Your search keyword '"Mustafa S Makia"' showing total 20 results

1. ROM1 is redundant to PRPH2 as a molecular building block of photoreceptor disc rims

Author

Tylor R Lewis, Mustafa S Makia, Carson M Castillo, Ying Hao, Muayyad R Al-Ubaidi, Nikolai P Skiba, Shannon M Conley, Vadim Y Arshavsky, and Muna I Naash

Subjects

vision, retina, photoreceptor, outer segment, cilia, tetraspanin, Medicine, Science, Biology (General), QH301-705.5

Abstract

Visual signal transduction takes place within a stack of flattened membranous ‘discs’ enclosed within the light-sensitive photoreceptor outer segment. The highly curved rims of these discs, formed in the process of disc enclosure, are fortified by large hetero-oligomeric complexes of two homologous tetraspanin proteins, PRPH2 (a.k.a. peripherin-2 or rds) and ROM1. While mutations in PRPH2 affect the formation of disc rims, the role of ROM1 remains poorly understood. In this study, we found that the knockout of ROM1 causes a compensatory increase in the disc content of PRPH2. Despite this increase, discs of ROM1 knockout mice displayed a delay in disc enclosure associated with a large diameter and lack of incisures in mature discs. Strikingly, further increasing the level of PRPH2 rescued these morphological defects. We next showed that disc rims are still formed in a knockin mouse in which the tetraspanin body of PRPH2 was replaced with that of ROM1. Together, these results demonstrate that, despite its contribution to the formation of disc rims, ROM1 can be replaced by an excess of PRPH2 for timely enclosure of newly forming discs and establishing normal outer segment structure.

Published

2023

2. Author Correction: Downregulation of rhodopsin is an effective therapeutic strategy in ameliorating peripherin-2-associated inherited retinal disorders

Author

Christian T. Rutan Woods, Mustafa S. Makia, Tylor R. Lewis, Ryan Crane, Stephanie Zeibak, Paul Yu, Mashal Kakakhel, Carson M. Castillo, Vadim Y. Arshavsky, Muna I. Naash, and Muayyad R. Al-Ubaidi

Subjects

Science

Published

2024

3. Downregulation of rhodopsin is an effective therapeutic strategy in ameliorating peripherin-2-associated inherited retinal disorders

Author

Christian T. Rutan Woods, Mustafa S. Makia, Tylor R. Lewis, Ryan Crane, Stephanie Zeibak, Paul Yu, Mashal Kakakhel, Carson M. Castillo, Vadim Y. Arshavsky, Muna I. Naash, and Muayyad R. Al-Ubaidi

Subjects

Science

Abstract

Abstract Given the absence of approved treatments for pathogenic variants in Peripherin-2 (PRPH2), it is imperative to identify a universally effective therapeutic target for PRPH2 pathogenic variants. To test the hypothesis that formation of the elongated discs in presence of PRPH2 pathogenic variants is due to the presence of the full complement of rhodopsin in absence of the required amounts of functional PRPH2. Here we demonstrate the therapeutic potential of reducing rhodopsin levels in ameliorating disease phenotype in knockin models for p.Lys154del (c.458-460del) and p.Tyr141Cys (c.422 A > G) in PRPH2. Reducing rhodopsin levels improves physiological function, mitigates the severity of disc abnormalities, and decreases retinal gliosis. Additionally, intravitreal injections of a rhodopsin-specific antisense oligonucleotide successfully enhance the physiological function of photoreceptors and improves the ultrastructure of discs in mutant mice. Presented findings shows that reducing rhodopsin levels is an effective therapeutic strategy for the treatment of inherited retinal degeneration associated with PRPH2 pathogenic variants.

Published

2024

4. Effective intravitreal gene delivery to retinal pigment epithelium with hyaluronic acid nanospheres

Author

Ryan Crane, Mustafa S. Makia, Stephanie Zeibak, Lars Tebbe, Larissa Ikele, Christian Rutan Woods, Shannon M. Conley, Ghanashyam Acharya, Muna I. Naash, and Muayyad R. Al-Ubaidi

Subjects

MT: Delivery Strategies, hyaluronic acid, retina, photoreceptor, retinal pigment epithelium, intravitreal injection, Therapeutics. Pharmacology, RM1-950

Abstract

Inherited retinal degeneration (IRD) can cause a wide range of different forms of vision loss and blindness, and in spite of extensive advancements in gene therapy research, therapeutic approaches for targeting IRDs are still lacking. We have recently developed an approach for the intravitreal co-delivery of hyaluronic-acid nanospheres (HA-NSs) with sulfotyrosine (ST), effectively reaching the outer retina from the vitreal cavity. Here, our goal was to understand whether DNA-filled HA-NSs could generate gene expression in the outer retina. TxRed-labeled HA-NSs were compacted with plasmid DNA carrying a GFP reporter gene and intravitreally injected into the mouse retina. Follow-up at 4 weeks showed widespread gene expression in the outer retina and reduced, albeit present, expression at 8 weeks post-injection. Further analysis revealed this expression to be largely localized to the retinal pigment epithelium (RPE). These data show that intravitreal delivery of HA-NSs is a promising non-viral platform for the delivery of therapeutic genes and can generate pan-tissue, persistent gene expression in the RPE.

Published

2024

5. Riboflavin deficiency leads to irreversible cellular changes in the RPE and disrupts retinal function through alterations in cellular metabolic homeostasis

Author

Tirthankar Sinha, Larissa Ikelle, Mustafa S. Makia, Ryan Crane, Xue Zhao, Mashal Kakakhel, Muayyad R. Al-Ubaidi, and Muna I. Naash

Subjects

Flavins, Retbindin, Ariboflavinosis, Metabolism, Retinal degeneration, RPE dystrophy, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Ariboflavinosis is a pathological condition occurring as a result of riboflavin deficiency. This condition is treatable if detected early enough, but it lacks timely diagnosis. Critical symptoms of ariboflavinosis include neurological and visual manifestations, yet the effects of flavin deficiency on the retina are not well investigated. Here, using a diet induced mouse model of riboflavin deficiency, we provide the first evidence of how retinal function and metabolism are closely intertwined with riboflavin homeostasis. We find that diet induced riboflavin deficiency causes severe decreases in retinal function accompanied by structural changes in the neural retina and retinal pigment epithelium (RPE). This is preceded by increased signs of cellular oxidative stress and metabolic disorder, in particular dysregulation in lipid metabolism, which is essential for both photoreceptors and the RPE. Though many of these deleterious phenotypes can be ameliorated by riboflavin supplementation, our data suggests that some patients may continue to suffer from multiple pathologies at later ages. These studies provide an essential cellular and mechanistic foundation linking defects in cellular flavin levels with the manifestation of functional deficiencies in the visual system and paves the way for a more in-depth understanding of the cellular consequences of ariboflavinosis.

Published

2022

6. Photoreceptor Disc Enclosure Occurs in the Absence of Normal Peripherin-2/rds Oligomerization

Author

Tylor R. Lewis, Mustafa S. Makia, Mashal Kakakhel, Muayyad R. Al-Ubaidi, Vadim Y. Arshavsky, and Muna I. Naash

Subjects

photoreceptor, peripherin, outer segment, disc, retina, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Mutations in the peripherin-2 gene (PRPH2, also known as rds) cause a heterogeneous range of autosomal dominant retinal diseases. PRPH2 encodes a photoreceptor-specific tetraspanin protein, PRPH2, that is a main structural component of the photoreceptor outer segment. PRPH2 distributes to the rims of outer segment disc membranes as they undergo the process of disc membrane enclosure. Within these rims, PRPH2 exists in homo-oligomeric form or as a hetero-oligomer with another tetraspanin protein, ROM1. While complete loss of PRPH2 prevents photoreceptor outer segment formation, mutations affecting the state of its oligomerization, including C150S, C213Y and Y141C, produce outer segment structural defects. In this study, we addressed whether any of these mutations also affect disc enclosure. We employed recently developed methodology for ultrastructural analysis of the retina, involving tissue processing with tannic acid, to assess the status of disc enclosure in knockin mouse models bearing either one or two alleles of the C150S, C213Y and Y141C PRPH2 mutations. While varying degrees of outer segment structural abnormalities were observed in each of these mouse models, they contained both newly forming “open” discs and mature “enclosed” discs. These data demonstrate that normal PRPH2 oligomerization is not essential for photoreceptor disc enclosure.

Published

2020

7. Co-Injection of Sulfotyrosine Facilitates Retinal Uptake of Hyaluronic Acid Nanospheres Following Intravitreal Injection

Author

Aiden Eblimit, Mustafa S. Makia, Daniel Strayve, Ryan Crane, Shannon M. Conley, Tirthankar Sinha, Ghanashyam Acharya, Muayyad R. Al-Ubaidi, and Muna I. Naash

Subjects

hyaluronic acid nanospheres, retina, photoreceptor, RPE, intravitreal injection, sulfotyrosine, Pharmacy and materia medica, RS1-441

Abstract

Gene and drug delivery to the retina is a critical therapeutic goal. While the majority of inherited forms of retinal degeneration affect the outer retina, specifically the photoreceptors and retinal pigment epithelium, effective targeted delivery to this region requires invasive subretinal delivery. Our goal in this work was to evaluate two innovative approaches for increasing both the persistence of delivered nanospheres and their penetration into the outer retina while using the much less invasive intravitreal delivery method. We formulated novel hyaluronic acid nanospheres (HA-NS, 250 nm and 500 nm in diameter) conjugated to fluorescent reporters and delivered them intravitreally to the adult Balb/C mouse retina. They exhibited persistence in the vitreous and along the inner limiting membrane (ILM) for up to 30 days (longest timepoint examined) but little retinal penetration. We thus evaluated the ability of the small molecule, sulfotyrosine, to disrupt the ILM, and found that 3.2 µg/µL sulfotyrosine led to significant improvement in delivery to the outer retina following intravitreal injections without causing retinal inflammation, degeneration, or loss of function. Co-delivery of sulfotyrosine and HA-NS led to robust improvements in penetration of HA-NS into the retina and accumulation along the interface between the photoreceptors and the retinal pigment epithelium. These exciting findings suggest that sulfotyrosine and HA-NS may be an effective strategy for outer retinal targeting after intravitreal injection.

Published

2021

8. Retbindin: A riboflavin Binding Protein, Is Critical for Photoreceptor Homeostasis and Survival in Models of Retinal Degeneration

Author

Ayse M. Genc, Mustafa S. Makia, Tirthankar Sinha, Shannon M. Conley, Muayyad R. Al-Ubaidi, and Muna I. Naash

Subjects

Prph2, retinal degeneration, inherited retinal degeneration, riboflavin, metabolism, flavoproteins, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The large number of inherited retinal disease genes (IRD), including the photopigment rhodopsin and the photoreceptor outer segment (OS) structural component peripherin 2 (PRPH2), has prompted interest in identifying common cellular mechanisms involved in degeneration. Although metabolic dysregulation has been shown to play an important role in the progression of the disease etiology, identifying a common regulator that can preserve the metabolic ecosystem is needed for future development of neuroprotective treatments. Here, we investigated whether retbindin (RTBDN), a rod-specific protein with riboflavin binding capability, and a regulator of riboflavin-derived cofactors flavin mononucleotide (FMN) and flavin adenine dinucleotide (FAD), is protective to the retina in different IRD models; one carrying the P23H mutation in rhodopsin (which causes retinitis pigmentosa) and one carrying the Y141C mutation in Prph2 (which causes a blended cone-rod dystrophy). RTBDN levels are significantly upregulated in both the rhodopsin (Rho)P23H/+ and Prph2Y141C/+ retinas. Rod and cone structural and functional degeneration worsened in models lacking RTBDN. In addition, removing Rtbdn worsened other phenotypes, such as fundus flecking. Retinal flavin levels were reduced in RhoP23H/+/Rtbdn−/− and Prph2Y141C/+/Rtbdn−/− retinas. Overall, these findings suggest that RTBDN may play a protective role during retinal degenerations that occur at varying rates and due to varying disease mechanisms.

Published

2020

9. The Interplay between Peripherin 2 Complex Formation and Degenerative Retinal Diseases

Author

Lars Tebbe, Mashal Kakakhel, Mustafa S. Makia, Muayyad R. Al-Ubaidi, and Muna I. Naash

Subjects

peripherin 2, retinal degeneration, retina, tetraspanin, photoreceptor, Cytology, QH573-671

Abstract

Peripherin 2 (Prph2) is a photoreceptor-specific tetraspanin protein present in the outer segment (OS) rims of rod and cone photoreceptors. It shares many common features with other tetraspanins, including a large intradiscal loop which contains several cysteines. This loop enables Prph2 to associate with itself to form homo-oligomers or with its homologue, rod outer segment membrane protein 1 (Rom1) to form hetero-tetramers and hetero-octamers. Mutations in PRPH2 cause a multitude of retinal diseases including autosomal dominant retinitis pigmentosa (RP) or cone dominant macular dystrophies. The importance of Prph2 for photoreceptor development, maintenance and function is underscored by the fact that its absence results in a failure to initialize OS formation in rods and formation of severely disorganized OS membranous structures in cones. Although the exact role of Rom1 has not been well studied, it has been concluded that it is not necessary for disc morphogenesis but is required for fine tuning OS disc size and structure. Pathogenic mutations in PRPH2 often result in complex and multifactorial phenotypes, involving not just photoreceptors, as has historically been reasoned, but also secondary effects on the retinal pigment epithelium (RPE) and retinal/choroidal vasculature. The ability of Prph2 to form complexes was identified as a key requirement for the development and maintenance of OS structure and function. Studies using mouse models of pathogenic Prph2 mutations established a connection between changes in complex formation and disease phenotypes. Although progress has been made in the development of therapeutic approaches for retinal diseases in general, the highly complex interplay of functions mediated by Prph2 and the precise regulation of these complexes made it difficult, thus far, to develop a suitable Prph2-specific therapy. Here we describe the latest results obtained in Prph2-associated research and how mouse models provided new insights into the pathogenesis of its related diseases. Furthermore, we give an overview on the current status of the development of therapeutic solutions.

Published

2020

10. Photoreceptor Disc Enclosure Is Tightly Controlled by Peripherin-2 Oligomerization

Author

Tylor R. Lewis, Muayyad R. Al-Ubaidi, Muna I. Naash, Vadim Y. Arshavsky, Mustafa S Makia, and Carson M. Castillo

Subjects

Peripherins, Mice, 03 medical and health sciences, chemistry.chemical_compound, Retinal Rod Photoreceptor Cells, medicine, Animals, Peripherin 2, Process (anatomy), Research Articles, 030304 developmental biology, 0303 health sciences, Retina, Chemistry, General Neuroscience, Cell Membrane, 030305 genetics & heredity, Membrane structure, Peripherin, Retinal, Rod Cell Outer Segment, Photoreceptor outer segment, Mice, Inbred C57BL, Membrane, medicine.anatomical_structure, Mutation, Retinal Cone Photoreceptor Cells, Biophysics, Photoreceptor Cells, Vertebrate

Abstract

Mutations in thePRPH2gene encoding the photoreceptor-specific protein PRPH2 (also known as peripherin-2 or rds) cause a broad range of autosomal dominant retinal diseases. Most of these mutations affect the structure of the light-sensitive photoreceptor outer segment, which is composed of a stack of flattened “disc” membranes surrounded by the plasma membrane. The outer segment is renewed on a daily basis in a process whereby new discs are added at the outer segment base and old discs are shed at the outer segment tip. New discs are formed as serial membrane evaginations, which eventually enclose through a complex process of membrane remodeling (completely in rods and partially in cones). As disc enclosure proceeds, PRPH2 localizes to the rims of enclosed discs where it forms oligomers which fortify the highly curved membrane structure of these rims. In this study, we analyzed the outer segment phenotypes of mice of both sexes bearing a single copy of either the C150S or the Y141C PRPH2 mutation known to prevent or increase the degree of PRPH2 oligomerization, respectively. Strikingly, both mutations increased the number of newly forming, not-yet-enclosed discs, indicating that the precision of disc enclosure is regulated by PRPH2 oligomerization. Without tightly controlled enclosure, discs occasionally over-elongate and form large membranous “whorls” instead of disc stacks. These data show that the defects in outer segment structure arising from abnormal PRPH2 oligomerization are manifested at the stage of disc enclosure.SIGNIFICANCE STATEMENTThe light-sensitive photoreceptor outer segment contains a stack of flattened “disc” membranes that are surrounded, or “enclosed,” by the outer segment membrane. Disc enclosure is an adaptation increasing photoreceptor light sensitivity by facilitating the diffusion of the second messenger along the outer segment axes. However, the molecular mechanisms by which photoreceptor discs enclose within the outer segment membrane remain poorly understood. We now demonstrate that oligomers of the photoreceptor-specific protein peripherin-2, or PRPH2, play an active role in this process. We further propose that defects in disc enclosure because of abnormal PRPH2 oligomerization result in major structural abnormalities of the outer segment, ultimately leading to loss of visual function and cell degeneration in PRPH2 mutant models and human patients.

Published

2021

11. Syntaxin 3 is essential for photoreceptor outer segment protein trafficking and survival

Author

Mustafa S Makia, Muayyad R. Al-Ubaidi, Mashal Kakakhel, Lars Tebbe, Muna I. Naash, Shannon M. Conley, and David M. Sherry

Subjects

0301 basic medicine, Retinal degeneration, Rhodopsin, genetic structures, Peripherins, 030105 genetics & heredity, Mice, 03 medical and health sciences, Tetraspanin, Microtubule, medicine, Animals, Retinal Photoreceptor Cell Inner Segment, Peripherin 2, Multidisciplinary, biology, Qa-SNARE Proteins, Chemistry, Biological Sciences, Retinal Photoreceptor Cell Outer Segment, medicine.disease, Photoreceptor outer segment, eye diseases, Syntaxin 3, Cell biology, Protein Transport, 030104 developmental biology, Membrane protein, Gene Knockdown Techniques, biology.protein, sense organs, SNARE Proteins, Photoreceptor Cells, Vertebrate

Abstract

Trafficking of photoreceptor membrane proteins from their site of synthesis in the inner segment (IS) to the outer segment (OS) is critical for photoreceptor function and vision. Here we evaluate the role of syntaxin 3 (STX3), in trafficking of OS membrane proteins such as peripherin 2 (PRPH2) and rhodopsin. Photoreceptor-specific Stx3 knockouts [Stx3(f/f(iCre75)) and Stx3(f/f(CRX-Cre))] exhibited rapid, early-onset photoreceptor degeneration and functional decline characterized by structural defects in IS, OS, and synaptic terminals. Critically, in the absence of STX3, OS proteins such as PRPH2, the PRPH2 binding partner, rod outer segment membrane protein 1 (ROM1), and rhodopsin were mislocalized along the microtubules to the IS, cell body, and synaptic region. We find that the PRPH2 C-terminal domain interacts with STX3 as well as other photoreceptor SNAREs, and our findings indicate that STX3 is an essential part of the trafficking pathway for both disc (rhodopsin) and rim (PRPH2/ROM1) components of the OS.

Published

2020

12. Co-Injection of Sulfotyrosine Facilitates Retinal Uptake of Hyaluronic Acid Nanospheres following Intravitreal Injection

Author

Shannon M. Conley, Aiden Eblimit, Muayyad R. Al-Ubaidi, Ryan Crane, Muna I. Naash, Mustafa S Makia, Tirthankar Sinha, Daniel Strayve, and Ghanashyam Acharya

Subjects

Retinal degeneration, medicine.medical_specialty, retina, genetic structures, Pharmaceutical Science, Article, chemistry.chemical_compound, Pharmacy and materia medica, sulfotyrosine, Ophthalmology, Hyaluronic acid, medicine, Retina, Retinal pigment epithelium, Chemistry, intravitreal injection, Retinal, Inner limiting membrane, Penetration (firestop), medicine.disease, photoreceptor, eye diseases, RS1-441, medicine.anatomical_structure, Drug delivery, inner limiting membrane, sense organs, RPE, hyaluronic acid nanospheres

Abstract

Gene and drug delivery to the retina is a critical therapeutic goal. While the majority of inherited forms of retinal degeneration affect the outer retina, specifically the photoreceptors and retinal pigment epithelium, effective targeted delivery to this region requires invasive subretinal delivery. Our goal in this work was to evaluate two innovative approaches for increasing both the persistence of delivered nanospheres and their penetration into the outer retina while using the much less invasive intravitreal delivery method. We formulated novel hyaluronic acid nanospheres (HA-NS, 250 nm and 500 nm in diameter) conjugated to fluorescent reporters and delivered them intravitreally to the adult Balb/C mouse retina. They exhibited persistence in the vitreous and along the inner limiting membrane (ILM) for up to 30 days (longest timepoint examined) but little retinal penetration. We thus evaluated the ability of the small molecule, sulfotyrosine, to disrupt the ILM, and found that 3.2 µg/µL sulfotyrosine led to significant improvement in delivery to the outer retina following intravitreal injections without causing retinal inflammation, degeneration, or loss of function. Co-delivery of sulfotyrosine and HA-NS led to robust improvements in penetration of HA-NS into the retina and accumulation along the interface between the photoreceptors and the retinal pigment epithelium. These exciting findings suggest that sulfotyrosine and HA-NS may be an effective strategy for outer retinal targeting after intravitreal injection.

Published

2021

13. Absence of retbindin blocks glycolytic flux, disrupts metabolic homeostasis, and leads to photoreceptor degeneration

Author

Jianhai Du, James B. Hurley, Muna I. Naash, Mustafa S Makia, Muayyad R. Al-Ubaidi, and Tirthankar Sinha

Subjects

Retinal degeneration, Citric Acid Cycle, Pyruvate Kinase, PKM2, Pentose phosphate pathway, Retina, Mice, chemistry.chemical_compound, Flavins, medicine, Animals, Homeostasis, Humans, Glycolysis, Eye Proteins, Multidisciplinary, Chemistry, Retinal Degeneration, Retinal, Biological Sciences, medicine.disease, Cell biology, Citric acid cycle, Disease Models, Animal, Flux (metabolism), Pyruvate kinase

Abstract

We previously reported a model of progressive retinal degeneration resulting from the knockout of the retina-specific riboflavin binding protein, retbindin (Rtbdn(−/−)). We also demonstrated a reduction in neural retinal flavins as a result of the elimination of RTBDN. Given the role of flavins in metabolism, herein we investigated the underlying mechanism of this retinal degeneration by performing metabolomic analyses on predegeneration at postnatal day (P) 45 and at the onset of functional degeneration in the P120 retinas. Metabolomics of hydrophilic metabolites revealed that individual glycolytic products accumulated in the P45 Rtbdn(−/−) neural retinas along with the elevation of pentose phosphate pathway, while TCA cycle intermediates remained unchanged. This was confirmed by using (13)C-labeled flux measurements and immunoblotting, revealing that the key regulatory step of phosphoenolpyruvate to pyruvate was inhibited via down-regulation of the tetrameric pyruvate kinase M2 (PKM2). Separate metabolite assessments revealed that almost all intermediates of acylcarnitine fatty acid oxidation, ceramides, sphingomyelins, and multiple toxic metabolites were significantly elevated in the predegeneration Rtbdn(−/−) neural retina. Our data show that lack of RTBDN, and hence reduction in flavins, forced the neural retina into repurposing glucose for free-radical mitigation over ATP production. However, such sustained metabolic reprogramming resulted in an eventual metabolic collapse leading to neurodegeneration.

Published

2021

14. Retbindin: A riboflavin Binding Protein, Is Critical for Photoreceptor Homeostasis and Survival in Models of Retinal Degeneration

Author

Shannon M. Conley, Muayyad R. Al-Ubaidi, Muna I. Naash, Ayse M Genc, Mustafa S Makia, and Tirthankar Sinha

Subjects

0301 basic medicine, Retinal degeneration, Male, rho GTP-Binding Proteins, genetic structures, Peripherins, lcsh:Chemistry, chemistry.chemical_compound, Mice, 0302 clinical medicine, Homeostasis, lcsh:QH301-705.5, Spectroscopy, Mice, Knockout, biology, inherited retinal degeneration, Retinal Degeneration, General Medicine, Photoreceptor outer segment, Computer Science Applications, Cell biology, Rhodopsin, Female, Prph2, Photoreceptor Cells, Vertebrate, Flavoprotein, Catalysis, Article, Retina, Riboflavin binding, Inorganic Chemistry, 03 medical and health sciences, Retinitis pigmentosa, medicine, Animals, Physical and Theoretical Chemistry, riboflavin, Peripherin 2, Eye Proteins, Molecular Biology, flavoproteins, Organic Chemistry, Retinal, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, chemistry, lcsh:Biology (General), lcsh:QD1-999, rhodopsin, Mutation, 030221 ophthalmology & optometry, biology.protein, sense organs, metabolism

Abstract

The large number of inherited retinal disease genes (IRD), including the photopigment rhodopsin and the photoreceptor outer segment (OS) structural component peripherin 2 (PRPH2), has prompted interest in identifying common cellular mechanisms involved in degeneration. Although metabolic dysregulation has been shown to play an important role in the progression of the disease etiology, identifying a common regulator that can preserve the metabolic ecosystem is needed for future development of neuroprotective treatments. Here, we investigated whether retbindin (RTBDN), a rod-specific protein with riboflavin binding capability, and a regulator of riboflavin-derived cofactors flavin mononucleotide (FMN) and flavin adenine dinucleotide (FAD), is protective to the retina in different IRD models, one carrying the P23H mutation in rhodopsin (which causes retinitis pigmentosa) and one carrying the Y141C mutation in Prph2 (which causes a blended cone-rod dystrophy). RTBDN levels are significantly upregulated in both the rhodopsin (Rho)P23H/+ and Prph2Y141C/+ retinas. Rod and cone structural and functional degeneration worsened in models lacking RTBDN. In addition, removing Rtbdn worsened other phenotypes, such as fundus flecking. Retinal flavin levels were reduced in RhoP23H/+/Rtbdn&minus, /&minus, and Prph2Y141C/+/Rtbdn&minus, retinas. Overall, these findings suggest that RTBDN may play a protective role during retinal degenerations that occur at varying rates and due to varying disease mechanisms.

Published

2020

15. ROM1 contributes to phenotypic heterogeneity in PRPH2-associated retinal disease

Author

Muayyad R. Al-Ubaidi, Daniel Strayve, Mustafa S Makia, Muna I. Naash, Shannon M. Conley, Mashal Kakakhel, and Haarthi Sakthivel

Subjects

Retinal degeneration, Tetraspanins, Mutant, Peripherins, Biology, medicine.disease_cause, Retina, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Genetics, medicine, Animals, Humans, 030212 general & internal medicine, Allele, Peripherin 2, Eye Proteins, Molecular Biology, Genetics (clinical), Mice, Knockout, 0303 health sciences, Mutation, Genetic heterogeneity, 030305 genetics & heredity, Retinal Degeneration, Retinal, General Medicine, medicine.disease, Molecular biology, Disease Models, Animal, medicine.anatomical_structure, chemistry, Retinal Cone Photoreceptor Cells, sense organs, General Article

Abstract

Peripherin 2 (PRPH2) is a retina-specific tetraspanin protein essential for the formation of rod and cone photoreceptor outer segments (OS). Patients with mutations in PRPH2 exhibit severe retinal degeneration characterized by vast inter- and intra-familial phenotypic heterogeneity. To help understand contributors to this within-mutation disease variability, we asked whether the PRPH2 binding partner rod OS membrane protein 1 (ROM1) could serve as a phenotypic modifier. We utilized knockin and transgenic mouse models to evaluate the structural, functional and biochemical effects of eliminating one allele of Rom1 (Rom1+/−) in three different Prph2 models which mimic human disease: C213Y Prph2 (Prph2C/+), K153Del Prph2 (Prph2K/+) and R172W (Prph2R172W). Reducing Rom1 in the absence of Prph2 mutations (Rom1+/−) had no effect on retinal structure or function. However, the effects of reducing Rom1 in the presence of Prph2 mutations were highly variable. Prph2K/+/Rom1+/− mice had improved rod and cone function compared with Prph2K/+ as well as amelioration of K153Del-associated defects in PRPH2/ROM1 oligomerization. In contrast, Prph2R172W/Rom1+/− animals had worsened rod and cone function and exacerbated retinal degeneration compared with Prph2R172W animals. Removing one allele of Rom1 had no effect in Prph2C/+. Combined, our findings support a role for non-pathogenic ROM1 null variants in contributing to phenotypic variability in mutant PRPH2-associated retinal degeneration. Since the effects of Rom1 reduction are variable, our data suggest that this contribution is specific to the type of Prph2 mutation.

Published

2020

16. The Interplay between Peripherin 2 Complex Formation and Degenerative Retinal Diseases

Author

Muayyad R. Al-Ubaidi, Muna I. Naash, Mustafa S Makia, Lars Tebbe, and Mashal Kakakhel

Subjects

0301 basic medicine, Retinal degeneration, retina, Peripherins, Review, Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tetraspanin, medicine, Morphogenesis, Animals, Humans, Peripherin 2, lcsh:QH301-705.5, Retina, Retinal pigment epithelium, Retinal Degeneration, Retinal, General Medicine, Genetic Therapy, medicine.disease, Phenotype, photoreceptor, Cell biology, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, tetraspanin, chemistry, Membrane protein, lcsh:Biology (General), Mutation, 030221 ophthalmology & optometry, peripherin 2, sense organs

Abstract

Peripherin 2 (Prph2) is a photoreceptor-specific tetraspanin protein present in the outer segment (OS) rims of rod and cone photoreceptors. It shares many common features with other tetraspanins, including a large intradiscal loop which contains several cysteines. This loop enables Prph2 to associate with itself to form homo-oligomers or with its homologue, rod outer segment membrane protein 1 (Rom1) to form hetero-tetramers and hetero-octamers. Mutations in PRPH2 cause a multitude of retinal diseases including autosomal dominant retinitis pigmentosa (RP) or cone dominant macular dystrophies. The importance of Prph2 for photoreceptor development, maintenance and function is underscored by the fact that its absence results in a failure to initialize OS formation in rods and formation of severely disorganized OS membranous structures in cones. Although the exact role of Rom1 has not been well studied, it has been concluded that it is not necessary for disc morphogenesis but is required for fine tuning OS disc size and structure. Pathogenic mutations in PRPH2 often result in complex and multifactorial phenotypes, involving not just photoreceptors, as has historically been reasoned, but also secondary effects on the retinal pigment epithelium (RPE) and retinal/choroidal vasculature. The ability of Prph2 to form complexes was identified as a key requirement for the development and maintenance of OS structure and function. Studies using mouse models of pathogenic Prph2 mutations established a connection between changes in complex formation and disease phenotypes. Although progress has been made in the development of therapeutic approaches for retinal diseases in general, the highly complex interplay of functions mediated by Prph2 and the precise regulation of these complexes made it difficult, thus far, to develop a suitable Prph2-specific therapy. Here we describe the latest results obtained in Prph2-associated research and how mouse models provided new insights into the pathogenesis of its related diseases. Furthermore, we give an overview on the current status of the development of therapeutic solutions.

Published

2020

17. Novel molecular mechanisms for Prph2-associated pattern dystrophy

Author

Muayyad R. Al-Ubaidi, Dibyendu Chakraborty, Mustafa S Makia, Daniel Strayve, Shannon M. Conley, Muna I. Naash, and Mashal Kakahel

Subjects

0301 basic medicine, Tetraspanins, Mutant, Mutation, Missense, Peripherins, Mice, Transgenic, medicine.disease_cause, Biochemistry, Article, 03 medical and health sciences, Macular Degeneration, Mice, 0302 clinical medicine, Mutant protein, Retinal Rod Photoreceptor Cells, Retinitis pigmentosa, Genetics, medicine, Animals, Humans, Peripherin 2, Eye Proteins, Molecular Biology, Mutation, Chemistry, medicine.disease, Cell biology, 030104 developmental biology, Membrane protein, Amino Acid Substitution, Retinal Cone Photoreceptor Cells, Protein folding, sense organs, Protein Multimerization, 030217 neurology & neurosurgery, Retinitis Pigmentosa, Biotechnology, Cysteine

Abstract

Mutations in peripherin 2 (PRPH2) have been associated with retinitis pigmentosa (RP) and macular/pattern dystrophies, but the origin of this phenotypic variability is unclear. The majority of Prph2 mutations are located in the large intradiscal loop (D2), a region that contains seven cysteines involved in intra- and intermolecular disulfide bonding and protein folding. A mutation at cysteine 213, which is engaged in an intramolecular disulfide bond, leads to butterfly-shaped pattern dystrophy in humans, in sharp contrast to mutations in the adjacent cysteine at position 214 which result in RP. To help understand this unexpected phenotypic variability, we generated a knockin mouse line carrying the C213Y disease mutation. The mutant Prph2 protein lost the ability to oligomerize with rod outer segment membrane protein 1 (Rom1), but retained the ability to form homotetramers. C213Y heterozygotes had significantly decreased overall Prph2 levels as well as decreased rod and cone function. Critically, supplementation with extra wild-type Prph2 protein elicited improvements in Prph2 protein levels and rod outer segment structure, but not functional rescue in rods or cones. These findings suggest that not all interruptions of D2 loop intramolecular disulfide bonding lead to haploinsufficiency-related RP, but rather that more subtle changes can lead to mutant proteins stable enough to exert gain-of-function defects in rods and cones. This outcome highlights the difficulty in targeting Prph2-associated gain-of-function disease and suggests that elimination of the mutant protein will be a pre-requisite for any curative therapeutic strategy.

Published

2019

18. Elimination of a Retinal Riboflavin Binding Protein Exacerbates Degeneration in a Model of Cone-Rod Dystrophy

Author

Mustafa S Makia, Muna I. Naash, Tirthankar Sinha, Shannon M. Conley, Muayyad R. Al-Ubaidi, and Ayse M Genc

Subjects

Male, 0301 basic medicine, Retinal degeneration, peripherin/RDS, mouse model, Mice, Transgenic, Riboflavin, Flavin group, Retina, Mice, 03 medical and health sciences, chemistry.chemical_compound, Adenosine Triphosphate, 0302 clinical medicine, Microscopy, Electron, Transmission, Retinitis pigmentosa, Electroretinography, medicine, Animals, Fluorescein Angiography, Eye Proteins, Chromatography, High Pressure Liquid, Mice, Knockout, medicine.diagnostic_test, Chemistry, Biochemistry and Molecular Biology, Membrane Transport Proteins, Dystrophy, Retinal, flavin, medicine.disease, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, retinal diseases, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, retinal degeneration, peripherin 2, Female, sense organs, Cone-Rod Dystrophies, 030217 neurology & neurosurgery

Abstract

Purpose Riboflavin and its cofactors are essential for cellular energy generation, responses to oxidative stress, and overall homeostasis. Retbindin is a novel retina-specific riboflavin binding protein essential for the maintenance of retinal flavin levels, but its function remains poorly understood. To further elucidate the function of retbindin in retinal health and disease, we evaluated its role in retinal degeneration in a cone-rod dystrophy model associated with the R172W mutation in the photoreceptor tetraspanin Prph2. Methods We performed structural, functional, and biochemical characterization of R172W-Prph2 mice with and without retbindin (Rtbdn-/-/Prph2R172W). Results Retbindin is significantly upregulated during degeneration in the R172W model, suggesting that retbindin plays a protective role in retinal degenerative diseases. This hypothesis was supported by our findings that R172W mice lacking retbindin (Rtbdn-/-/Prph2R172W) exhibit functional and structural defects in rods and cones that are significantly worse than in controls. Retinal flavin levels were also altered in the Rtbdn-/-/Prph2R172W retina. However, in contrast to the Rtbdn-/- retina which has reduced flavin levels compared to wild-type, Rtbdn-/-/Prph2R172W retinas exhibited elevated levels of riboflavin and the flavin cofactor FMN. Conclusions These results indicate that retbindin plays a protective role during retinal degeneration, but that its function is more complex than previously thought, and suggest a possible role for retbindin in protecting the retina from phototoxicity associated with unbound flavins. This study highlights the essential role of precisely regulated homeostatic mechanisms in photoreceptors, and shows that disruption of this metabolic balance can contribute to the degenerative process associated with other cellular defects.

Published

2020

19. Flavin homeostasis in the mouse retina during aging and degeneration

Author

Mustafa S Makia, Tirthankar Sinha, Muna I. Naash, Jianhai Du, and Muayyad R. Al-Ubaidi

Subjects

0301 basic medicine, Retinal degeneration, Aging, animal structures, Light, Dinitrocresols, Flavin Mononucleotide, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Flavin mononucleotide, Cellular homeostasis, Riboflavin, Retinal Pigment Epithelium, Biochemistry, Retina, Article, 03 medical and health sciences, chemistry.chemical_compound, medicine, Animals, Homeostasis, heterocyclic compounds, Molecular Biology, Chromatography, High Pressure Liquid, Flavin adenine dinucleotide, Nutrition and Dietetics, Retinal pigment epithelium, Retinal Degeneration, Retinal, Fasting, medicine.disease, eye diseases, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, chemistry, Flavin-Adenine Dinucleotide, sense organs

Abstract

Involvement of flavin adenine dinucleotide (FAD) and flavin mononucleotide (FMN) in cellular homeostasis has been well established for tissues other than the retina. Here, we present an optimized method to effectively extract and quantify FAD and FMN from a single neural retina and its corresponding retinal pigment epithelium (RPE). Optimizations led to detection efficiency of 0.1 pmol for FAD and FMN while 0.01 pmol for riboflavin. Interestingly, levels of FAD and FMN in the RPE were found to be 1.7- and 12.5-fold higher than their levels in the retina, respectively. Both FAD and FMN levels in the RPE and retina gradually decline with age and preceded the age-dependent drop in the functional competence of the retina as measured by electroretinography. Further, quantifications of retinal levels of FAD and FMN in different mouse models of retinal degeneration revealed differential metabolic requirements of these two factors in relation to the rate and degree of photoreceptor degeneration. We also found twofold reductions in retinal levels of FAD and FMN in two mouse models of diabetic retinopathy. Altogether, our results suggest that retinal levels of FAD and FMN can be used as potential markers to determine state of health of the retina in general and more specifically the photoreceptors.

Published

2018

20. The usherin mutation c.2299delG leads to its mislocalization and disrupts interactions with whirlin and VLGR1

Author

Lars Tebbe, Maggie L. Mwoyosvi, Ryan Crane, Mustafa S. Makia, Mashal Kakakhel, Dominic Cosgrove, Muayyad R. Al-Ubaidi, and Muna I. Naash

Subjects

Science

Abstract

The c.2299delG mutation in usherin causes loss of hearing and vision. Here, the authors show in a mouse model of this disease that the expression of mutant usherin leads to retinitis pigmentosa and structural defects in the photoreceptor cilium associated with mislocalization of VLGR1 and WHRN.

Published

2023