapies did not appear to be associated with less end-stage peripheral joint damage.

Published

2021

50. Knee Osteoarthritis, Potential Mediators, and Risk of All-Cause Mortality: Data From the Osteoarthritis Initiative.

Author

Wang, Yilun, Wang, Yilun, Nguyen, Uyen-Sa DT, Lane, Nancy E, Lu, Na, Wei, Jie, Lei, Guanghua, Zeng, Chao, Zhang, Yuqing, Wang, Yilun, Wang, Yilun, Nguyen, Uyen-Sa DT, Lane, Nancy E, Lu, Na, Wei, Jie, Lei, Guanghua, Zeng, Chao, and Zhang, Yuqing

Abstract

ObjectiveTo assess the relation of symptomatic knee osteoarthritis (OA), knee pain, and radiographic knee OA to All-cause mortality and to identify mediators in the causal pathway.MethodsParticipants from the Osteoarthritis Initiative were divided into 4 groups: 1) symptomatic knee OA (i.e., both radiographic knee OA [Kellgren/Lawrence grade ≥2] and knee pain); 2) knee pain only; 3) radiographic knee OA only; and 4) neither radiographic knee OA nor knee pain. We examined the relation of knee OA status to All-cause mortality using a multivariable Cox proportional hazards model and assessed the extent to which the association was mediated by disability, physical component summary (PCS) and mental component summary (MCS) scores for quality of life (QoL), and use of oral pain-relief medications (i.e., nonsteroidal antiinflammatory drugs and opioids).ResultsAmong 4,796 participants, 282 died over the 96-month follow-up period. Compared with those with neither radiographic knee OA nor knee pain, multivariable-adjusted hazard ratios (HRs) of mortality were 2.2 (95% confidence interval [95% CI] 1.6-3.1) for symptomatic knee OA, 0.9 (95% CI 0.6-1.4) for knee pain only, and 2.0 (95% CI 1.4-2.9) for radiographic knee OA only, respectively. Indirect effects (HRs) of symptomatic knee OA on mortality via disability and PCS of QoL were 1.1 (95% CI 1.0-1.4) and 1.2 (95% CI 1.0-1.4), respectively. No apparent mediation effect was observed through either MCS of QoL or oral pain-relief medications use.ConclusionParticipants with either symptomatic or radiographic knee OA were at an increased risk of All-cause mortality. Increased risk of mortality from symptomatic knee OA was partially mediated through its effect on disability and PCS of QoL.

Published

2021