Your search keyword '"Benson CT"' showing total 213 results

1. GLP-1 receptor agonist-based therapies and cardiovascular risk: a review of mechanisms.

Author

Mullur, Neerav, Morissette, Arianne, Morrow, Nadya M., and Mulvihill, Erin E.

Subjects

GLUCAGON-like peptide 1, GLUCAGON receptors, ANTIOBESITY agents, TYPE 2 diabetes, CARDIOVASCULAR system

Abstract

Cardiovascular outcome trials (CVOTs) in people living with type 2 diabetes mellitus and obesity have confirmed the cardiovascular benefits of glucagon-like peptide 1 receptor agonists (GLP-1RAs), including reduced cardiovascular mortality, lower rates of myocardial infarction, and lower rates of stroke. The cardiovascular benefits observed following GLP-1RA treatment could be secondary to improvements in glycemia, blood pressure, postprandial lipidemia, and inflammation. Yet, the GLP-1R is also expressed in the heart and vasculature, suggesting that GLP-1R agonism may impact the cardiovascular system. The emergence of GLP-1RAs combined with glucose-dependent insulinotropic polypeptide and glucagon receptor agonists has shown promising results as new weight loss medications. Dual-agonist and tri-agonist therapies have demonstrated superior outcomes in weight loss, lowered blood sugar and lipid levels, restoration of tissue function, and enhancement of overall substrate metabolism compared to using GLP-1R agonists alone. However, the precise mechanisms underlying their cardiovascular benefits remain to be fully elucidated. This review aims to summarize the findings from CVOTs of GLP-1RAs, explore the latest data on dual and tri-agonist therapies, and delve into potential mechanisms contributing to their cardioprotective effects. It also addresses current gaps in understanding and areas for further research. [ABSTRACT FROM AUTHOR]

Published

2024

2. Tirzepatide a novel anti diabetic molecule unfold dual action.

Author

Sweta, Gupta, Sumeet, Bansal, Seema, Devi, Siwani, Sharma, Sheenam, Laxmi, and Deepa

Subjects

CARDIOVASCULAR disease prevention, KIDNEY disease prevention, GLUCAGON-like peptide-1 agonists, NON-alcoholic fatty liver disease, INCRETINS, GLYCEMIC control, BODY weight, PANCREATIC beta cells, HYPOGLYCEMIC agents, INSULIN, GASTROINTESTINAL hormones, PHARMACY information services, TYPE 2 diabetes, MOLECULAR structure, DRUG interactions, DRUG efficacy, OBESITY, CELL receptors, PHARMACODYNAMICS, CHEMICAL inhibitors

Abstract

This review article provides an in-depth examination of various aspects related to tirzepatide, a synthetic peptide given the positive signal by the "United States Food and Drug Administration" for managing type 2 diabetes. Beginning with an overview of diabetes introduction, epidemiology, and issues related to β-cell dysfunction, is explored in the narrative. It further delves into the significance of incretins in the context of diabetes and introduces tirzepatide as a novel "twincretin" owing to its dual agonistic activity on the glucagon-like peptide 1 (GLP-1) and gastric inhibitory polypeptide (GIP) receptors. The document delves into the chemistry and structure of tirzepatide, providing insights into its unique composition of 39 amino acids derived from native GLP-1, GIP, and semaglutide sequences. Tirzepatide's pharmacology, with a focus on its pharmacokinetic characteristics, and its mechanism of action (MOA) are extensively discussed. Notably, tirzepatide exhibits a preference for GIP receptors, leading to effective reduction of hyperglycemia and positive effects on pancreatic β-cells. Clinical trials examining tirzepatide's impact on glycemic and obesity control are detailed, demonstrating its efficacy in reducing body weight and appetite. Furthermore, the review article explores tirzepatide's effects on cardiovascular and kidney function, highlighting potential renal benefits for diabetic and elevated cardiovascular risk individuals. The narrative also addresses the association between tirzepatide and NAFLD, emphasizing potential benefits in mitigating NAFLD outcomes. Additionally, a comprehensive overview of tirzepatide's side effects, supported by scientific trials, is presented in this article. In conclusion, this review article provides a thorough examination of tirzepatide's multifaceted impact on diabetes management, shedding light on its pharmacological properties, clinical implications, and potential side effects. The information presented contributes to a comprehensive understanding of tirzepatide's role in the evolving landscape of T2D therapeutics. [ABSTRACT FROM AUTHOR]

Published

2024

3. Gut hormone multi-agonists for the treatment of type 2 diabetes and obesity: advances and challenges.

Author

Xianxian Huang, Jing Liu, Guangquan Peng, Mingyue Lu, Zhongbo Zhou, Neng Jiang, and Zhiming Yan

Subjects

TYPE 2 diabetes, GLUCAGON receptors, GASTROINTESTINAL hormones, WEIGHT loss, HORMONE receptors, GLUCAGON-like peptide-1 agonists, GASTRIC inhibitory polypeptide

Abstract

The rapidly rising incidence of obesity, coupled with type 2 diabetes mellitus (T2DM), is a growing concern. Glucagonlike peptide 1 (GLP-1), an endogenous peptide secreted by enteroendocrine L-cells, demonstrates exceptional pharmacological potential for the treatment of T2DM and obesity, primarily through its pivotal roles in regulating glucose homeostasis, stimulating glucose-dependent insulin secretion, and promoting satiety. Considering its proven efficacy in glucoregulation and weight loss, GLP-1 receptor agonists (GLP-1RAs) have emerged as a revolutionary breakthrough in the arena of diabetes management and weight control. Additional gastrointestinal hormones, such as glucose-dependent insulinotropic peptide (GIP) and glucagon, exhibit structural similarities to GLP-1 and work synergistically to lower blood glucose levels or aid in weight loss. Today, various classes of gut hormone receptor multiple agonists are steadily progressing through development and clinical trials, including dual GLP-1/glucagon receptor agonists (first discovered in 2009), dual GLP-1/GIP receptor agonists (first described in 2013), and triple GLP-1/GIP/glucagon receptor agonists (initially designed in 2015). The GLP-1/GIP receptor co-agonist, tirzepatide, was approved by the U.S. Food and Drug Administration (FDA) for the treatment of T2DM, outperforming basal insulin or selective GLP-1RAs by providing superior HbA1c reductions. Remarkably, tirzepatide also facilitated unprecedented weight loss of up to 22.5% in non-diabetic individuals living with obesity. This result is comparable to those achieved with certain types of bariatric surgery. Therefore, the advent of gut hormone multi-agonists signifies the dawn of an exciting new era in peptide-based therapy for obesity and T2DM. This review offers a comprehensive summary of the various types of gut hormone multiple agonists, including their discovery, development, action of mechanisms, and clinical effectiveness. We further delve into potential hurdles, limitations, and prospective advancements in the field. [ABSTRACT FROM AUTHOR]

Published

2024

4. Relationship Between Osteoporosis and Serum Sclerostin Levels in Kidney Transplant Recipients.

Author

Basir, Hasan, Altunoren, Orcun, Erken, Ertugrul, Kilinc, Metin, Sarisik, Feyza Nur, Isiktas, Songul, and Gungor, Ozkan

Published

2024

5. Reduced incretin receptor trafficking upon activation enhances glycemic control and reverses obesity in diet-induced obese mice.

Author

Bauri, Rathin, Bele, Shilpak, Edelli, Jhansi, Reddy, Neelesh C., Kurukuti, Sreenivasulu, Devasia, Tom, Ibrahim, Ahamed, Rai, Vishal, and Mitra, Prasenjit

Subjects

GLYCEMIC control, INSULIN, GLUCAGON-like peptide-1 receptor, N-terminal residues, INSULIN receptors, PEPTIDES, OBESITY, INSULIN derivatives

Abstract

Activation of incretin receptors by their cognate agonist augments sustained cAMP generation both from the plasma membrane as well as from the endosome. To address the functional outcome of this spatiotemporal signaling, we developed a nonacylated glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP) receptor dual agonist I-M-150847 that reduced receptor internalization following activation of the incretin receptors. The incretin receptor dual agonist I-M-150847 was developed by replacing the tryptophan cage of exendin-4 tyrosine substituted at the amino terminus with the C-terminal undecapeptide sequence of oxyntomodulin that placed lysine 30 of I-M-150847 in frame with the corresponding lysine residue of GIP. The peptide I-M-150847 is a partial agonist of GLP-1R and GIPR; however, the receptors, upon activation by I-M-150847, undergo reduced internalization that promotes agonist-mediated iterative cAMP signaling and augments glucose-stimulated insulin exocytosis in pancreatic β cells. Chronic administration of I-M-150847 improved glycemic control, enhanced insulin sensitivity, and provided profound weight loss in diet-induced obese (DIO) mice. Our results demonstrated that despite being a partial agonist, I-M-150847, by reducing the receptor internalization upon activation, enhanced the incretin effect and reversed obesity. NEW & NOTEWORTHY: Replacement of the tryptophan cage (Trp-cage) with the C-terminal oxyntomodulin undecapeptide along with the tyrosine substitution at the amino terminus converts the selective glucagon-like peptide-1 receptor (GLP-1R) agonist exendin-4 to a novel GLP-1R and GIPR dual agonist I-M-150847. Reduced internalization of incretin receptors upon activation by the GLP-1R and GIPR dual agonist I-M-150847 promotes iterative receptor signaling that enhances the incretin effect and reverses obesity. [ABSTRACT FROM AUTHOR]

Published

2024

6. Pharmacological Advances in Incretin-Based Polyagonism: What We Know and What We Don't.

Author

Novikoff, Aaron and Müller, Timo D.

Subjects

GLUCAGON-like peptide-1 receptor, GLUCAGON-like peptide-1 agonists, TYPE 2 diabetes, GLUCOSE metabolism, ENERGY metabolism

Abstract

The prevalence of obesity continues to rise in both adolescents and adults, in parallel obesity is strongly associated with the increased incidence of type 2 diabetes, heart failure, certain types of cancer, and all-cause mortality. In relation to obesity, many pharmacological approaches of the past have tried and failed to combat the rising obesity epidemic, particularly due to insufficient efficacy or unacceptable side effects. However, while the history of antiobesity medication is plagued by failures and disappointments, we have witnessed over the last 10 years substantial progress, particularly in regard to biochemically optimized agonists at the receptor for glucagon-like peptide-1 (GLP-1R) and unimolecular coagonists at the receptors for GLP-1 and the glucose-dependent insulinotropic polypeptide (GIP). Although the GIP receptor:GLP-1R coagonists are being heralded as premier pharmacological tools for the treatment of obesity and diabetes, uncertainty remains as to why these drugs testify superiority over best-in-class GLP-1R monoagonists. Particularly with regard to GIP, there remains great uncertainty if and how GIP acts on systems metabolism and if the GIP system should be activated or inhibited to improve metabolic outcome in adjunct to GLP-1R agonism. In this review, we summarize recent advances in GLP-1- and GIP-based pharmacology and discuss recent findings and open questions related to how the GIP system affects systemic energy and glucose metabolism. [ABSTRACT FROM AUTHOR]

Published

2024

7. The antiemetic actions of GIP receptor agonism.

Author

Borner, Tito, De Jonghe, Bart C., and Hayes, Matthew R.

Subjects

GASTRIC inhibitory polypeptide, ANTIEMETICS, TERMINATION of treatment, GLUCAGON-like peptide-1 receptor, REGULATION of body weight, VOMITING

Abstract

Nausea and vomiting are primitive aspects of mammalian physiology and behavior that ensure survival. Unfortunately, both are ubiquitously present side effects of drug treatments for many chronic diseases with negative consequences on pharmacotherapy tolerance, quality of life, and prognosis. One of the most critical clinical examples is the profound emesis and nausea that occur in patients undergoing chemotherapy, which continue to be among the most distressing side effects, even with the use of modern antiemetic medications. Similarly, antiobesity/diabetes medications that target the glucagon-like peptide-1 system, despite their remarkable metabolic success, also cause nausea and vomiting in a significant number of patients. These side effects hinder the ability to administer higher dosages for optimal glycemic and weight management and represent the major reasons for treatment discontinuation. Our inability to effectively control these side effects highlights the need to anatomically, molecularly, and functionally characterize novel neural substrates that drive and inhibit nausea and emesis. Here, we discuss clinical and preclinical evidence that highlights the glucose-dependent insulinotropic peptide receptor system as a novel therapeutic central target for the management of nausea and emesis. [ABSTRACT FROM AUTHOR]

Published

2024

8. Population pharmacokinetics of the GIP/GLP receptor agonist tirzepatide.

Author

Schneck, Karen and Urva, Shweta

Subjects

GLUCAGON-like peptide-1 receptor, TYPE 2 diabetes, GLUCAGON-like peptide-1 agonists, PHARMACOKINETICS, ALLOMETRY, PEPTIDE receptors, BODY size, GLUCAGON receptors

Abstract

Tirzepatide is a first‐in‐class glucose‐dependent insulinotropic polypeptide and glucagon‐like peptide‐1 receptor agonist approved as for the treatment of type 2 diabetes mellitus. A population‐based pharmacokinetic (PK) model was developed from 19 pooled studies. Tirzepatide pharmacokinetics were well‐described by a two‐compartment model with first order absorption and elimination. The tirzepatide population PK model utilized a semimechanistic allometry model to describe the relationship between body size and tirzepatide PK. The half‐life of tirzepatide was ~5 days and enabled sustained exposure with once‐weekly subcutaneous dosing. The covariate analysis suggested that adjustment of the dose regimen based on demographics or subpopulations was unnecessary. The tirzepatide PK model can be used to predict tirzepatide exposure for various scenarios or populations. [ABSTRACT FROM AUTHOR]

Published

2024

9. Reduction of prevalence of patients meeting the criteria for metabolic syndrome with tirzepatide: a post hoc analysis from the SURPASS Clinical Trial Program.

Author

Nicholls, Stephen J., Tofé, Santiago, le Roux, Carel W., D'Alessio, David A., Wiese, Russell J., Pavo, Imre, Brown, Katelyn, Weerakkody, Govinda J., Zeytinoglu, Meltem, and Romera, Irene C.

Subjects

METABOLIC syndrome, WEIGHT loss, DYSLIPIDEMIA, CARDIOVASCULAR diseases risk factors, CLINICAL trials, INSULIN resistance

Abstract

Background: Metabolic syndrome is characterized as the co-occurrence of interrelated cardiovascular risk factors, including insulin resistance, hyperinsulinemia, abdominal obesity, dyslipidemia and hypertension. Once weekly tirzepatide is approved in the US and EU for the treatment of type 2 diabetes (T2D) and obesity. In the SURPASS clinical trial program for T2D, tirzepatide demonstrated greater improvements in glycemic control, body weight reduction and other cardiometabolic risk factors versus placebo, subcutaneous semaglutide 1 mg, insulin degludec, and insulin glargine. This post hoc analysis assessed the effect of tirzepatide use on the prevalence of patients meeting the criteria for metabolic syndrome across SURPASS 1–5. Methods: Metabolic syndrome was defined as having ≥ 3 of 5 criteria according to the US National Cholesterol Education Program: Adult Treatment Panel III. Analyses were based on on-treatment data at the primary endpoint from patients adherent to treatment (taking ≥ 75% study drug). A logistic regression model with metabolic syndrome status as the response variable, metabolic syndrome status at the baseline visit as an adjustment, and randomized treatment as fixed explanatory effect was used. The effect of tirzepatide use on the prevalence of patients meeting the criteria for metabolic syndrome by categorical weight loss, background medication and gender were assessed. Results: In SURPASS, the prevalence of patients meeting the criteria for metabolic syndrome at baseline was 67–88% across treatment groups with reductions at the primary endpoint to 38–64% with tirzepatide versus 64–82% with comparators. Reductions in the prevalence of patients meeting the criteria for metabolic syndrome was significantly greater with all tirzepatide doses versus placebo, semaglutide 1 mg, insulin glargine, and insulin degludec (p < 0.001). Individual components of metabolic syndrome were also reduced to a greater extent with tirzepatide vs comparators. Greater reductions in body weight were associated with greater reductions in the prevalence of patients meeting the criteria for metabolic syndrome and its individual components. Background SGLT2i or sulfonylurea use or gender did not impact the change in prevalence of patients meeting the criteria for metabolic syndrome. Conclusions: In this post hoc analysis, tirzepatide at all doses studied was associated with a greater reduction in the prevalence of patients meeting the criteria for metabolic syndrome compared to placebo, semaglutide 1 mg, insulin degludec, and insulin glargine. Although more evidence is needed, these data would support greater potential improvement in cardiovascular risk factor profile with tirzepatide treatment in people across the continuum of T2D. [ABSTRACT FROM AUTHOR]

Published

2024

10. The Body weight Reducing Effects of Tirzepatide in People with and without Type 2 Diabetes: A Review on Efficacy and Adverse Effects.

Author

Jensen, Thomas Leth, Brønden, Andreas, Karstoft, Kristian, Sonne, David Peick, and Christensen, Mikkel Bring

Subjects

WEIGHT loss, TYPE 2 diabetes, BODY weight, POSTOPERATIVE nausea & vomiting, GLYCEMIC control, GLYCOSYLATED hemoglobin

Abstract

Obesity is becoming more frequent and has several negative health impacts. Recent advances in weight management strategies have primarily resided in pharmaceutical treatments, and the glucagon-like peptide-1 (GLP-1) receptor agonists have shown great potential in terms of body weight reduction in addition to improving glycemic control in patients with type 2 diabetes (T2D). Recently, the dual GLP-1 and glucose-dependent insulinotropic polypeptide (GIP) receptor agonist tirzepatide has been developed. Tirzepatide has shown strong effects on glycated hemoglobin (HbA1C) levels in several clinical trials including participants with T2D (SURPASS program). In addition to its lowering effect on HbA1C, tirzepatide leads to substantial reductions in body weight, and a series of clinical trials (SURMOUNT program) have investigated the effects on body weight as the primary outcome. In these two trial programs, tirzepatide in doses of 5 mg to 15 mg administered subcutaneously once weekly resulted in body weight reduction of up to 15% in participants with T2D and up to 21% in participants without T2D, despite comparable baseline bodyweight. Across the two trial programs, adverse effects were mainly gastrointestinal (nausea, diarrhea, and vomiting) occurring with similar incidences of vomiting and lower incidences of diarrhea and nausea in trial participants with T2D compared to trials participants without T2D. Overall, discontinuation due to adverse events occurred in 3– 7% of participants with no major differences between individuals with and without T2D. The higher weight-reducing efficacy of tirzepatide in trial participants without T2D is currently unexplained and may be partly reflected in dissimilarities in frequencies of gastrointestinal adverse events. The weight reducing effects of tirzepatide hold great promise for weight management in obese patients regardless of the presence of T2D. [ABSTRACT FROM AUTHOR]

Published

2024

11. Safety, pharmacokinetics, and target engagement of a brain penetrant RIPK1 inhibitor, SAR443820 (DNL788), in healthy adult participants.

Author

Hincelin‐Mery, Agnes, Nicolas, Xavier, Cantalloube, Cathy, Pomponio, Robert, Lewanczyk, Pascale, Benamor, Myriam, Ofengeim, Dimitry, Krupka, Emmanuel, Hsiao‐Nakamoto, Jennifer, Eastenson, Amy, and Atassi, Nazem

Subjects

AMYOTROPHIC lateral sclerosis, PHARMACOKINETICS, CEREBROSPINAL fluid examination, TERMINATION of treatment, PROTEIN kinases, MULTIPLE sclerosis

Abstract

SAR443820 (DNL788) is a selective, orally bioavailable, brain penetrant inhibitor of receptor‐interacting serine/threonine protein kinase 1 (RIPK1). This phase I first‐in‐human healthy participant study (NCT05795907) was comprised of three parts: randomized, double‐blind, placebo‐controlled single ascending dose (SAD; part 1a); 14‐day multiple ascending dose (MAD; part 2) parts that evaluated safety, tolerability, pharmacokinetics (PK), and pharmacodynamics of SAR443820; and a separate open‐label, single‐dose part 1b (PK‐cerebrospinal fluid [CSF]) to assess SAR443820 levels in CSF. SAR443820 was well‐tolerated in healthy participants, and no treatment discontinuation related to an adverse event (AE) occurred. Most common AEs were dizziness and headache. No clinically meaningful changes were noted in laboratory values, vital signs, or electrocardiogram parameters. SAR443820 had a favorable PK profile, with plasma half‐lives (geometric mean) ranged between 5.7–8.0 h and 7.2–8.9 h after single and repeated doses, respectively. There were no major deviations from dose proportionality for maximum concentration and area under the curve across SAR443820 doses. Mean CSF‐to‐unbound plasma concentration ratio ranged from 0.8 to 1.3 over time (assessed up to 10 h postdose), indicating high brain penetrance. High levels of inhibition of activated RIPK1, as measured by decrease in pS166‐RIPK1, were achieved in both SAD and MAD parts, with a maximum median inhibition from baseline close to 90% at predose (Ctrough) after multiple dosing in MAD, reflecting a marked RIPK1 target engagement at the peripheral level. These results support further development of SAR443820 in phase II trials in amyotrophic lateral sclerosis (NCT05237284) and multiple sclerosis (NCT05630547). [ABSTRACT FROM AUTHOR]

Published

2024

12. Pizza and 2-Structures.

Author

Ehrenborg, Richard, Morel, Sophie, and Readdy, Margaret

Subjects

COXETER groups, PIZZA, ORBITS (Astronomy), POINT set theory, VALUATION

Abstract

Let H be a Coxeter hyperplane arrangement in n-dimensional Euclidean space. Assume that the negative of the identity map belongs to the associated Coxeter group W. Furthermore assume that the arrangement is not of type A 1 n . Let K be a measurable subset of the Euclidean space with finite volume which is stable by the Coxeter group W and let a be a point such that K contains the convex hull of the orbit of the point a under the group W. In a previous article the authors proved the generalized pizza theorem: that the alternating sum over the chambers T of H of the volumes of the intersections T ∩ (K + a) is zero. In this paper we give a dissection proof of this result. In fact, we lift the identity to an abstract dissection group to obtain a similar identity that replaces the volume by any valuation that is invariant under affine isometries. This includes the cases of all intrinsic volumes. Apart from basic geometry, the main ingredient is a theorem of the authors where we relate the alternating sum of the values of certain valuations over the chambers of a Coxeter arrangement to similar alternating sums for simpler subarrangements called 2-structures introduced by Herb to study discrete series characters of real reduced groups. [ABSTRACT FROM AUTHOR]

Published

2023

13. An Identity for the Coefficients of Characteristic Polynomials of Hyperplane Arrangements.

Author

Kabluchko, Zakhar

Subjects

METRIC projections, POLYNOMIALS, ABSOLUTE value, HYPERPLANES, EUCLIDEAN distance, MATHEMATICS

Abstract

Consider a finite collection of affine hyperplanes in R d . The hyperplanes dissect R d into finitely many polyhedral chambers. For a point x ∈ R d and a chamber P the metric projection of x onto P is the unique point y ∈ P minimizing the Euclidean distance to x. The metric projection is contained in the relative interior of a uniquely defined face of P whose dimension is denoted by dim (x , P) . We prove that for every given k ∈ { 0 , ... , d } , the number of chambers P for which dim (x , P) = k does not depend on the choice of x, with an exception of some Lebesgue null set. Moreover, this number is equal to the absolute value of the k-th coefficient of the characteristic polynomial of the hyperplane arrangement. In a special case of reflection arrangements, this proves a conjecture of Drton and Klivans [A geometric interpretation of the characteristic polynomial of reflection arrangements. Proc. Amer. Math. Soc. 138(8), 2873–2887 (2010)]. [ABSTRACT FROM AUTHOR]

Published

2023

14. Mechanisms of action of incretin receptor based dual- and tri-agonists in pancreatic islets.

Author

Folli, Franco, Finzi, Giovanna, Manfrini, Roberto, Galli, Alessandra, Casiraghi, Francesca, Centofanti, Lucia, Berra, Cesare, Fiorina, Paolo, Davalli, Alberto, Rosa, Stefano La, Perego, Carla, and Higgins, Paul B.

Subjects

GASTRIC inhibitory polypeptide, ISLANDS of Langerhans, GLUCAGON-like peptide-1 receptor, GLUCAGON receptors, PEPTIDE receptors, G protein coupled receptors

Abstract

Simultaneous activation of the incretin G-protein-coupled receptors (GPCRs) via unimolecular dual-receptor agonists (UDRA) has emerged as a new therapeutic approach for type 2 diabetes. Recent studies also advocate triple agonism with molecules also capable of binding the glucagon receptor. In this scoping review, we discuss the cellular mechanisms of action (MOA) underlying the actions of these novel and therapeutically important classes of peptide receptor agonists. Clinical efficacy studies of several UDRAs have demonstrated favorable results both as monotherapies and when combined with approved hypoglycemics. Although the additive insulinotropic effects of dual glucagon-like peptide-1 receptor (GLP-1R) and glucose-dependent insulinotropic peptide receptor (GIPR) agonism were anticipated based on the known actions of either glucagon-like peptide-1 (GLP-1) or glucose-dependent insulinotropic peptide (GIP) alone, the additional benefits from GCGR were largely unexpected. Whether additional synergistic or antagonistic interactions among these G-protein receptor signaling pathways arise from simultaneous stimulation is not known. The signaling pathways affected by dual- and tri-agonism require more trenchant investigation before a comprehensive understanding of the cellular MOA. This knowledge will be essential for understanding the chronic efficacy and safety of these treatments. [ABSTRACT FROM AUTHOR]

Published

2023

15. The New S7B/E14 Q&A Document Provides Additional Opportunities to Replace the Thorough QT Study.

Author

Darpo, Borje and Leishman, Derek J.

Subjects

CLINICAL drug trials, PHARMACOLOGY, INVESTIGATIONAL drugs, LONG QT syndrome, RISK assessment, MARKETING, ELECTROCARDIOGRAPHY, DRUG development, HEART conduction system, DISEASE risk factors

Abstract

Since 2015, concentration–QTc (C–QTc) analysis has been used to exclude the possibility that a drug has a concerning effect on the QTc interval. This has enabled the replacement of the designated thorough QT (TQT) study with serial electrocardiograms (ECGs) in routine clinical pharmacology studies, such as the first‐in‐human (FIH) study. The E14 revision has led to an increased proportion of FIH studies with the added objective of QT evaluation, with the intention of replacing the TQT study. With the more recent revision of the S7B/E14 Q&A document in February 2022, nonclinical assays/studies can be brought into the process of regulatory decisions at the time of marketing application. If the hERG (human ether‐a‐go‐go‐related gene) and the non‐rodent in vivo study are conducted according to the described best practices and are negative, the previous requirement that a QTc effect of >10 milliseconds must be excluded in healthy subjects at plasma concentrations 2‐fold above what can be seen in patients can be reduced to covering the concentrations seen in patients. For drugs that cannot be safely given in high doses to healthy subjects, ECG evaluation is often performed at the therapeutic dose in patients. If a QTc effect of >10 milliseconds can be excluded, an argument can be made that the drug should be considered as having a low likelihood of proarrhythmic effects due to delayedrepolarization, if supported by negative best practices hERG and in vivo studies. In this article, we describe what clinicians involved in early clinical development need to understand in terms of the hERG and in vivo studies to determine whether these meet best practices and therefore can be used in an integrated clinical/nonclinical QT/QTc risk assessment. [ABSTRACT FROM AUTHOR]

Published

2023

16. Synergistic Combinations of Gut- and Pancreas-Hormone-Based Therapies: Advancements in Treatments for Metabolic Diseases.

Author

Lyons, Sulayman Aslan and Beaudry, Jacqueline Leah

Subjects

METABOLIC disorder treatment, GLUCAGON-like peptide-1 agonists

Abstract

Metabolic diseases, such as obesity, type 2 diabetes mellitus (T2DM), cardiovascular disease, and liver disease, have become increasingly prevalent around the world. As an alternative to bariatric surgery, glucagon-like peptide 1 (GLP-1) receptor agonists have been at the forefront of weight loss medication to combat these metabolic complications. Recently, there has been an exciting rapid emergence of new weight loss medications that combine GLP-1 receptor (GLP-1R) agonists with other gut- and pancreatic-derived hormones, such as glucose-dependent insulinotropic polypeptide (GIP) and glucagon (GCG) receptor agonists. Dual-agonist (GLP-1/GIP and GLP-1/GCG) and tri-agonist (GLP-1/GIP/GCG) administration generally result in greater weight loss, reduction of blood sugar and lipid levels, restoration of tissue function, and improvement in whole-body substrate metabolism compared to when GLP-1R agonists are used alone. The aim of this review is to summarize the recent literature of both preclinical and clinical studies on how these emerging gut-peptide therapies further improve weight loss and metabolic health outcomes for various metabolic diseases. [ABSTRACT FROM AUTHOR]

Published

2023

17. "The Future Ain't What It Used to Be": Anesthesia Research, Practice, and Management in 2050.

Author

Pandit, Jaideep J.

Published

2024

18. A potential therapeutic drug for osteoporosis: prospect for osteogenic LncRNAs.

Author

Fanjin Meng, Yang Yu, Ye Tian, Meng Deng, Kaiyuan Zheng, Xiaolan Guo, Beilei Zeng, Jingjia Li, Airong Qian, and Chong Yin

Subjects

MICRORNA, BONE growth, GENOME editing, LINCRNA

Abstract

Long non-coding RNAs (LncRNAs) play essential roles in multiple physiological processes including bone formation. Investigators have revealed that LncRNAs regulated bone formation through various signaling pathways and micro RNAs (miRNAs). However, several problems exist in current research studies on osteogenic LncRNAs, including sophisticated techniques, high cost for in vivo experiment, as well as low homology of LncRNAs between animal model and human, which hindered translational medicine research. Moreover, compared with gene editing, LncRNAs would only lead to inhibition of target genes rather than completely knocking them out. As the studies on osteogenic LncRNA gradually proceed, some of these problems have turned osteogenic LncRNA research studies into slump. This review described some new techniques and innovative ideas to address these problems. Although investigations on osteogenic LncRNAs still have obtacles to overcome, LncRNA will work as a promising therapeutic drug for osteoporosis in the near future. [ABSTRACT FROM AUTHOR]

Published

2023

19. Sclerostin small-molecule inhibitors promote osteogenesis by activating canonical Wnt and BMP pathways.

Author

Sangadala, Sreedhara, Chi Heon Kim, Fernandes, Lorenzo M., Makkar, Pooja, Beck, George R., Boden, Scott D., Drissi, Hicham, and Presciutti, Steven M.

Published

2023

20. Development of consensus-driven SPIRIT and CONSORT extensions for early phase dose-finding trials: the DEFINE study.

Author

Solovyeva, Olga, Dimairo, Munyaradzi, Weir, Christopher J., Hee, Siew Wan, Espinasse, Aude, Ursino, Moreno, Patel, Dhrusti, Kightley, Andrew, Hughes, Sarah, Jaki, Thomas, Mander, Adrian, Evans, Thomas R. Jeffry, Lee, Shing, Hopewell, Sally, Rantell, Khadija Rerhou, Chan, An-Wen, Bedding, Alun, Stephens, Richard, Richards, Dawn, and Roberts, Lesley

Subjects

CRIME & the press, GREY literature, THEMATIC analysis, MEDICAL protocols, QUANTITATIVE research

Abstract

Background: Early phase dose-finding (EPDF) trials are crucial for the development of a new intervention and influence whether it should be investigated in further trials. Guidance exists for clinical trial protocols and completed trial reports in the SPIRIT and CONSORT guidelines, respectively. However, both guidelines and their extensions do not adequately address the characteristics of EPDF trials. Building on the SPIRIT and CONSORT checklists, the DEFINE study aims to develop international consensus-driven guidelines for EPDF trial protocols (SPIRIT-DEFINE) and reports (CONSORT-DEFINE). Methods: The initial generation of candidate items was informed by reviewing published EPDF trial reports. The early draft items were refined further through a review of the published and grey literature, analysis of real-world examples, citation and reference searches, and expert recommendations, followed by a two-round modified Delphi process. Patient and public involvement and engagement (PPIE) was pursued concurrently with the quantitative and thematic analysis of Delphi participants' feedback. Results: The Delphi survey included 79 new or modified SPIRIT-DEFINE (n = 36) and CONSORT-DEFINE (n = 43) extension candidate items. In Round One, 206 interdisciplinary stakeholders from 24 countries voted and 151 stakeholders voted in Round Two. Following Round One feedback, one item for CONSORT-DEFINE was added in Round Two. Of the 80 items, 60 met the threshold for inclusion (≥ 70% of respondents voted critical: 26 SPIRIT-DEFINE, 34 CONSORT-DEFINE), with the remaining 20 items to be further discussed at the consensus meeting. The parallel PPIE work resulted in the development of an EPDF lay summary toolkit consisting of a template with guidance notes and an exemplar. Conclusions: By detailing the development journey of the DEFINE study and the decisions undertaken, we envision that this will enhance understanding and help researchers in the development of future guidelines. The SPIRIT-DEFINE and CONSORT-DEFINE guidelines will allow investigators to effectively address essential items that should be present in EPDF trial protocols and reports, thereby promoting transparency, comprehensiveness, and reproducibility. Trial registration: SPIRIT-DEFINE and CONSORT-DEFINE are registered with the EQUATOR Network (https://www.equator-network.org/). [ABSTRACT FROM AUTHOR]

Published

2023

21. Molecular changes in skeletal muscle in chronic kidney disease: A systematic review.

Author

Wong, Limy, Kenny, Rachel, Howard, Jennifer, and McMahon, Lawrence P.

Published

2023

22. Medikamentöse Therapie der Adipositas – Konkurrenz zur bariatrischen Chirurgie oder sinnvolle Ergänzung?

Author

Mazaheri, Tina, Ansari, Saleem, Nallagonda, Madhavi, Kollmann, Lars, Nickel, Felix, Seyfried, Florian, and Miras, Alexander Dimitri

Abstract

Copyright of Chirurgie (2731-6971) is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

23. Novel insights on the effect of sclerostin on bone and other organs.

Author

Dreyer, Timothy J., Keen, Jacob A. C., Wells, Leah M., and Roberts, Scott J.

Subjects

SCLEROSTIN, CHRONIC kidney failure, BONE remodeling, BONE growth, BONE diseases

Abstract

As a key regulator of bone homeostasis, sclerostin has garnered a lot of interest over the last two decades. Although sclerostin is primarily expressed by osteocytes and is well known for its role in bone formation and remodelling, it is also expressed by a number of other cells and potentially plays a role in other organs. Herein, we aim to bring together recent sclerostin research and discuss the effect of sclerostin on bone, cartilage, muscle, liver, kidney and the cardiovascular and immune systems. Particular focus is placed on its role in diseases, such as osteoporosis and myeloma bone disease, and the novel development of sclerostin as a therapeutic target. Anti-sclerostin antibodies have recently been approved for the treatment of osteoporosis. However, a cardiovascular signal was observed, prompting extensive research into the role of sclerostin in vascular and bone tissue crosstalk. The study of sclerostin expression in chronic kidney disease was followed by the investigation of its role in liver–lipid– bone interactions, and the recent discovery of sclerostin as a myokine prompted new research into sclerostin within the bone–muscle relationship. Potentially, the effects of sclerostin reach beyond that of bone alone. We further summarise recent developments in the use of sclerostin as a potential therapeutic for osteoarthritis, osteosarcoma and sclerosteosis. Overall, these new treatments and discoveries illustrate progress within the field, however, also highlight remaining gaps in our knowledge. [ABSTRACT FROM AUTHOR]

Published

2023

24. Crosstalk between bone and muscle in chronic kidney disease.

Author

Wong, Limy and McMahon, Lawrence P.

Subjects

CHRONIC kidney failure, MUSCLE metabolism, MUSCULOSKELETAL system, ENDOCRINE system, EXERCISE therapy, BONE metabolism

Abstract

With increasing life expectancy, the related disorders of bone loss, metabolic dysregulation and sarcopenia have become major health threats to the elderly. Each of these conditions is prevalent in patients with chronic kidney disease (CKD), particularly in more advanced stages. Our current understanding of the bone-muscle interaction is beyond mechanical coupling, where bone and muscle have been identified as interrelated secretory organs, and regulation of both bone and muscle metabolism occurs through osteokines and myokines via autocrine, paracrine and endocrine systems. This review appraises the current knowledge regarding biochemical crosstalk between bone and muscle, and considers recent progress related to the role of osteokines and myokines in CKD, including modulatory effects of physical exercise and potential therapeutic targets to improve musculoskeletal health in CKD patients. [ABSTRACT FROM AUTHOR]

Published

2023

25. Multiple doses of SHR-1222, a sclerostin monoclonal antibody, in postmenopausal women with osteoporosis: A randomized, double-blind, placebocontrolled, dose-escalation phase 1 trial.

Author

Zhijie Dai, Ronghua Zhu, Zhifeng Sheng, Guijun Qin, Xianghang Luo, Qun Qin, Chunli Song, Liping Li, Ping Jin, Guoping Yang, Yanxiang Cheng, Danhong Peng, Chong Zou, Lijuan Wang, Jianzhong Shentu, Qin Zhang, Zhe Zhang, Xiang Yan, Pingfei Fang, and Qiangyong Yan

Subjects

TERIPARATIDE, OSTEOPOROSIS in women, SCLEROSTIN, MONOCLONAL antibodies, POSTMENOPAUSE, BONE growth

Abstract

SHR-1222, a novel humanized monoclonal antibody targeting sclerostin, has been shown to induce bone formation and decrease bone resorption at a single dose ranging 50-400 mg in our previous phase 1 trial. This study was a randomized, double-blind, placebo-controlled, dose-escalation phase 1 trial, which further investigated the safety, tolerability, pharmacokinetics (PK), pharmacodynamics (PD), and immunogenicity of multiple ascending doses of SHR-1222 in women with postmenopausal osteoporosis (POP). A total of 105 women with POP were enrolled and randomly assigned. Twenty-one received placebo and eighty-four received SHR-1222 sequentially (100 mg QM, n=4; 200 or 300 mg QM, n=20; and 400 or 600 mg Q2M, n=20). The most common adverse events included increased blood parathyroid hormone, increased low-density lipoprotein, increased blood alkaline phosphatase, increased blood cholesterol, back pain, and arthralgia, the majority of which were mild in severity without noticeable safety concerns. Serum SHR-1222 exposure (Cmax,ss and AUC0-tau,ss) increased in a greater than dose-proportional manner. Following multiple doses of SHR-1222, the bone formation markers (terminal propeptide of type I procollagen, bonespecific alkaline phosphatase, and osteocalcin) increased in a dosedependent manner, whereas the bone resorption marker (b-C-telopeptide) was downregulated. Accordingly, BMD gains in the lumbar spine, total hip, and femoral neck were observed. The maximum BMD increase from baseline at the lumbar spine was detected in the 300 mg QM cohort (14.6% vs. 0.6% in the placebo group on day 169). Six (6/83; 7.2%) subjects developed anti-SHR- 1222 antibodies with no discernible effects on PKs, PDs, and safety. Thus, multiple doses of SHR-1222 showed an acceptable safety profile and dosedependent plasma exposure in women with POP, and could improve their BMD rapidly and prominently by promoting bone formation and inhibiting bone resorption. These findings further support SHR-1222 as a potential alternative agent for the treatment of POP. [ABSTRACT FROM AUTHOR]

Published

2023

26. Cardiovascular effects of incretins: focus on glucagon-like peptide-1 receptor agonists.

Author

Madsbad, Sten and Holst, Jens J

Subjects

GLUCAGON-like peptide-1 receptor, GLUCAGON-like peptide-1 agonists, WEIGHT loss, DIABETIC nephropathies, CARDIOVASCULAR diseases risk factors

Abstract

Glucagon-like peptide-1 receptor agonists (GLP-1 RAs) have been used to treat patients with type 2 diabetes since 2005 and have become popular because of the efficacy and durability in relation to glycaemic control in combination with weight loss in most patients. Today in 2022, seven GLP-1 RAs, including oral semaglutide are available for treatment of type 2 diabetes. Since the efficacy in relation to reduction of HbA1c and body weight as well as tolerability and dosing frequency vary between agents, the GLP-1 RAs cannot be considered equal. The short acting lixisenatide showed no cardiovascular benefits, while once daily liraglutide and the weekly agonists, subcutaneous semaglutide, dulaglutide, and efpeglenatide, all lowered the incidence of cardiovascular events. Liraglutide, oral semaglutide and exenatide once weekly also reduced mortality. GLP-1 RAs reduce the progression of diabetic kidney disease. In the 2019 consensus report from European Association for the Study of Diabetes/American Diabetes Association, GLP-1 RAs with demonstrated cardio-renal benefits (liraglutide, semaglutide and dulaglutide) are recommended after metformin to patients with established cardiovascular diseases or multiple cardiovascular risk factors. European Society of Cardiology suggests starting with a sodium-glucose cotransprter-2 inhibitor or a GLP-1 RA in drug naïve patients with type 2 diabetes (T2D) and atherosclerotic cardiovascular disease (CVD) or high CV Risk. However, the results from cardiovascular outcome trials (CVOT) are very heterogeneous suggesting that some GLP-1RAs are more suitable to prevent CVD than others. The CVOTs provide a basis upon which individual treatment decisions for patients with T2D and CVD can be made. [ABSTRACT FROM AUTHOR]

Published

2023

27. Η επίδραση των νεότερων αντιδιαβητικών παραγόντων στην μη αλκοολική λιπώδης νόσος του ήπατος

Author

Εμινίδου, Βαλέρια and Παπαζαφειροπούλου, Αθανασία

Abstract

Copyright of Scientific Chronicles / Epistimonika Chronika is the property of Tzaneio General Hospital and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

28. Efficacy and Safety of Tirzepatide in Adults With Type 2 Diabetes: A Perspective for Primary Care Providers.

Author

Kushner, Pamela, Anderson, John E., Simon, Jörg, Boye, Kristina S., Ranta, Kari, Torcello-Gómez, Amelia, and Levine, Joshua A.

Subjects

DRUG efficacy, GLYCOSYLATED hemoglobin, GLUCAGON-like peptide 1, HYPOGLYCEMIC agents, PHYSICIANS' attitudes, CELL receptors, TYPE 2 diabetes, SOCIOECONOMIC factors, TREATMENT effectiveness, RESEARCH funding, PATIENT safety, PEPTIDES, PHARMACODYNAMICS, ADULTS

Abstract

This article reviews the efficacy and safety data of tirzepatide, a once-weekly, novel glucose-dependent insulinotropic polypeptide and glucagon-like peptide 1 (GLP-1) receptor agonist approved in the United States, the European Union, and other regions for the treatment of type 2 diabetes. All doses of tirzepatide demonstrated superiority in reducing A1C and body weight from baseline versus placebo or active comparators. The safety profile of tirzepatide was consistent with that of the GLP-1 receptor agonist class, with mild to moderate and transient gastrointestinal side effects being the most common adverse events. With clinically and statistically significant reductions in A1C and body weight without increased risk of hypoglycemia in various populations, tirzepatide has demonstrated potential as a first-in-class treatment option for many people with type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2023

29. Sclerostin antibody promotes bone formation through the Wnt/β-catenin signaling pathway in femoral trochlear after patellar instability.

Author

Xu, Chenyue, Ji, Gang, Chen, Xiaobo, Yan, Lirong, Liang, Tuwan, Liu, Junle, and Wang, Fei

Subjects

BONE growth, SCLEROSTIN, CELLULAR signal transduction, STAINS & staining (Microscopy), INTRA-articular injections, PATELLOFEMORAL joint, CANCELLOUS bone

Abstract

The molecular mechanism of patellar instability (PI) remains unknown. The purpose of this study was to explore the function of SOST/sclerostin in PI and examine the effect of sclerostin antibody (Scl-Ab). We randomly divided 60 male 3-week-old C57Bl/6 mice into four groups: sham, PI, Scl-Ab intraperitoneal injection (Scl-Ab IP), Scl-Ab intraarticular injection (Scl-Ab IA). PI was established in the latter three groups. The Scl-Ab IP/IA groups were administered with an intraperitoneal/intraarticular Scl-Ab injection (100 mg/kg, 20 µl), respectively, at 5-day intervals. Distal femurs were collected 30 days after the surgery. The SOST/sclerostin, β-catenin, ALP, OPG and RANKL expression in distal femur were determined. Trochlear morphology and structural parameters of the trabecular and cortical bone compartments were determined by micro-CT. Further sub-regional analysis was performed. HE staining and Masson's trichrome staining were performed to evaluate cartilage changes. PI increased the expression of SOST/sclerostin and RANKL, and decreased β-catenin, ALP and OPG levels, while Scl-Ab IP reversed these changes. Scl-Ab IP brought trochlear morphology closer to normality. Additionally, Scl-Ab IP significantly improved most of the bone parameters. Importantly, both PI and Scl-Ab IP acted mainly on trabecular bone. Histological analysis showed that Scl-Ab IP protected cartilage from degeneration. However, Scl-Ab IA did not protect against bone loss or cartilage degradation. SOST/sclerostin plays an important role in PI and systemic Scl-Ab use promotes bone formation through the Wnt/β-catenin signaling pathway in the femoral trochlear after PI. [ABSTRACT FROM AUTHOR]

Published

2023

30. Role of Wnt signaling and sclerostin in bone and as therapeutic targets in skeletal disorders.

Author

Marini, Francesca, Giusti, Francesca, Palmini, Gaia, and Brandi, Maria Luisa

Subjects

OSTEOPOROSIS prevention, BONE metabolism, THERAPEUTIC use of monoclonal antibodies, MUSCULOSKELETAL system diseases, DRUG efficacy, WNT proteins, BONE morphogenetic proteins, HIP fractures, CELLULAR signal transduction, OSTEOPOROSIS, BONE density, PATIENT safety

Abstract

Summary: Wnt signaling and its bone tissue–specific inhibitor sclerostin are key regulators of bone homeostasis. The therapeutic potential of anti-sclerostin antibodies (Scl-Abs), for bone mass recovery and fragility fracture prevention in low bone mass phenotypes, has been supported by animal studies. The Scl-Ab romosozumab is currently used for osteoporosis treatment. Introduction: Wnt signaling is a key regulator of skeletal development and homeostasis; germinal mutations affecting genes encoding components, inhibitors, and enhancers of the Wnt pathways were shown to be responsible for the development of rare congenital metabolic bone disorders. Sclerostin is a bone tissue–specific inhibitor of the Wnt/β-catenin pathway, secreted by osteocytes, negatively regulating osteogenic differentiation and bone formation, and promoting osteoclastogenesis and bone resorption. Purpose and methods: Here, we reviewed current knowledge on the role of sclerostin and Wnt pathways in bone metabolism and skeletal disorders, and on the state of the art of therapy with sclerostin-neutralizing antibodies in low-bone-mass diseases. Results: Various in vivo studies on animal models of human low-bone-mass diseases showed that targeting sclerostin to recover bone mass, restore bone strength, and prevent fragility fracture was safe and effective in osteoporosis, osteogenesis imperfecta, and osteoporosis pseudoglioma. Currently, only treatment with romosozumab, a humanized monoclonal anti-sclerostin antibody, has been approved in human clinical practice for the treatment of osteoporosis, showing a valuable capability to increase BMD at various skeletal sites and reduce the occurrence of new vertebral, non-vertebral, and hip fragility fractures in treated male and female osteoporotic patients. Conclusions: Preclinical studies demonstrated safety and efficacy of therapy with anti-sclerostin monoclonal antibodies in the preservation/restoration of bone mass and prevention of fragility fractures in low-bone-mass clinical phenotypes, other than osteoporosis, to be validated by clinical studies for their approved translation into prevalent clinical practice. [ABSTRACT FROM AUTHOR]

Published

2023

31. Tirzepatide for the treatment of adults with type 2 diabetes: An endocrine perspective.

Author

De Block, Christophe, Bailey, Clifford, Wysham, Carol, Hemmingway, Andrea, Allen, Sheryl Elaine, and Peleshok, Jennifer

Subjects

TYPE 2 diabetes, MAJOR adverse cardiovascular events, GASTRIC inhibitory polypeptide, ADVERSE health care events, GLYCOSYLATED hemoglobin, INSULIN aspart, GLYCEMIC control, ARTIFICIAL hearts

Abstract

Tirzepatide is a novel glucose‐dependent insulinotropic polypeptide/glucagon‐like peptide 1 (GLP‐1) receptor agonist approved in the United States as an adjunct to diet and exercise to improve glycaemic control in adults with type 2 diabetes and under investigation for use in chronic weight management, major adverse cardiovascular events and the management of other conditions, including heart failure with preserved ejection fraction and obesity and non‐cirrhotic non‐alcoholic steatohepatitis. The Phase 3 SURPASS 1‐5 clinical trial programme was designed to assess efficacy and safety of once‐weekly subcutaneously injected tirzepatide (5, 10 and 15 mg), as monotherapy or combination therapy, across a broad spectrum of people with type 2 diabetes. Use of tirzepatide in clinical studies was associated with marked reductions of glycated haemoglobin (−1.87 to −2.59%, −20 to −28 mmol/mol) and body weight (−6.2 to −12.9 kg), as well as reductions in parameters commonly associated with heightened cardiometabolic risk such as blood pressure, visceral adiposity and circulating triglycerides. In SUPRASS‐2, these reductions were greater than with the GLP‐1 receptor agonist semaglutide 1 mg. Tirzepatide was well tolerated, with a low risk of hypoglycaemia when used without insulin or insulin secretagogues and showed a generally similar safety profile to the GLP‐1 receptor agonist class. Accordingly, evidence from these clinical trials suggests that tirzepatide offers a new opportunity for the effective lowering of glycated haemoglobin and body weight in adults with type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2023

32. Rapid in vitro assessment of the immunogenicity potential of engineered antibody therapeutics through detection of CD4+ T cell interleukin-2 secretion.

Author

Arata, Yoshiyuki, Motoyama, Shigeki, Yano, Mariko, Ikuno, Tatsuya, Ito, Shunsuke, Matsushita, Tomochika, Takeiri, Akira, Nishito, Yukari, Yabuki, Nami, Mizuno, Hideaki, Sampei, Zenjiro, Mishima, Masayuki, Honda, Masaki, Kiyokawa, Jumpei, Suzuki, Hiromi, Chiba, Shuichi, Tabo, Mitsuyasu, and Kubo, Chiyomi

Published

2023

33. Estudios de asociación de genoma completo (GWAS) versus validación funcional: reto de la era post-GWAS.

Author

Martínez-Gil, Núria, Patiño-Salazar, Juan David, Rabionet, Raquel, Grinberg, Daniel, and Balcells, Susanna

Abstract

Copyright of Journal of Osteoporosis & Mineral Metabolism / Revista de Osteoporosis y Metabolismo Mineral (Spanish edition) is the property of Ibanez y Plaza and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

34. Genome-wide association studies (GWAS) vs functional validation: the challenge of the post-GWAS era.

Author

Martínez-Gil, Núria, David Patiño-Salazar, Juan, Rabionet, Raquel, Grinberg, Daniel, and Balcells, Susanna

Subjects

GENOME-wide association studies, BONE density, GENETIC correlations, GENETIC variation, BONE diseases

Abstract

Over the past few years, efforts have been made to determine the variants and genes that may be important to determine bone mineral density (BMD) that, at the same time, are involved in several bone diseases. To achieve this, the approach that has been the most successful of all has been genome-wide association studies (GWAS). In particular, in research on bone biology over 50 different large GWAS or GWAS metanalyses have been published identifying a total of 500 genetic loci associated with different bone parameters such as BMD, bone resistance, and risk of fracture. Although the discovery of associated variants is an essential aspect, the functional validation of such variants is equally important to elucidate their effect, as well as the causal correlation they have with genetic disease. Since it is a much more time consuming and tedious aspect it has become the new challenge of this post-GWAS era. Among the genes that have already been studied several Wnt signaling pathway genes have been included, among them, the SOST gene that plays a crucial role both determining the BMD of the population and monogenic diseases with elevated bone mass giving rise to a new therapy against osteoporosis. In this review we'll be collecting the main GWAS associated with bone phenotypes, as well as some functional validations undertaken to analyze the associations found in them. [ABSTRACT FROM AUTHOR]

Published

2023

35. Advances in Diagnosis and Management of Childhood Osteoporosis.

Author

Lim, David B. N., Moon, Rebecca J., and Davies, Justin H.

Subjects

OSTEOPOROSIS diagnosis, OSTEOPOROSIS treatment, BONE diseases, OSTEOPOROSIS, RISK assessment, PATIENTS' attitudes, FRACTURE fixation, BONE density, BONE fractures, DISEASE risk factors, CHILDREN

Abstract

Childhood osteoporosis leads to increased propensity to fracture, and thus is an important cause of morbidity, pain and healthcare utilisation. Osteoporosis in children may be caused by a primary bone defect or secondary to an underlying medical condition and/or its treatment. Primary osteoporosis is rare, but there is an increasing number of children with risk factors for secondary osteoporosis. Therefore it is imperative that all paediatricians are aware of the diagnostic criteria and baseline investigations for childhood osteoporosis to enable timely referral to a specialist in paediatric bone health. This review will discuss the approach to diagnosis, investigation and management of childhood osteoporosis, with particular consideration to advances in molecular diagnosis of primary bone disorders, and current and emerging therapies for fracture reduction. [ABSTRACT FROM AUTHOR]

Published

2022

36. Novosti u farmakološkom liječenju osteoporoze.

Author

BILIĆ-ĆURČIĆ, INES, VARŽIĆ, SILVIJA CANECKI, and SCHÖNBERGER, EMA

Abstract

Copyright of Medicus (1330-013X) is the property of Pliva Hrvatska d.o.o. and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

37. The pathophysiology of osteoporosis in obesity and type 2 diabetes in aging women and men: The mechanisms and roles of increased bone marrow adiposity.

Author

Ali, Dalia, Tencerova, Michaela, Figeac, Florence, Kassem, Moustapha, and Jafari, Abbas

Subjects

OLDER men, TYPE 2 diabetes, BONE marrow, OSTEOPOROSIS, OLDER people

Abstract

Osteoporosis is defined as a systemic skeletal disease characterized by decreased bone mass and micro-architectural deterioration leading to increased fracture risk. Osteoporosis incidence increases with age in both post-menopausal women and aging men. Among other important contributing factors to bone fragility observed in osteoporosis, that also affect the elderly population, are metabolic disturbances observed in obesity and Type 2 Diabetes (T2D). These metabolic complications are associated with impaired bone homeostasis and a higher fracture risk. Expansion of the Bone Marrow Adipose Tissue (BMAT), at the expense of decreased bone formation, is thought to be one of the key pathogenic mechanisms underlying osteoporosis and bone fragility in obesity and T2D. Our review provides a summary of mechanisms behind increased Bone Marrow Adiposity (BMA) during aging and highlights the pre-clinical and clinical studies connecting obesity and T2D, to BMA and bone fragility in aging osteoporotic women and men. [ABSTRACT FROM AUTHOR]

Published

2022

38. Sclerostin immunohistochemical staining in surgically treated giant cell tumor of bone.

Author

Kelly, Sean P., Ramkumar, Dipak B., Peacock, Zachary S., Newman, Erik T., Venrick, Connor, Lozano‐Calderon, Santiago A., Raskin, Kevin A., Chebib, Ivan, and Schwab, Joseph H.

Published

2022

39. Tirzepatide, a dual GIP/GLP-1 receptor co-agonist for the treatment of type 2 diabetes with unmatched effectiveness regrading glycaemic control and body weight reduction.

Author

Nauck, Michael A. and D'Alessio, David A.

Subjects

WEIGHT loss, REGULATION of body weight, TYPE 2 diabetes, GLYCEMIC control, MYOCARDIAL infarction, BODY weight

Abstract

Tirzepatide is the first dual GIP/GLP-1 receptor co-agonist approved for the treatment of type 2 diabetes in the USA, Europe, and the UAE. Tirzepatide is an acylated peptide engineered to activate the GIP and GLP-1 receptors, key mediators of insulin secretion that are also expressed in regions of the brain that regulate food intake. Five clinical trials in type 2-diabetic subjects (SURPASS 1–5) have shown that tirzepatide at 5–15 mg per week reduces both HbA1c (1.24 to 2.58%) and body weight (5.4–11.7 kg) by amounts unprecedented for a single agent. A sizable proportion of patients (23.0 to 62.4%) reached an HbA1c of < 5.7% (which is the upper limit of the normal range indicating normoglycaemia), and 20.7 to 68.4% lost more than 10% of their baseline body weight. Tirzepatide was significantly more effective in reducing HbA1c and body weight than the selective GLP-1 RA semaglutide (1.0 mg per week), and titrated basal insulin. Adverse events related to tirzepatide were similar to what has been reported for selective GLP-1RA, mainly nausea, vomiting, diarrhoea, and constipation, that were more common at higher doses. Cardiovascular events have been adjudicated across the whole study program, and MACE-4 (nonfatal myocardial infarction, non-fatal stroke, cardiovascular death and hospital admission for angina) events tended to be reduced over up to a 2 year-period, albeit with low numbers of events. For none of the cardiovascular events analysed (MACE-4, or its components) was a hazard ratio > 1.0 vs. pooled comparators found in a meta-analysis covering the whole clinical trial program, and the upper bounds of the confidence intervals for MACE were < 1.3, fulfilling conventional definitions of cardiovascular safety. Tirzepatide was found to improve insulin sensitivity and insulin secretory responses to a greater extent than semaglutide, and this was associated with lower prandial insulin and glucagon concentrations. Both drugs caused similar reductions in appetite, although tirzepatide caused greater weight loss. While the clinical effects of tirzepatide have been very encouraging, important questions remain as to the mechanism of action. While GIP reduces food intake and body weight in rodents, these effects have not been demonstrated in humans. Moreover, it remains to be shown that GIPR agonism can improve insulin secretion in type 2 diabetic patients who have been noted in previous studies to be unresponsive to GIP. Certainly, the apparent advantage of tirzepatide, a dual incretin agonist, over GLP-1RA will spark renewed interest in the therapeutic potential of GIP in type 2 diabetes, obesity and related co-morbidities. [ABSTRACT FROM AUTHOR]

Published

2022

40. Modeling osteoporosis to design and optimize pharmacological therapies comprising multiple drug types.

Author

Jörg, David J., Fuertinger, Doris H., Cherif, Alhaji, Bushinsky, David A., Mermelstein, Ariella, Raimann, Jochen G., and Kotanko, Peter

Published

2022

41. Immunology of osteoporosis: relevance of inflammatory targets for the development of novel interventions.

Author

Ahmad, Syed Sufian, Ahmed, Faraha, Ali, Ruhi, Ghoneim, Mohammed M, Alshehri, Sultan, Najmi, Abul Kalam, Ahmad, Sayeed, Ahmad, Mohammad Zaki, Ahmad, Javed, and Khan, Mohammad Ahmed

Published

2022

42. Sclerostin Immunohistochemical Staining in Aggressive Maxillofacial Giant Cell Lesions: Initial Results and Potential Therapeutic Target.

Author

Kelly, Sean P., Ramkumar, Dipak B., Lozano-Calderon, Santiago A., Newman, Erik T., Raskin, Kevin A., Chebib, Ivan, Schwab, Joseph H., and Peacock, Zachary S.

Published

2022

43. Osteoporosis in 10 years time: a glimpse into the future of osteoporosis.

Author

Adami, Giovanni, Fassio, Angelo, Gatti, Davide, Viapiana, Ombretta, Benini, Camilla, Danila, Maria I., Saag, Kenneth G., and Rossini, Maurizio

Abstract

Patients living with osteoporosis are projected to increase dramatically in the next decade. Alongside the forecasted increased societal and economic burden, we will live a crisis of fractures. However, we will have novel pharmacological treatment to face this crisis and, more importantly, new optimized treatment strategies. Fracture liaison services will be probably implemented on a large scale worldwide, helping to prevent additional fractures in high-risk patients. In the next decade, novel advances in the diagnostic tools will be largely available. Moreover, new and more precise fracture risk assessment tools will change our ability to detect patients at high risk of fractures. Finally, big data and artificial intelligence will help us to move forward into the world of precision medicine. In the present review, we will discuss the future epidemiology and costs of osteoporosis, the advances in early and accurate diagnosis of osteoporosis, with a special focus on biomarkers and imaging tools. Then we will examine new and refined fracture risk assessment tools, the role of fracture liaison services, and a future perspective on osteoporosis treatment. [ABSTRACT FROM AUTHOR]

Published

2022

44. Concentration‐QT modelling in early clinical oncology settings: Simulation evaluation of performance.

Author

Cantet, Gael, Berges, Alienor, O'Sullivan, Rhianna, Cohen‐Rabbie, Sarit, Dota, Corina, Dubois, Vincent, Benoist, Guillemette E., Tomkinson, Helen, Rekić, Dinko, Parkinson, Joanna, and Schalkwijk, Stein

Subjects

ONCOLOGY, CONFIDENCE intervals

Abstract

Aims: Concentration‐QT modelling (C‐QTc) of first‐in‐human data has been rapidly adopted as the primary evaluation of QTc interval prolongation risk. Here, we evaluate the performance of C‐QTc in early oncology settings (i.e., patients, no placebo or supratherapeutic dose, 3 + 3 designs). Methods: C‐QTc performance was evaluated across three oncology scenarios using a simulation‐estimation approach: (scen1) typical dose‐escalation testing six dose levels (n = 21); (scen2) small dose‐escalation testing two dose levels (n = 9); (scen3) expansion cohorts at one dose level (n = 6–140). True ΔΔQTc effects ranged from 3 ms ("no effect") to 20 ms ("large effect"). Performance was assessed based on the upper limit of the ΔQTc two‐sided 90% CI against a threshold of 10 or 20 ms. Results: The performance against the 10 ms threshold was limited based on C‐QTc data from typical dose escalation (scen1) and acceptable performance was observed only for relatively large expansions (n ≥ 45; scen3). Performance against the 20 ms threshold was acceptable based on C‐QTc data from a typical dose escalation (scen1) or dose expansion cohort n > 10 (scen3). In general, pooling C‐QTc data from dose escalation and expansion cohorts substantially improved the performance and reduced the ΔQTc 90% CI width. Conclusion: C‐QTc performance appeared limited using a 10 ms threshold, but acceptable against a 20 ms threshold. Selection of threshold may be informed by the benefit–risk balance in a specific disease area. Acceptable precision (i.e., confidence intervals) of the estimated ΔQTc, regardless of its magnitude, can be facilitated by pooling data from dose escalation and expansion cohorts. [ABSTRACT FROM AUTHOR]

Published

2022

45. Targeting the Wnt signaling pathway for breast cancer bone metastasis therapy.

Author

Cui, Jingyao, Chen, Haoran, Zhang, Kaiwen, and Li, Xin

Subjects

METASTATIC breast cancer, WNT signal transduction, CELLULAR signal transduction, BONE metastasis, METASTASIS

Abstract

Osteolytic bone destruction is found in approximately 60% of advanced breast cancer patients. With the pathogenesis of bone metastasis being unclear, traditional antiresorptive therapeutic strategies might not be ideal for treatment. The Wnt pathway is a highly organized cascade involved in multiple stages of cancer bone metastasis, and Wnt-targeted therapeutic strategies have shown promise in achieving favorable outcomes. In this review, we summarize the current progress of pharmacological Wnt modulators against breast cancer bone metastasis, discuss emerging therapeutic strategies based on Wnt pathway-related targets for bone therapy, and highlight opportunities to better harness the Wnt pathway for bone metastasis therapeutics to further reveal the implications of the Wnt pathway in bone metastasis pathology and provide new ideas for the development of Wnt-based intervention strategies against breast cancer bone metastasis. [ABSTRACT FROM AUTHOR]

Published

2022

46. Gut peptide regulation of food intake – evidence for the modulation of hedonic feeding.

Author

Woodward, Orla R. M., Gribble, Fiona M., Reimann, Frank, and Lewis, Jo E.

Subjects

FOOD consumption, PEPTIDES, GASTRIC bypass, FOOD preferences, LEPTIN, NUTRITIONAL status

Abstract

The number of people living with obesity has tripled worldwide since 1975 with serious implications for public health, as obesity is linked to a significantly higher chance of early death from associated comorbidities (metabolic syndrome, type 2 diabetes, cardiovascular disease and cancer). As obesity is a consequence of food intake exceeding the demands of energy expenditure, efforts are being made to better understand the homeostatic and hedonic mechanisms governing food intake. Gastrointestinal peptides are secreted from enteroendocrine cells in response to nutrient and energy intake, and modulate food intake either via afferent nerves, including the vagus nerve, or directly within the central nervous system, predominantly gaining access at circumventricular organs. Enteroendocrine hormones modulate homeostatic control centres at hypothalamic nuclei and the dorso‐vagal complex. Additional roles of these peptides in modulating hedonic food intake and/or preference via the neural systems of reward are starting to be elucidated, with both peripheral and central peptide sources potentially contributing to central receptor activation. Pharmacological interventions and gastric bypass surgery for the treatment of type 2 diabetes and obesity elevate enteroendocrine hormone levels and also alter food preference. Hence, understanding of the hedonic mechanisms mediated by gut peptide action could advance development of potential therapeutic strategies for the treatment of obesity and its comorbidities. [ABSTRACT FROM AUTHOR]

Published

2022

47. A PRIMER ON OBESITY-RELATED CARDIOMYOPATHY.

Author

Samson, Willis K., Yosten, Gina L. C., and Remme, Carol Ann

Subjects

TYPE 2 diabetes, SCIENTIFIC literature, CARDIOMYOPATHIES, WEIGHT loss, OBESITY complications, BRANCHED chain amino acids

Published

2022

48. Osteocytes and Estrogen Deficiency.

Author

McNamara, Laoise M.

Abstract

Purpose of Review: Postmenopausal osteoporosis reduces circulating estrogen levels, which leads to osteoclast resorption, bone loss, and fracture. This review addresses emerging evidence that osteoporosis is not simply a disease of bone loss but that mechanosensitive osteocytes that regulate both osteoclasts and osteoblasts are also impacted by estrogen deficiency. Recent Findings: At the onset of estrogen deficiency, the osteocyte mechanical environment is altered, which coincides with temporal changes in bone tissue composition. The osteocyte microenvironment is also altered, apoptosis is more prevalent, and hypermineralization occurs. The mechanobiological responses of osteocytes are impaired under estrogen deficiency, which exacerbates osteocyte paracrine regulation of osteoclasts. Summary: Recent research reveals changes in osteocytes during estrogen deficiency that may play a critical role in the etiology of the disease. A paradigm change for osteoporosis therapy requires an advanced understanding of such changes to establish the efficacy of osteocyte-targeted therapies to inhibit resorption and secondary mineralization. [ABSTRACT FROM AUTHOR]

Published

2021

49. The dual glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) receptor agonist tirzepatide: a novel cardiometabolic therapeutic prospect.

Author

Fisman, Enrique Z. and Tenenbaum, Alexander

Subjects

GASTRIC inhibitory polypeptide, TYPE 2 diabetes, GLYCEMIC control, INSULIN sensitivity, SUBCUTANEOUS injections, DRUGS

Abstract

Incretin hormones are peptides released in the intestine in response to the presence of nutrients in its lumen. The main incretins are glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP). GLP-1 stimulates insulin secretion, inhibits glucagon secretion at pancreatic α cells and has also extrapancreatic influences as slowing of gastric emptying which increases the feeling of satiety. GIP is the main incretin hormone in healthy people, causative of most the incretin effects, but the insulin response after GIP secretion in type 2 diabetes mellitus (T2DM) is strongly reduced. Therefore, in the past GIP has been considered an unappealing therapeutic target for T2DM. This conception has been changing during recent years, since it has been reported that resistance to GIP can be reversed and its effectiveness restored by improving glycemic control. This fact paved the way for the development of a GIP receptor agonist-based therapy for T2DM, looking also for the possibility of finding a combined GLP-1/GIP receptor agonist. In this framework, the novel dual GIP and GLP-1 receptor agonist tirzepatide seems to be not just a new antidiabetic medication. Administered as a subcutaneous weekly injection, it is a manifold single pharmacological agent that has the ability to significantly lower glucose levels, as well as improve insulin sensitivity, reduce weight and amend dyslipidemia favorably modifying the lipid profile. Tirzepatide and additional dual GLP-1/GIP receptor agonists that could eventually be developed in the future seem to be a promising furthest advance for the management of several cardiometabolic settings. Obviously, it is too early to be overly hopeful since it is still necessary to determine the long-term effects of these compounds and properly verify the potential cardiovascular benefits. Anyway, we are currently facing a novel and very appealing therapeutic option. [ABSTRACT FROM AUTHOR]

Published

2021

50. The New S7B/E14 Question and Answer Draft Guidance for Industry: Contents and Commentary.

Author

Darpo, Borje and Ferber, Georg

Subjects

HEALTH care industry, CARDIOLOGY, CONSENSUS (Social sciences), EXPERIMENTAL design, PHARMACOLOGY, ANTINEOPLASTIC agents, ELECTROCARDIOGRAPHY, ARRHYTHMIA

Abstract

In August 2020, the International Council on Harmonisation (ICH) released a new draft document, which for the first time combined nonclinical (S7B) and clinical (E14) Questions and Answers (Q&As) into 1 document. FDA describes the revision as a "value proposition": if the human ether‐à‐go‐go assay and the in vivo study are performed in a standardized way, the number of dedicated thorough QT (TQT) studies can be reduced. In this article, we describe and discuss the Q&As that relate to clinical ECG evaluation. If supported by negative standardized nonclinical assays, Q&A 5.1 will obviate the need for a TQT study in the case that a >2‐fold exposure margin vs high clinical scenario cannot be obtained. Q&A 6.1 addresses drugs that are poorly tolerated in healthy subjects and cannot be studied at high doses or in placebo‐controlled studies; it therefore mainly applies to oncology drugs. It will enable sponsors to claim that a new drug has a "low likelihood of proarrhythmic effects" in the case that the mean corrected QT effect is <10 milliseconds at the time of market application. The E14 2015 revision allowed application of concentration–corrected QT analysis on data from routinely performed clinical pharmacology studies, for example, the first‐in‐human study and the proportion of dedicated TQT studies has since steadily decreased. It can be foreseen that the proposed new revision will further reduce the number of TQT studies. To achieve harmonization across regulatory regions, it seems important to reach consensus within the International Council on Harmonisation group on the new threshold proposed in 6.1. For this purpose, the Implementation Working Group has asked for public comments. [ABSTRACT FROM AUTHOR]

Published

2021