Your search keyword '"Almannai, Mohammed"' showing total 6 results

1. Mitochondrial DNA maintenance defects: potential therapeutic strategies.

Author

Almannai, Mohammed, El-Hattab, Ayman W., Azamian, Mahshid S., Ali, May, and Scaglia, Fernando

Subjects

*MITOCHONDRIAL DNA, *MITOCHONDRIAL pathology, *NUCLEAR proteins, *CLINICAL trials, *MITOCHONDRIA, *PATHOLOGICAL physiology

Abstract

Mitochondrial DNA (mtDNA) replication depends on the mitochondrial import of hundreds of nuclear encoded proteins that control the mitochondrial genome maintenance and integrity. Defects in these processes result in an expanding group of disorders called mtDNA maintenance defects that are characterized by mtDNA depletion and/or multiple mtDNA deletions with variable phenotypic manifestations. As it applies for mitochondrial disorders in general, current treatment options for mtDNA maintenance defects are limited. Lately, with the development of model organisms, improved understanding of the pathophysiology of these disorders, and a better knowledge of their natural history, the number of preclinical studies and existing and planned clinical trials has been increasing. In this review, we discuss recent preclinical studies and current and future clinical trials concerning potential therapeutic options for the different mtDNA maintenance defects. [ABSTRACT FROM AUTHOR]

Published

2022

2. Nitric Oxide Deficiency in Mitochondrial Disorders: The Utility of Arginine and Citrulline.

Author

Almannai, Mohammed and El-Hattab, Ayman W.

Subjects

MELAS syndrome, MITOCHONDRIAL pathology, CITRULLINE, ARGININE, NITRIC oxide, NITRIC-oxide synthases

Abstract

Mitochondrial diseases represent a growing list of clinically heterogeneous disorders that are associated with dysfunctional mitochondria and multisystemic manifestations. In spite of a better understanding of the underlying pathophysiological basis of mitochondrial disorders, treatment options remain limited. Over the past two decades, there is growing evidence that patients with mitochondrial disorders have nitric oxide (NO) deficiency due to the limited availability of NO substrates, arginine and citrulline; decreased activity of nitric oxide synthase (NOS); and NO sequestration. Studies evaluating the use of arginine in patients with mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) presenting with stroke-like episodes showed symptomatic improvement after acute administration as well as a reduction in the frequency and severity of stroke-like episodes following chronic use. Citrulline, another NO precursor, was shown through stable isotope studies to result in a greater increase in NO synthesis. Recent studies showed a positive response of arginine and citrulline in other mitochondrial disorders besides MELAS. Randomized-controlled studies with a larger number of patients are warranted to better understand the role of NO deficiency in mitochondrial disorders and the efficacy of NO precursors as treatment modalities in these disorders. [ABSTRACT FROM AUTHOR]

Published

2021

3. Clinical trials in mitochondrial disorders, an update.

Author

Almannai, Mohammed, El-Hattab, Ayman W., Ali, May, Soler-Alfonso, Claudia, and Scaglia, Fernando

Subjects

*MITOCHONDRIAL pathology, *CLINICAL trials, *MITOCHONDRIA, *NANOTECHNOLOGY, *SYMPTOMS

Abstract

Mitochondrial disorders comprise a molecular and clinically diverse group of diseases that are associated with mitochondrial dysfunction leading to multi-organ disease. With recent advances in molecular technologies, the understanding of the pathomechanisms of a growing list of mitochondrial disorders has been greatly expanded. However, the therapeutic approaches for mitochondrial disorders have lagged behind with treatment options limited mainly to symptom specific therapies and supportive measures. There is an increasing number of clinical trials in mitochondrial disorders aiming for more specific and effective therapies. This review will cover different treatment modalities currently used in mitochondrial disorders, focusing on recent and ongoing clinical trials. [ABSTRACT FROM AUTHOR]

Published

2020

4. FARS2 deficiency; new cases, review of clinical, biochemical, and molecular spectra, and variants interpretation based on structural, functional, and evolutionary significance.

Author

Almannai, Mohammed, Wang, Julia, Dai, Hongzheng, El-Hattab, Ayman W., Faqeih, Eissa A., Saleh, Mohammed A., Al Asmari, Ali, Alwadei, Ali H., Aljadhai, Yaser I., AlHashem, Amal, Tabarki, Brahim, Lines, Matthew A., Grange, Dorothy K., Benini, Ruba, Alsaman, Abdulaziz S., Mahmoud, Adel, Katsonis, Panagiotis, Lichtarge, Olivier, and Wong, Lee-Jun C.

Subjects

*MITOCHONDRIAL pathology, *TRANSFER RNA, *PHENYLALANINE, *HUMAN phenotype, *MISSENSE mutation

Abstract

Abstract An increasing number of mitochondrial diseases are found to be caused by pathogenic variants in nuclear encoded mitochondrial aminoacyl-tRNA synthetases. FARS2 encodes mitochondrial phenylalanyl-tRNA synthetase (mtPheRS) which transfers phenylalanine to its cognate tRNA in mitochondria. Since the first case was reported in 2012, a total of 21 subjects with FARS2 deficiency have been reported to date with a spectrum of disease severity that falls between two phenotypes; early onset epileptic encephalopathy and a less severe phenotype characterized by spastic paraplegia. In this report, we present an additional 15 individuals from 12 families who are mostly Arabs homozygous for the pathogenic variant Y144C, which is associated with the more severe early onset phenotype. The total number of unique pathogenic FARS2 variants known to date is 21 including three different partial gene deletions reported in four individuals. Except for the large deletions, all variants but two (one in-frame deletion of one amino acid and one splice-site variant) are missense. All large deletions and the single splice-site variant are in trans with a missense variant. This suggests that complete loss of function may be incompatible with life. In this report, we also review structural, functional, and evolutionary significance of select FARS2 pathogenic variants reported here. [ABSTRACT FROM AUTHOR]

Published

2018

5. Therapies for mitochondrial diseases and current clinical trials.

Author

El-Hattab, Ayman W., Zarante, Ana Maria, Almannai, Mohammed, and Scaglia, Fernando

Subjects

*MITOCHONDRIAL pathology, *CLINICAL trials, *OXIDATIVE phosphorylation, *GENETIC code, *ETIOLOGY of diseases, *THERAPEUTICS

Abstract

Mitochondrial diseases are a clinically and genetically heterogeneous group of disorders that result from dysfunction of the mitochondrial oxidative phosphorylation due to molecular defects in genes encoding mitochondrial proteins. Despite the advances in molecular and biochemical methodologies leading to better understanding of the etiology and mechanism of these diseases, there are still no satisfactory therapies available for mitochondrial disorders. Treatment for mitochondrial diseases remains largely symptomatic and does not significantly alter the course of the disease. Based on limited number of clinical trials, several agents aiming at enhancing mitochondrial function or treating the consequences of mitochondrial dysfunction have been used. Several agents are currently being evaluated for mitochondrial diseases. Therapeutic strategies for mitochondrial diseases include the use of agents enhancing electron transfer chain function (coenzyme Q 10 , idebenone, riboflavin, dichloroacetate, and thiamine), agents acting as energy buffer (creatine), antioxidants (vitamin C, vitamin E, lipoic acid, cysteine donors, and EPI-743), amino acids restoring nitric oxide production (arginine and citrulline), cardiolipin protector (elamipretide), agents enhancing mitochondrial biogenesis (bezafibrate, epicatechin, and RTA 408), nucleotide bypass therapy, liver transplantation, and gene therapy. Although, there is a lack of curative therapies for mitochondrial disorders at the current time, the increased number of clinical research evaluating agents that target different aspects of mitochondrial dysfunction is promising and is expected to generate more therapeutic options for these diseases in the future. [ABSTRACT FROM AUTHOR]

Published

2017

6. Utility of citrulline in treating hypoargininemia in children with MELAS.

Author

El-Hattab, Ayman W., Emrick, Lisa T., Chanprasert, Sirisak, Hsu, Jean W., Almannai, Mohammed, Craigen, William J., Jahoor, Farook, and Scaglia, Fernando

Subjects

*MELAS syndrome, *LACTIC acidosis, *MITOCHONDRIAL pathology, *JUVENILE diseases, *CITRULLINE, *PHYSIOLOGICAL effects of nitric oxide, *AMINO acids

Published

2015