The effects of neutropenic diet with or without Magnesium supplementation on inflammatory factors and outcomes of Allogenic -Hematopoietic stem cell transplantation in patients with acute leukemia : A double blind randomized clinical trial

Start Date20 Jan 2025

Sponsor / Collaborator

Shahid Beheshti University of Medical Sciences

IRCT20241026063495N1

/ SuspendedPhase 3IIT

Studying the effect of consuming effervescent magnesium tablets before surgery on pain intensity after elective abdominal surgery

Start Date08 Jan 2025

Sponsor / Collaborator

Islamic Azad University

NCT06721247

/ Not yet recruitingPhase 2/3IIT

Efficacy Of Oral Magnesium Supplementation in Controlled Bronchial Asthma Patients

The goal of this clinical trial is to assess the efficacy of oral magnesium supplements in controlled asthmatic patients for proper effective asthma management to reduce frequency of asthma exacerbation & to test the effect of oral magnesium supplementation on improvement of both clinical symptoms and lung functions in patients with bronchial asthma.. The main questions it aims to answer are:
• Can oral supplementation of magnesium play a role in decrease the number of bronchial asthma exacerbations , number of ER visits , number of doctor visits and improve lung function ? Researchers will compare patients on usual treatment according to GINA guidelines 2024 group B and those taking oral magnesium together with the usual group A .
Participants will:
* Take oral magnesium treatment with usual asthma medications according to GINA guidelines (2024) every day for 1year
* Visit the clinic once every 2 weeks for checkups and tests
* Keep a diary of their day and night symptoms and the number of times they had activity limitation due to asthma and the number of use reliever.

Start Date02 Jan 2025

Sponsor / Collaborator

Zagazig University

100 Clinical Results associated with Magnesium Carbonate

100 Translational Medicine associated with Magnesium Carbonate

100 Patents (Medical) associated with Magnesium Carbonate

23,256

Literatures (Medical) associated with Magnesium Carbonate

01 Dec 2025·Current Pain and Headache Reports

Nutraceuticals and Headache 2024: Riboflavin, Coenzyme Q10, Feverfew, Magnesium, Melatonin, and Butterbur

Review

Author: Tepper, Stewart J ; Tepper, Katharine

PURPOSE OF REVIEWNutraceuticals are not regulated by the US Food and Drug Administration, so a careful literature review is essential to make clinical decisions. Riboflavin or vitamin B2 can be recommended for migraine prevention in adults, but pediatric use is not proven. Adverse events are minimal. Coenzyme Q10 has Level C evidence for migraine prevention and low adverse events. Feverfew may be effective for migraine prevention, but the absence of clear safety studies, the differences in doses and characteristics of dried leaf preparations, and the myriad of feverfew cellular effects suggest caution in recommendation for use. Magnesium is recommended for migraine prevention and intravenous acute use, with the potential for generally mild gastrointestinal tolerability adverse events. Melatonin has very low certainty for evidence of efficacy, and is weakly recommended in those with sleep problems. However, purity of US sold melatonin is very poor. Butterbur or petasites preparations have strong evidence for efficacy and concern for hepatotoxicity. Please see the US National Center for Complementary and Integrative Health/NIH online site https://www.nccih.nih.gov/health/butterbur for up-to-date recommendations on whether to use this nutraceutical.

01 Jun 2025·Separation and Purification Technology

Separation and utilization of lithium, magnesium, and boron resources from salt lakes through Ionic liquid extraction and CO2 mineralization

Author: Zhang, Guoquan ; He, Jun ; Li, Gaomiao ; Luo, Mingzhi ; Li, Jia

Salt lakes are abundant in three crucial resources - lithium(Li), magnesium(Mg), and boron(B).The separation efficiency of these resources is low, the excessive use of acid and the environmental harm caused by the accumulation of magnesium source after Li⁺ extraction still exist.In this work, a new process of step-by-step extraction of B-Li and Mg mineralization is proposed to sep. the three resources.Boron was extracted using 2-ethyl-1,3-hexanediol (EHD) + kerosene, and it was found that the addition of FeCl₃ could significantly improve the boron extraction rate(E).In the R(O:A) = 1:3, 40 %EHD + 60 %kerosene, adding 0.15 mol/L FeCl₃, after three-stage countercurrent extraction, the E(B³⁺) reached 99 %, E(Fe³⁺), E(Li⁺) and E(Mg²⁺) less than 4 %.Tri-Bu Phosphate (TBP)-Ionic Liquids (ILs)-kerosene-FeCl₃ system was used to extract Li⁺, the ILs and FeCl₃ existed in the extraction process with a competitive behavior.The extraction efficiency of lithium was improved by cationic [C₄mim⁺] exchange reaction.Under the conditions of R(O:A) = 1:1, 5 %ILs + 65 %TBP + 30 %kerosene, and three-stage extraction, the E(Li⁺) was reached 91 %.(NH₄)₂CO₃ was used to mineralize the magnesium resources.At a reaction temperature of 40 °C, the product was magnesium carbonate trihydrate(MgCO₃·3H₂O) with a smooth surface and rod-like structure, and the conversion rate reached 85 %.At 75 °C, the product was an irregular spheroidal basic magnesium carbonate(4MgCO₃·Mg(OH)₂·5H₂O) with a magnesium conversion of 91.7 %.

01 May 2025·Journal of the American Ceramic Society

Structural and electric properties of Na super ionic conductor solid electrolyte M^II_x_/2Li₁₋_xTi₂(PO₄)₃ (M^II = Mg, Zn, and Cd)

Author: Bih, Lahcen ; Ababou, Yahya ; Rjeb, Abdelilah ; Bouftila, Nour El Hoda ; Faik, Abdessamad ; Chouiekh, Abdelhak ; Naji, Mohamed

AbstractAll‐solid‐state lithium‐ion batteries, employing solid electrolytes, offer a promising solution to address safety concerns inherent in conventional lithium‐ion batteries. Among the various types of Li‐ion solid electrolytes, LiTi2(PO4)3 (LTP) with the Na Super Ionic CONductor (NASICON) structure stands out as a particularly attractive material, despite its relatively low ionic conductivity at room temperature. One approach to enhance the performance of LTP solid electrolytes involves modifying the network size or redistributing Li cations and vacancies within the adjacent sites of the NASICON structure. Therefore, this study seeks to replace lithium ions with divalent cations, thereby increasing the concentration of vacancies, and facilitates the migration of Li+ ions between adjacent partially populated M1 sites. Introducing divalent elements not only augments vacancies in the lithium sites but also induces variations in local disorder within NASICON structures. Consequently, NASICON compounds, MIIx/2Li1−xTi2(PO4)3 (MII = Mg, Zn, and Cd), were synthesized via the sol–gel method, and their structural, microstructural, and electrical properties were thoroughly analyzed using a variety of techniques. The presence of divalent cations in the M1 site results in a reduction of symmetry and an enhancement of local disorder. A correlation between ionic conductivity and structure was established, which was linked to the disorder of lithium atoms within the structure. Electric modulus formalism was employed to explore electric relaxation, revealing that the diffusion and relaxation processes are thermally activated.

News (Medical) associated with Magnesium Carbonate

23 Dec 2024

·www.drugs.com

Coffee Can Boost the Brains of People with Certain Heart Conditions

MONDAY, Dec. 23, 2024 -- Coffee provides a quick morning boost, but it might also protect the brain health of people with a common heart rhythm disorder . A study published recently in the Journal of the American Heart Association shows patients with atrial fibrillation who drank more than five cups of coffee a day performed better on an array of cognitive tests than those who drank little to no coffee. In fact, the brains of heavy coffee drinkers were nearly seven years younger in cognitive age compared to coffee teetotalers. “Many myths are around, but our study found no reason to discourage or forbid a patient with A-Fib from drinking coffee. Instead, say, ‘Enjoy, it may even be good for you!’” senior researcher Dr. Jürg Beer , a professor of medicine and hematology at the University of Zürich in Switzerland, said in an American Heart Association (AHA) news release. Atrial fibrillation is the most common heart rhythm disorder in adults, affecting more than 5 million people in the United States, according to the AHA. A-Fib occurs when the upper chambers of the heart -- the atria -- begin beating in a quivering and uncoordinated way. This allows blood to pool in the atria and potentially clot. A-Fib increases a person’s risk of stroke fivefold, as a blood clot can travel from the atria and block blood flow to the brain, according to the U.S. Centers for Disease Control and Prevention. Current American Heart Association guidelines say that abstaining from caffeine doesn’t benefit people with A-Fib, unless patients report that caffeine triggers or worsens their symptoms, researchers noted. Symptoms can include rapid heartbeat, dizziness, fatigue, shortness of breath and chest pain. “It is known that regular coffee consumption benefits cognitive performance among healthy people. The most frequent cardiac arrhythmia, atrial fibrillation, is known to independently increase the risk of dementia,” said lead researcher Dr. Massimo Barbagallo , a resident in the neuro intensive care unit at the University Hospital Zürich. “Thus, the question is whether coffee might offset the increased risk of cognitive impairment in people with A-Fib,” Barbagallo said. For the study, researchers recruited more than 2,400 people in Switzerland diagnosed with atrial fibrillation between 2014 and 2017. Participants completed several brain tests and reported how many cups of caffeinated coffee they drank during the last 12 months. Results showed that the more coffee a person drank, the better they performed on cognitive tests. “There was a very clear and consistent ‘dose-response’ association between drinking more coffee and doing better on several different sophisticated cognitive tests,” Beer said. Specifically, their scores were about 11% higher than people who drank little to no coffee, researchers found. Coffee also appeared to lower inflammation in A-Fib patients. Inflammatory markers were more than 20% lower in people drinking five cups daily than those drinking less than one cup a day. “Inflammatory markers decreased with higher coffee consumption, an association that remained after considering variables such as age, sex, body mass index, smoking status, physical activity and a history of stroke,” Beer said. It’s not quite clear why coffee might help brain health, researchers said. It could be due to caffeine or other active ingredients in coffee, like magnesium and niacin, or it might be due to coffee’s anti-inflammatory effects. However, an outside expert warns that this observational study cannot prove a direct link between heavy coffee drinking and better brain aging, particularly in people with A-Fib. “Other studies have shown coffee has cognitive-enhancing functions across the board. This, however, is not specific to the A-Fib population. We cannot conclude that coffee prevents long-term cognitive decline,” said Dr. Jose Joglar , a professor of internal medicine at UT Southwestern Medical Center in Dallas. “Coffee does not seem to worsen A-Fib so there is no need to stop drinking it,” Joglar continued. “However, we cannot say starting to drink coffee would prevent A-Fib or prevent long-term cognitive decline.” Researchers also noted that the study measured brain health and coffee consumption at the same point in time, so it could not track the long-term effect of coffee on brain aging over time. “To detect a relevant cognitive decline, a follow-up of at least 5 to 10 years is required,” Barbagallo said. “However, the nutritive habits including coffee consumption reported by participants reflect exposure over many years and we likely see here the results of this.” Whatever your topic of interest, subscribe to our newsletters to get the best of Drugs.com in your inbox.

Clinical ResultAHA

13 Feb 2024

·www.prnewswire.com

Innocan Provides Corporate Update & Preliminary Q4 and Fiscal Year 2023 Financial Highlights

HERZLIYA, Israel and CALGARY, AB, Feb. 13, 2024 /PRNewswire/ -- Innocan Pharma Corporation (CSE: INNO) (FSE: IP4) (OTC: INNPF) (the " Company" or " Innocan"), is pleased to provide the following corporate update: Innocan is uniquely positioned within the pharmaceutical technology industry with its dual focus on pharmaceuticals and consumer wellness, leveraging cutting-edge science to enhance patient and consumer well-being. Technological Edge: Innocan's product development is centered around its proprietary CBD-loaded liposome platform technology ("LPT"), a testament to its commitment to innovation. This technology is designed for both human and animal applications, offering a new paradigm in treatment efficacy and safety. Additionally, Innocan's consumer wellness portfolio, featuring topicals and cosmetics, underscores its dedication to health and wellness, catering to the growing consumer demand for effective wellness products. The Opportunity: The global pain management market presents a vast opportunity for Innocan. With over 20% of adults in the US market reporting chronic pain,[1] the need for novel and effective treatments is more pressing than ever. As Innocan enters the market, Innocan's innovative technology and focus on CBD's therapeutic potential positions it well in this sizeable and growing marketplace. Product Overview Innocan's product portfolio includes advanced CBD-based formulations for both injectable and topical applications. The product portfolio includes patent-pending, injectable liposome-delivery platforms for human and veterinary use, and a range of topical products for direct pain relief and wellness product lines. Each product category is at a strategic development and growth stage backed by clinical & efficacy trials. Market Summary The pain management market for human applications continues to grow, targeting US$109 billion by 2032.[2] Similarly, the market for topical pain relief is forecasted to grow significantly, from US$10.68 billion in 2023 to over US$14 billion by 2028.[3] For animal applications, the global veterinary medicine market is expected to reach nearly US$50 billion by 2024, with the pain management segment experiencing robust growth.[4] Regulatory Pathway "The development of our LPT platform is progressing much faster than is usual in the pharmaceutical sector," said Prof. Chezy Barenholz, Innocan's scientific director. Innocan has been able to obtain extensive data derived from several pre-clinical studies previously conducted on various animal models including mice, dogs, and goats. The data obtained from these studies indicated a similar behavior of the drug among the different animals exhibited by long pharmacokinetics over weeks, high bioavailability, good drug tolerance and long-lasting efficacy. Studies conducted in large mammals supported LPT-CBD efficacy by showing long lasting relieving effect in indications such as chronic pain and drug resistance epileptic seizures. Innocan is currently testing the LPT platform on a new animal species and expects to receive results shortly. Following successful pre-clinical trials, Innocan is actively pursuing United States Food and Drug Administration (" FDA") approval for our human pharmaceutical applications. Innocan expects that pre-investigational new drug applications will be submitted to the FDA before the end of March, 2024. Innocan boasts a robust intellectual property portfolio, comprising 12 families of patent applications. These applications include a diverse range of conditions, including pain management, diabetes and vaginal applications. One patent family has already been granted in the United States related to the Company's combined cannabis and magnesium topical pain-relief technology. Preliminary Q4 and Fiscal Year 2023 Financial Highlights (unaudited) Innocan's preliminary revenues for Q4 2023 are expected to be at least US$4.89M, representing an approximate increase of 20% from Q3 2023 and an increase of at least 331% compared to Q4 2022. For the 2023 fiscal year, Innocan's preliminary revenues are expected to be at least US$13.6 million, representing an approximate increase of 433% over fiscal year 2022. This surge in revenue is primarily attributable to the robust sales performance of Innocan's subsidiary, B.I. Sky Global Ltd. These preliminary revenue figures exceed expenses in the respective periods. The above information should be read in conjunction with Innocan's audited consolidated financial statements as of December 31, 2023 (the " Audited Financial Statements"), and the accompanying management's discussion and analysis for the year ended December 31, 2023, which will be filed on the Innocan's SEDAR+ profile at . Corporate Update Link About Innocan Innocan is a pharmaceutical tech company that operates under two main segments: Pharmaceuticals and Consumer Wellness. In the Pharmaceuticals segment, Innocan focuses on developing innovative drug delivery platform technologies comprises with cannabinoids science, to treat various conditions to improve patients' quality of life. This segment involves two drug delivery technologies: (i) LPT CBD-loaded liposome platform facilitating exact dosing and the prolonged and controlled release of CBD into the blood stream. The LPT delivery platform research is in the preclinical trial phase for two indications: Epilepsy and Pain Management. In the Consumer Wellness segment, Innocan develops and markets a wide portfolio of innovative and high-performance self-care products to promote a healthier lifestyle. Under this segment Innocan has established a Joint Venture by the name of BI Sky Global Ltd. that focuses developing on advanced targeted online sales. For further information, please contact: For Innocan Pharma Corporation: Iris Bincovich, CEO +1 5162104025 +972-54-3012842 +442037699377 [email protected] NEITHER THE CANADIAN SECURITIES EXCHANGE NOR ITS REGULATION SERVICES PROVIDER HAVE REVIEWED OR ACCEPT RESPONSIBILITY FOR THE ADEQUACY OR ACCURACY OF THIS RELEASE. Disclaimer Regarding Financial Information The financial information presented in this press release is based on preliminary, unaudited financial statements prepared by management, for the fourth quarter and fiscal year ended December 31, 2023. Accordingly, such financial information may be subject to change. While the Company does not expect there to be any material changes to the financial information presented in this press release, to the extent that it is inconsistent with the information contained in the Audited Financial Statements, the financial information contained in this news release shall be deemed to be modified or superseded by such Audited Financial Statements. The making of a modifying or superseding statement shall not be deemed an admission for any purposes that the modified or superseded statement, when made, constituted a misrepresentation for purposes of applicable securities laws. Caution regarding forward-looking information Certain information set forth in this news release, including, without limitation, the Company's positioning in the global pain management market, expectations regarding the size of the human and veterinary pain management markets, growth potential for the Company's products as they are introduced to the market, plans for strategic expansion in the human pharmaceuticals, veterinary and topical market segments, statements relating to the Company's financial results for Q4 2023 and the 2023 fiscal year, expectations regarding the timing for submission of the Company's pre-investigational new drug applications to the FDA, and expectations regarding the Company's pending patent applications, is forward-looking information within the meaning of applicable securities laws. By its nature, forward-looking information is subject to numerous risks and uncertainties, some of which are beyond Innocan's control. The forward-looking information contained in this news release is based on certain key expectations and assumptions made by Innocan, including expectations and assumptions concerning the anticipated benefits of the products, satisfaction of regulatory requirements in various jurisdictions and satisfactory completion of requisite production and distribution arrangements. Forward-looking information is subject to various risks and uncertainties which could cause actual results and experience to differ materially from the anticipated results or expectations expressed in this news release. The key risks and uncertainties include but are not limited to: general global and local (national) economic, political, market and business conditions; governmental and regulatory requirements and actions by governmental authorities; and potential disruption of relationships with suppliers, manufacturers, customers, business partners and competitors. There are also risks that are inherent in the nature of product distribution, including import / export matters and the failure to obtain any required regulatory and other approvals (or to do so in a timely manner) and availability in each market of product inputs and finished products. The anticipated timeline for entry to markets may change for a number of reasons, including the inability to secure necessary regulatory requirements, or the need for additional time to conclude and/or satisfy the manufacturing and distribution arrangements. As a result of the foregoing, readers should not place undue reliance on the forward-looking information contained in this news release concerning the timing of launch of product distribution. A comprehensive discussion of other risks that impact Innocan can also be found in Innocan's public reports and filings which are available under Innocan's profile at . Readers are cautioned that undue reliance should not be placed on forward-looking information as actual results may vary materially from the forward-looking information. Innocan does not undertake to update, correct or revise any forward-looking information as a result of any new information, future events or otherwise, except as may be required by applicable law. [1] One in Five U.S. Adults Have Chronic Pain — Pain News Network, Study finds high rates of persistent chronic pain among US adults (medicalxpress.com); Pain Management Therapeutics Market Size Report 2022 to 2030 (precedenceresearch.com) [2] Pain Management Drugs Market Share, Trends & Forecast, 2032 (gminsights.com) [3]Study finds high rates of persistent chronic pain among US adults (medicalxpress.com), [4] Veterinary Medicine Market - Trends, Growth & Size (mordorintelligence.com) Logo: SOURCE Innocan Pharma Corporation

Financial Statement

29 Jan 2024

·www.biospace.com

Sarepta Therapeutics Announces Positive Data from Part B of MOMENTUM, a Phase 2 Study of SRP-5051 in Patients with Duchenne Muscular Dystrophy Amenable to Skipping Exon 51

At target dose (~30 mg/kg), SRP-5051 dosed monthly resulted in mean dystrophin expression of 5.17% and mean exon skipping of 11.11% at 28 weeks (n=20) The data support a positive benefit-risk pro SRP-5051 Sarepta will host a conference call at 8:30 a.m. Eastern time on Jan. 29, 2024 CAMBRIDGE, Mass.--(BUSINESS WIRE)-- Sarepta Therapeutics, Inc. (NASDAQ:SRPT), the leader in precision genetic medicine for rare diseases, today announced positive data from Part B of the MOMENTUM study (Study SRP-5051-201), a global, Phase 2, multi-ascending dose clinical trial of SRP-5051 (vesleteplirsen) that enrolled patients aged 8 to 21 years. SRP-5051 is a next-generation peptide phosphorodiamidate morpholino oligomer (PPMO) treatment for patients with Duchenne muscular dystrophy who are amenable to exon 51 skipping. Data from Part B of MOMENTUM found that at the higher, target dose, approximately 30 mg/kg dosed every four weeks, SRP-5051 resulted in mean dystrophin expression of 5.17%, and mean exon skipping of 11.11% at 28 weeks (n=20). Consistent dystrophin expression was seen in ambulatory (4.76%, n=11) and non-ambulatory (5.67%, n=9) participants at 28 weeks. Hypomagnesemia has previously been identified in patients taking SRP-5051 and was managed and monitored through prophylactic magnesium supplementation as part of the study protocol. “SRP-5051 dosed every four weeks is showing substantially higher increases in dystrophin and exon skipping compared to eteplirsen dosed weekly,” said Louise Rodino-Klapac, Ph.D., executive vice president, chief scientific officer and head of research and development, Sarepta Therapeutics. “The data suggest a favorable benefit-risk pro SRP-5051 and we look forward to discussing the results and next steps with FDA. As the leader in Duchenne, Sarepta is committed to advancing meaningful treatments for those with Duchenne and other rare diseases where there is unmet need.” High dose results at 28 weeks (~30 mg/kg, dosed every four weeks, n=20): 5.17% mean dystrophin expression as measured by western blot 4.53% mean change from baseline, P < 0.0001 Mean exon skipping of 11.11%, as measured by digital drop polymerase chain reaction (ddPCR), and a mean change from baseline in exon skipping of 10.07% The changes from baseline represent a 12.2-fold increase in dystrophin expression and a 24.6-fold increase in exon skipping compared to a weekly 30 mg/kg dose of eteplirsen at 24 weeks (mean dystrophin expression of 0.82%, mean exon skipping of 0.59%, n=16). Low dose results at 28 weeks (~20 mg/kg, dosed every four weeks, n=20): 2.81% mean dystrophin expression as measured by western blot 1.60% mean change from baseline, P= 0.0012 Mean exon skipping of 2.47%, as measured by ddPCR, and a mean change from baseline in exon skipping of 2.00% The changes from baseline represent a 4.3-fold increase in dystrophin expression and a 4.9-fold increase in exon skipping compared to a weekly 30 mg/kg dose of eteplirsen at 24 weeks. “The dystrophin production delivered by SRP-5051 in the MOMENTUM study is very encouraging. Importantly, with effective supplementation and monitoring, we have not seen additional complications from the hypomagnesemia,” said Eugenio Mercuri, M.D., Ph.D., head of the Neuromuscular Unit, Catholic University, Rome, Italy, and an investigator in the study. “The results with SRP-5051 to date suggest it could play an important role in the treatment of Duchenne patients with a confirmed exon 51-amenable mutation.” There were seven serious, treatment-emergent adverse events in MOMENTUM Part B, four serious events of hypomagnesemia and three serious cases of hypokalemia. Hypomagnesemia has been seen in earlier clinical studies of SRP-5051 and, throughout MOMENTUM Part B, supplemental magnesium was administered prophylactically. No treatment-related discontinuations occurred in the study. Conference call details At 8:30 a.m. Eastern time on Jan. 29, 2024, Sarepta will host a conference call and webcast to discuss the results. The event will be webcast live under the investor relations section of Sarepta’s website at and following the event a replay will be archived there for one year. Interested parties participating by phone will need to register using this online form. After registering for dial-in details, all phone participants will receive an auto-generated e-mail containing a link to the dial-in number along with a personal PIN number to use to access the event by phone. About SRP-5051 (vesleteplirsen) SRP-5051 is an investigational agent using Sarepta’s PPMO chemistry and exon-skipping technology to skip exon 51 of the dystrophin gene. SRP-5051 is designed to bind to exon 51 of dystrophin pre-mRNA, resulting in exclusion of this exon during mRNA processing in patients with genetic mutations that are amenable to exon 51 skipping. Exon skipping is intended to allow for production of an internally shortened dystrophin protein. PPMO is Sarepta’s next-generation chemistry platform designed around a proprietary cell-penetrating peptide conjugated to the PMO backbone, with the goal of increasing tissue penetration, increasing exon skipping, and significantly increasing dystrophin production. Around 13% of Duchenne patients have mutations that make them amenable to skipping exon 51. If successful, the PPMO offers the potential for improved efficacy and less frequent dosing for patients. About MOMENTUM (Study SRP-5051-201) MOMENTUM is a global, Phase 2, multi-arm, ascending dose study of SRP-5051, infused every four weeks, and will assess dystrophin protein levels in skeletal muscle tissue following SRP-5051 treatment. The study will also assess safety and tolerability. Part B enrolled 40 participants, both ambulant and non-ambulant, between the ages of 8 to 21 at sites in the U.S., Canada, and Europe. More information can be found on . About EXONDYS 51 EXONDYS 51 (eteplirsen) uses Sarepta’s proprietary phosphorodiamidate morpholino oligomer (PMO) chemistry and exon-skipping technology to bind to exon 51 of dystrophin pre-mRNA, resulting in exclusion, or “skipping”, of this exon during mRNA processing in patients with genetic mutations that are amenable to exon 51 skipping. Exon skipping is intended to allow for production of an internally truncated dystrophin protein. EXONDYS 51 is indicated for the treatment of Duchenne muscular dystrophy in patients who have a confirmed mutation of the dystrophin gene that is amenable to exon 51 skipping. This indication is approved under accelerated approval based on an increase in dystrophin production in skeletal muscle observed in some patients treated with EXONDYS 51. Continued approval may be contingent upon verification of a clinical benefit in confirmatory trials. EXONDYS 51 has met the full statutory standards for safety and effectiveness and as such is not considered investigational or experimental. Important Safety Information About EXONDYS 51 Hypersensitivity reactions, bronchospasm, chest pain, cough, tachycardia, and urticaria have occurred in patients who were treated with EXONDYS 51. If a hypersensitivity reaction occurs, institute appropriate medical treatment and consider slowing the infusion or interrupting the EXONDYS 51 therapy. Adverse reactions in Duchenne patients (N=8) treated with EXONDYS 51 30 mg or 50 mg/kg/week by intravenous (IV) infusion with an incidence of at least 25% more than placebo (N=4) (Study 1, 24 weeks) were (EXONDYS 51, placebo): balance disorder (38%, 0%), vomiting (38%, 0%) and contact dermatitis (25%, 0%). The most common adverse reactions were balance disorder and vomiting. Because of the small numbers of patients, these represent crude frequencies that may not reflect the frequencies observed in practice. The 50 mg/kg once weekly dosing regimen of EXONDYS 51 is not recommended. The following adverse reactions have been identified during observational studies that were conducted as part of the clinical development program and continued post approval. In open-label observational studies, 163 patients received at least one intravenous dose of EXONDYS 51, with doses ranging between 0.5 mg/kg (0.017 times the recommended dosage) and 50 mg/kg (1.7 times the recommended dosage). All patients were male and had genetically confirmed Duchenne muscular dystrophy. Age at study entry was 6 months to 19 years. Most (85%) patients were Caucasian. The most common adverse reactions from observational clinical studies (N=163) seen in greater than 10% of the study population were headache, cough, rash, and vomiting. For further information, please see the full Prescribing Information. About Sarepta Therapeutics Sarepta is on an urgent mission: engineer precision genetic medicine for rare diseases that devastate lives and cut futures short. We hold leadership positions in Duchenne muscular dystrophy (DMD) and limb-girdle muscular dystrophies (LGMDs), and we currently have more than 40 programs in various stages of development. Our vast pipeline is driven by our multi-platform Precision Genetic Medicine Engine in gene therapy, RNA and gene editing. For more information, please visit or follow us on Twitter, LinkedIn, Instagram and Facebook. Internet Posting of Information We routinely post information that may be important to investors in the 'For Investors' section of our website at . We encourage investors and potential investors to consult our website regularly for important information about us. Forward-Looking Statements In order to provide Sarepta’s investors with an understanding of its current results and future prospects, this press release contains statements that are forward-looking. Any statements contained in this press release that are not statements of historical fact may be deemed to be forward-looking statements. Words such as “believes,” “anticipates,” “plans,” “expects,” “will,” “may,” “intends,” “prepares,” “looks,” “potential,” “possible” and similar expressions are intended to identify forward-looking statements. These forward-looking statements include statements relating to our future operations, financial performance and projections, business plans, market opportunities, priorities and research and development programs and technologies; the potential benefits of our technologies and scientific approaches; the potential benefits of SRP-5051, including its potential for higher dystrophin and exon-skipping than eteplirsen and a favorable benefit-risk profile, including that hypomagnesemia is manageable; and plans and milestones, including discussing results and next steps with FDA. These forward-looking statements involve risks and uncertainties, many of which are beyond Sarepta’s control. Actual results could materially differ from those stated or implied by these forward-looking statements as a result of such risks and uncertainties. Known risk factors include the following: success in preclinical and clinical trials, especially if based on a small patient sample, does not ensure that later clinical trials will be successful, and the results of future research may not be consistent with past positive results or may fail to meet regulatory approval requirements for the safety and efficacy of product candidates; certain programs may never advance in the clinic or may be discontinued for a number of reasons, including regulators imposing a clinical hold and us suspending or terminating clinical research or trials; if the actual number of patients suffering from the diseases we aim to treat is smaller than estimated, our revenue and ability to achieve profitability may be adversely affected; because we are developing product candidates for the treatment of certain diseases in which there is little clinical experience and we are using new endpoints or methodologies, there is increased risk that the FDA, the EMA or other regulatory authorities may not consider the endpoints of our clinical trials to provide clinically meaningful results and that these results may be difficult to analyze; we may not be able to execute on our business plans, including meeting our expected or planned regulatory milestones and timelines, research and clinical development plans, and bringing our product candidates to market, for various reasons, some of which may be outside of our control, including possible limitations of company financial and other resources, manufacturing limitations that may not be anticipated or resolved for in a timely manner, and regulatory, court or agency decisions, such as decisions by the United States Patent and Trademark Office with respect to patents that cover our product candidates; and those risks identified under the heading “Risk Factors” in our most recent Annual Report on Form 10-K for the year ended December 31, 2022 and our most recent Quarterly Report on Form 10-Q filed with the Securities and Exchange Commission (SEC) as well as other SEC filings made by the Company which you are encouraged to review.

Clinical ResultPhase 2Drug ApprovalPhase 1

100 Deals associated with Magnesium Carbonate

R&D Status

10 top approved records.

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Indication	Country/Location	Organization	Date
Constipation	Japan	Yamazen Co. Ltd.	02 Feb 1951
Duodenal Ulcer	Japan	Yamazen Co. Ltd.	02 Feb 1951
Gastritis	Japan	Yamazen Co. Ltd.	02 Feb 1951
Gastrointestinal Diseases	Japan	Yamazen Co. Ltd.	02 Feb 1951
Stomach Ulcer	Japan	Yamazen Co. Ltd.	02 Feb 1951

Clinical Result

Indication

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


EASD2023	Not Applicable	Diabetes Mellitus, Type 2 serum magnesium level	14	Magnesium supplementation (15 mmol/day)	nwxeruuspk(trfgvphyxd) = xsmyvyohzg rwczyqlrix (yxaxestlsv ) View more	Negative	05 Oct 2023
				Magnesium (Placebo)	nwxeruuspk(trfgvphyxd) = pylujbeaul rwczyqlrix (yxaxestlsv ) View more
ASN2022	Phase 1	Mesothelioma	5	High Dose Intravenous Magnesium	gsuhqksgxv(snftueoqsv) = exaqjsyeov ovyysstonj (ffmqwpbuta, 1 - 1.1) View more	Positive	04 Nov 2022
ERA2022	Not Applicable	pre-dialysis Mg levels	206	Magnesium (Mg serum level < 2.2 mg/dL)	mbtigrjnga(lkfmuxvxqh) = xdfyzkibzm ngcxuiaxhn (mthtdoibkc )	Positive	03 May 2022
				Magnesium (Mg serum level > 2.2 mg/dL)	mbtigrjnga(lkfmuxvxqh) = glgqyxgpdw ngcxuiaxhn (mthtdoibkc )
NIH Field Administration of Stroke Therapy Magnesium (FAST-MAG) (ISC2022)	Not Applicable	Brain Ischemia low serum magnesium levels	1,245	Magnesium	mosavafopn(mnzccpeinm) = opjairtuiq naupnusvuu (whomuswfga )	-	01 Feb 2022
				Placebo	mosavafopn(mnzccpeinm) = oaiayxxwdf naupnusvuu (whomuswfga )
ESC2021	Not Applicable	Diabetes Mellitus \| Heart Failure diabetes mellitus	606	magnesium	mttonssaxy(skaxakpojo) = rcuftdoqrj quydhmlkib (iwasysikej ) View more	-	29 Jun 2021
				magnesium	mttonssaxy(skaxakpojo) = ofzpevcfmw quydhmlkib (iwasysikej ) View more
ASN2019	Not Applicable	Chronic Kidney Diseases plasma magnesium	20	Magnesium (Patients with CKD 3-4 without diabetes)	jslrtaceiv(gatzrcjpde) = avkrecnigv wcvbyrhkgh (ecjhjzzgkd, 0.04)	Positive	05 Nov 2019
				Magnesium (Healthy controls)	jslrtaceiv(gatzrcjpde) = jzhezyivhx wcvbyrhkgh (ecjhjzzgkd, 0.07)
ASN2018	Not Applicable	Chronic Kidney Diseases	335	Magnesium (CKD patients)	paxejyljls(mtolsbhwgq) = gphkcwcaab cfyutnulgd (xgaiahkmnv )	-	23 Oct 2018
				Magnesium (Healthy participants)	paxejyljls(mtolsbhwgq) = qwcymnsbjk cfyutnulgd (xgaiahkmnv )
MACH study (ESH2018)	Not Applicable	Heart Diseases NTproBNP levels \| Serum creatinine levels	21	Magnesium Orotate Therapy	uafapeayst(adbkdixgsi) = 75% of magnesium treated patients reported an improvement of quality of life gfantkpvxj (fmvrosfdsj ) View more	Positive	01 Jun 2018
				Magnesium (Control Group)
MP691 (ERA2017)	Not Applicable	-	64	Sucroferric oxyhydroxide	ibzfcsejdz(beaqxsqxro) = gqnxmtpnvj ppwcfcxrkh (dqtksiubgg ) View more	Positive	26 May 2017
				Sevelamer and/or calcium acetate + magnesium carbonate	ibzfcsejdz(beaqxsqxro) = xeohfnwxij ppwcfcxrkh (dqtksiubgg ) View more
ACR2016	Not Applicable	Electrolyte imbalance	-	Denosumab 60mg	(coqgtrmdbl) = detected in 3 patients: 2 patients 1 week after administration, and 1 patient 2 weeks after. 1 patient had hypocalcemia 1 week after the second administration chxecamjqg (ndgjdlvtcs ) View more	Positive	13 Nov 2016
				Oral calcium tablet combined with native vitamin D and magnesium

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