Your search keyword '"Polyol pathway"' showing total 1,749 results

1. Regulation of glucose metabolism: Effects on oocyte, preimplantation embryo, assisted reproductive technology and embryonic stem cell

Author

Xiong, Yu-Ying, Zhu, Hai-Ying, Shi, Ruo-Jin, Wu, Yun-Feng, Fan, Yong, and Jin, Long

Published

2024

2. Quantification of total phenols in Coleus forskohlii and inhibition of aldose reductase by rosmarinic acid

Author

Kundur, Sunitha and Shyam, Perugu

Published

2024

3. Excessive gluconeogenesis causes the hepatic insulin resistance paradox and its sequelae

Author

Onyango, Arnold N.

Published

2022

4. New hope for the world cancer day.

Author

Melino, Gerry, Bischof, Julia, Chen, Wen-Lian, Jia, Wei, Juhl, Harmut, Kopeina, Gelina S, Mauriello, Alessandro, Novelli, Flavia, Scimeca, Manuel, Shi, Yufang, Pirozzi, Brunella Maria, Sica, Giuseppe, Zamaraev, Alexey V., and Zhivotovsky, Boris

Subjects

*MYELOID-derived suppressor cells, *CELL metabolism, *REGULATORY T cells, *PROGNOSIS, *CIRCULATING tumor DNA, *POLYOLS, *MOLECULAR clusters

Published

2025

5. Immortalized Schwann cell lines as useful tools for pathogenesis-based therapeutic approaches to diabetic peripheral neuropathy.

Author

Sango, Kazunori, Yako, Hideji, Niimi, Naoko, and Takaku, Shizuka

Subjects

SCHWANN cells, DIABETIC neuropathies, LABORATORY mice, CELL lines, GLYCOLYSIS

Abstract

Growing evidence suggests that hyperglycemia-related abnormalities in Schwann cells play a pivotal role in the development and progression of diabetic peripheral neuropathy (DPN). Several immortalized Schwann cell lines have been established in our laboratory and utilized for the study of DPN; IMS32 from normal ICR mice, 1970C3 from normal C57BL/6 mice, IWARS1 and IKARS1 from wild-type and aldose reductase-deficient C57BL/6 mice, and IFRS1 from normal Fischer 344 rats. These cell lines retain biological features of Schwann cells and display high proliferative activities that enable us to perform molecular and biochemical analyses. In addition, these cells have exhibited metabolic alterations under exposure to diabetes-associated conditions, such as hyperglycemia, dyslipidemia, glycative and oxidative stress load. Herein, recent studies with these cell lines regarding the pathogenic factors of DPN (augmentation of the polyol and other collateral glycolysis pathways, glycative and oxidative stress-induced cell injury, autophagic and proteostatic disturbances, etc.) and therapeutic strategies targeting these factors are introduced. [ABSTRACT FROM AUTHOR]

Published

2025

6. Nicotinamide and Nicotinoyl-Gamma-Aminobutyric Acid as Neuroprotective Agents Against Type 1 Diabetes-Induced Nervous System Impairments in Rats.

Author

Kuchmerovska, Tamara, Tykhonenko, Tetiana, Yanitska, Lesya, Savosko, Serhiy, and Pryvrotska, Iryna

Subjects

*PERIPHERAL nervous system, *MYELIN basic protein, *NIACIN, *SCIATIC nerve, *NERVOUS system, *NICOTINAMIDE, *SORBITOL

Abstract

Diabetes is a multifunctional chronic disease that affects both the central and/or peripheral nervous systems. This study assessed whether nicotinamide (NAm) or conjugate of nicotinic acid with gamma-aminobutyric acid (N-GABA) could be potential neuroprotective agents against type 1 diabetes (T1D)-induced nervous system impairments in rats. After six weeks of T1D, induced by streptozotocin, nonlinear male Wistar rats were treated for two weeks with NAm (100 mg/kg, i. p.) or N-GABA (55 mg/kg, i. p.). Expression levels of myelin basic protein (MBP) were analyzed by immunoblotting. Polyol pathway parameters of the sciatic nerves were assessed spectrophotometrically, and their structure was examined histologically. NAm had no effect on blood glucose or body weight in T1D, while N-GABA reduced glucose by 1.5-fold. N-GABA also increased MBP expression by 1.48-fold, enhancing neuronal myelination, while NAm showed no such effect. Activation of the polyol pathway was observed in the T1D sciatic nerves. Both compounds decreased sorbitol content and aldose reductase activity, thereby alleviating changes similar to primary degeneration in the sciatic nerves and preventing peripheral neuropathy development. These results demonstrate that NAm and, more notably, N-GABA may exert neuroprotective effects against T1D-induced nervous system impairments by increasing MBP expression levels, improving myelination processes in the brain, inhibiting the polyol pathway, and partially restoring morphometric parameters in the sciatic nerves. This suggests their potential therapeutic efficacy as promising agents for the prevention of T1D-induced nervous system alterations. [ABSTRACT FROM AUTHOR]

Published

2025

7. Inhibition of the polyol pathway by Ducrosia anethifolia extract: plausible implications for diabetic retinopathy treatment.

Author

Ahmad, Saheem, Ahmad, Mohammad Faizan Ali, Khan, Saif, Alouffi, Sultan, Khan, Mahvish, Khan, Mohd Wajid Ali, and Ansari, Irfan Ahmad

Subjects

ADVANCED glycation end-products, ALDOSE reductase, VISION disorders, DIABETIC retinopathy, ERYTHROCYTES, SORBITOL

Abstract

Introduction: Diabetic retinopathy is a significant microvascular disorder and the leading cause of vision impairment in working-age individuals. Hyperglycemia triggers retinal damage through mechanisms such as the polyol pathway and the accumulation of advanced glycation end products (AGEs). Inhibiting key enzymes in this pathway, aldose reductase (AR) and sorbitol dehydrogenase (SD), alongside preventing AGE formation, may offer therapeutic strategies for diabetic retinopathy and other vascular complications. This study investigates the ability of Ducrosia anethifolia , an Arabian plant, to inhibit AR and SD enzymes. Methods: Methanolic extracts of the plant were tested in enzyme assays and further analyzed using Lineweaver-Burk plots for kinetic insights. Additionally, the effects on AGE production and sorbitol accumulation in red blood cells were evaluated. Results: The methanolic extract showed strong inhibitory effects on AR (IC50: 69.41 ± 3.59 μg/mL) and SD (IC50: 31.11 ± 5.58 μg/mL), acting through a mixed-inhibition mechanism. It also significantly reduced sorbitol accumulation and AGE formation. Discussion: These findings suggest that the extract's inhibition of the polyol pathway enzymes is due to its phytochemical content. Further isolation and identification of these active compounds could provide valuable insights for developing future pharmaceutical treatments for diabetic retinopathy. [ABSTRACT FROM AUTHOR]

Published

2025

8. Beyond boundaries: pioneering discoveries in aldose reductase inhibition for diabetic neuropathy.

Author

A., Nagarajan, C., Vignesh, T., Ramasamy, M., Sasikala, and S., Mohan

Subjects

*ALDOSE reductase, *DIABETIC neuropathies, *VIRTUAL high-throughput screening (Drug development), *MOLECULAR dynamics, *PHARMACOPHORE

Abstract

Aldose reductase enzyme is involved in key step controlling the polyol pathway and acknowledged as a possible target for diabetic neuropathy. The anionic region of the active site comprising residues His110 and Tyr48 is involved in the detoxification mechanism that is considered important. This process involves eliminating toxicity through conversion of aldehydes such as methylglyoxal (MeG) and 3-deoxyglucosone. So far, no drug has been developed that could selectively inhibit reduction of glucose to sorbitol without affecting the detoxification mechanism. To comprehend the critical interactions of the known aldose reductase inhibitors and the enzyme, molecular docking was conducted in this study. Anionic region, specificity region and the active site are the three regions used separately for grid molecular docking studies to identify the possible inhibitors that selectively bind to specificity region. Among the docked compounds, quercetin was found to bind to specificity region, so we chose reported quercetin analogue and built a pharmacophore model. Subsequently, a collection of 82,000 natural substances from the IBS databank (InterBioScreen) was searched using a 6-point pharmacophore (AAARRR) that was created. After the initial search returned 2,394 hits, a hierarchical docking approach was used to identify an intriguing hit molecule (mol_7921), which is quite close to a flavonoid compound. Molecular dynamics simulation was used to confirm the hit molecule-aldose reductase complex’s structural stability. For its possible inhibitory effect, this molecule could be tested and used to treat diabetic neuropathy [ABSTRACT FROM AUTHOR]

Published

2024

9. Targeting the Polyol Pathway with Pithecellobium dulce for Diabetic Cataract Prevention.

Author

Bandaru, Nagaraju, Devi Jajula, Naga Venkata Indira, Mamidisetti, Yaso Deepika, Bonthu, Mohan Gandhi, Gayatri, Alluri Pavani, Swathi, Perla, Gambhire, Makarand Suresh, Nadhreddy, Dodda Thulase, and Tata, Prasanna Kumari

Subjects

AQUEOUS humor, ALDOSE reductase, BIOACTIVE compounds, CRYSTALLINE lens, VISION disorders, GOAT milk, ELLAGIC acid

Published

2024

10. High glucose combined with lipopolysaccharide stimulation inhibits cell proliferation and migration of human HaCaT keratinocytes by impacting redox homeostasis and activating the polyol pathway.

Author

Xie, Zhenhui, Zhou, Shufan, Tang, Songtao, Zhang, Qiu, and Liu, Lei

Abstract

Background: High glucose level and chronic inflammation are characteristic features of diabetic cutaneous wounds. Keratinocytes make up the epidermis and play an important role in skin repair. However, metabolomic changes of keratinocytes in chronic diabetic ulcers have not been fully studied. Methods and Results: This study used high levels of glucose combined with lipopolysaccharide to treat human HaCaT keratinocytes. Untargeted metabolomic combined with colorimetric assays were used to explore the changes of keratinocyte metabolites and related metabolic pathways caused by high glucose and lipopolysaccharide. Results demonstrated that high glucose combined with lipopolysaccharide treatment increased intracellular reactive oxygen species and impaired proliferation and migration of keratinocytes. Untargeted metabolomics analysis identified a total of 273 differential metabolites. Redox metabolism associated metabolites were largely altered. Reduced nicotinamide adenine dinucleotide, gamma-glutamylcysteine, superoxide dismutase activity and SOD2 gene expression were significantly upregulated while nicotinamide adenine dinucleotide, glutathione, glutathione peroxidase, several types of lysophosphatidylcholine, lysophosphatidylinositol, and GPR55 gene expression were downregulated. Alterations of glutathione and nicotinamide adenine dinucleotide were verified by colorimetric assays. For the first time, high glucose and LPS were observed to boost the levels of fructose, aldose reductase and sorbitol dehydrogenase of the polyol pathway in HaCaT cells. Further treatment of HaCaT with fructose leading to inhibition of cell proliferation and migration. Conclusions: Our data suggest high glucose combined with lipopolysaccharide significantly altered redox homeostasis associated metabolites and activate the polyol pathway in keratinocytes to impact cell proliferation and migration, providing new strategies for the treatment of chronic diabetic ulcers. [ABSTRACT FROM AUTHOR]

Published

2024

11. Tempol, a Superoxide Dismutase Mimetic, Inhibits Wallerian Degeneration Following Spinal Cord Injury by Preventing Glutathione Depletion and Aldose Reductase Activation.

Author

Zeman, Richard J., Brown, Abraham M., Wen, Xialing, Ouyang, Nengtai, and Etlinger, Joseph D.

Subjects

*NEURODEGENERATION, *ALDOSE reductase, *SPINAL cord injuries, *SPINAL cord, *SUPEROXIDE dismutase, *SORBITOL

Abstract

Spinal cord contusion injury results in Wallerian degeneration of spinal cord axonal tracts, which are necessary for locomotor function. Axonal swelling and loss of axonal density at the contusion site, characteristic of Wallerian degeneration, commence within hours of injury. Tempol, a superoxide dismutase mimetic, was previously shown to reduce the loss of spinal cord white matter and improve locomotor function in an experimental model of spinal cord contusion, suggesting that tempol treatment might inhibit Wallerian degeneration of spinal cord axons. Here, we report that tempol partially inhibits Wallerian degeneration, resulting in improved locomotor recovery. We previously reported that Wallerian degeneration is reduced by inhibitors of aldose reductase (AR), which converts glucose to sorbitol in the polyol pathway. We observed that tempol inhibited sorbitol production in the injured spinal cord to the same extent as the AR inhibitor, sorbinil. Tempol also prevented post-contusion upregulation of AR (AKR1B10) protein expression within degenerating axons, as previously observed for AR inhibitors. Additionally, we hypothesized that tempol inhibits axonal degeneration by preventing loss of the glutathione pool due to polyol pathway activity. Consistent with our hypothesis, tempol treatment resulted in greater glutathione content in the injured spinal cord, which was correlated with increased expression and activity of gamma glutamyl cysteine ligase (γGCL; EC 6.3.2.2), the rate-limiting enzyme for glutathione synthesis. Administration of the γGCL inhibitor buthionine sulfoximine abolished all observed effects of tempol administration. Together, these results support a pathological role for polyol pathway activation in glutathione depletion, resulting in Wallerian degeneration after spinal cord injury (SCI). Interestingly, methylprednisolone, oxandrolone, and clenbuterol, which are known to spare axonal tracts after SCI, were equally effective in inhibiting polyol pathway activation. These results suggest that prevention of AR activation is a common target of many disparate post-SCI interventions. [ABSTRACT FROM AUTHOR]

Published

2024

12. Polyphenol-Rich Extract of Apocynum venetum L. Leaves Protects Human Retinal Pigment Epithelial Cells against High Glucose-Induced Damage through Polyol Pathway and Autophagy.

Author

Peng, Jun, Abdulla, Rahima, Liu, Xiaoyan, He, Fei, Xin, Xuelei, and Aisa, Haji Akber

Abstract

Diabetic retinopathy (DR) is a specific microvascular problem of diabetes, which is mainly caused by hyperglycemia and may lead to rapid vision loss. Dietary polyphenols have been reported to decrease the risk of DR. Apocynum venetum L. leaves are rich in polyphenolic compounds and are popular worldwide for their health benefits as a national tea drink. Building on previous findings of antioxidant activity and aldose reductase inhibition of A. venetum, this study investigated the chemical composition of polyphenol-rich extract of A. venetum leaves (AVL) and its protective mechanism on ARPE-19 cells in hyperglycemia. Ninety-three compounds were identified from AVL by LC-MS/MS, including sixty-eight flavonoids, twenty-one organic acids, and four coumarins. AVL regulated the polyol pathway by decreasing the expression of aldose reductase and the content of sorbitol, enhancing the Na+K+-ATPase activity, and weakening intracellular oxidative stress effectively; it also could regulate the expression of autophagy-related proteins via the AMPK/mTOR/ULK1 signaling pathway to maintain intracellular homeostasis. AVL could restore the polyol pathway, inhibit oxidative stress, and maintain intracellular autophagy to protect cellular morphology and improve DR. The study reveals the phytochemical composition and protective mechanisms of AVL against DR, which could be developed as a functional food and/or candidate pharmaceutical, aiming for retina protection in diabetic retinopathy. [ABSTRACT FROM AUTHOR]

Published

2024

13. Immortalized Schwann cell lines as useful tools for pathogenesis-based therapeutic approaches to diabetic peripheral neuropathy

Author

Kazunori Sango, Hideji Yako, Naoko Niimi, and Shizuka Takaku

Subjects

immortalized Schwann cells, diabetic peripheral neuropathy, polyol pathway, glycation, oxidative stress, autophagic and proteostatic disturbances, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Growing evidence suggests that hyperglycemia-related abnormalities in Schwann cells play a pivotal role in the development and progression of diabetic peripheral neuropathy (DPN). Several immortalized Schwann cell lines have been established in our laboratory and utilized for the study of DPN; IMS32 from normal ICR mice, 1970C3 from normal C57BL/6 mice, IWARS1 and IKARS1 from wild-type and aldose reductase-deficient C57BL/6 mice, and IFRS1 from normal Fischer 344 rats. These cell lines retain biological features of Schwann cells and display high proliferative activities that enable us to perform molecular and biochemical analyses. In addition, these cells have exhibited metabolic alterations under exposure to diabetes-associated conditions, such as hyperglycemia, dyslipidemia, glycative and oxidative stress load. Herein, recent studies with these cell lines regarding the pathogenic factors of DPN (augmentation of the polyol and other collateral glycolysis pathways, glycative and oxidative stress-induced cell injury, autophagic and proteostatic disturbances, etc.) and therapeutic strategies targeting these factors are introduced.

Published

2025

14. Inhibition of the polyol pathway by Ducrosia anethifolia extract: plausible implications for diabetic retinopathy treatment

Author

Saheem Ahmad, Mohammad Faizan Ali Ahmad, Saif Khan, Sultan Alouffi, Mahvish Khan, Mohd Wajid Ali Khan, and Irfan Ahmad Ansari

Subjects

diabetic retinopathy, polyol pathway, advanced glycation end products (AGEs), aldose reductase (AR), sorbitol dehydrogenase (SD), Therapeutics. Pharmacology, RM1-950

Abstract

IntroductionDiabetic retinopathy is a significant microvascular disorder and the leading cause of vision impairment in working-age individuals. Hyperglycemia triggers retinal damage through mechanisms such as the polyol pathway and the accumulation of advanced glycation end products (AGEs). Inhibiting key enzymes in this pathway, aldose reductase (AR) and sorbitol dehydrogenase (SD), alongside preventing AGE formation, may offer therapeutic strategies for diabetic retinopathy and other vascular complications. This study investigates the ability of Ducrosia anethifolia, an Arabian plant, to inhibit AR and SD enzymes.MethodsMethanolic extracts of the plant were tested in enzyme assays and further analyzed using Lineweaver-Burk plots for kinetic insights. Additionally, the effects on AGE production and sorbitol accumulation in red blood cells were evaluated.ResultsThe methanolic extract showed strong inhibitory effects on AR (IC50: 69.41 ± 3.59 μg/mL) and SD (IC50: 31.11 ± 5.58 μg/mL), acting through a mixed-inhibition mechanism. It also significantly reduced sorbitol accumulation and AGE formation.DiscussionThese findings suggest that the extract’s inhibition of the polyol pathway enzymes is due to its phytochemical content. Further isolation and identification of these active compounds could provide valuable insights for developing future pharmaceutical treatments for diabetic retinopathy.

Published

2024

15. The Synergistic Effects of Polyol Pathway-Induced Oxidative and Osmotic Stress in the Aetiology of Diabetic Cataracts.

Author

Thorne, Courtney A., Grey, Angus C., Lim, Julie C., and Donaldson, Paul J.

Subjects

*LABORATORY rats, *CRYSTALLINE lens, *OXIDATIVE stress, *GLUCOSE metabolism, *PHYSIOLOGICAL adaptation

Abstract

Cataracts are the world's leading cause of blindness, and diabetes is the second leading risk factor for cataracts after old age. Despite this, no preventative treatment exists for cataracts. The altered metabolism of excess glucose during hyperglycaemia is known to be the underlying cause of diabetic cataractogenesis, resulting in localised disruptions to fibre cell morphology and cell swelling in the outer cortex of the lens. In rat models of diabetic cataracts, this damage has been shown to result from osmotic stress and oxidative stress due to the accumulation of intracellular sorbitol, the depletion of NADPH which is used to regenerate glutathione, and the generation of fructose metabolites via the polyol pathway. However, differences in lens physiology and the metabolism of glucose in the lenses of different species have prevented the translation of successful treatments in animal models into effective treatments in humans. Here, we review the stresses that arise from hyperglycaemic glucose metabolism and link these to the regionally distinct metabolic and physiological adaptations in the lens that are vulnerable to these stressors, highlighting the evidence that chronic oxidative stress together with osmotic stress underlies the aetiology of human diabetic cortical cataracts. With this information, we also highlight fundamental gaps in the knowledge that could help to inform new avenues of research if effective anti-diabetic cataract therapies are to be developed in the future. [ABSTRACT FROM AUTHOR]

Published

2024

16. Recent Advances in Biomolecular Patho-Mechanistic Pathways behind the Development and Progression of Diabetic Neuropathy.

Author

Ratan, Yashumati, Rajput, Aishwarya, Pareek, Ashutosh, Pareek, Aaushi, Kaur, Ranjeet, Sonia, Sonia, Kumar, Rahul, and Singh, Gurjit

Subjects

SATELLITE cells, SCHWANN cells, DIABETIC neuropathies, NEUROGLIA, NEURALGIA, ENDOTHELIUM diseases

Abstract

Diabetic neuropathy (DN) is a neurodegenerative disorder that is primarily characterized by distal sensory loss, reduced mobility, and foot ulcers that may potentially lead to amputation. The multifaceted etiology of DN is linked to a range of inflammatory, vascular, metabolic, and other neurodegenerative factors. Chronic inflammation, endothelial dysfunction, and oxidative stress are the three basic biological changes that contribute to the development of DN. Although our understanding of the intricacies of DN has advanced significantly over the past decade, the distinctive mechanisms underlying the condition are still poorly understood, which may be the reason behind the lack of an effective treatment and cure for DN. The present study delivers a comprehensive understanding and highlights the potential role of the several pathways and molecular mechanisms underlying the etiopathogenesis of DN. Moreover, Schwann cells and satellite glial cells, as integral factors in the pathogenesis of DN, have been enlightened. This work will motivate allied research disciplines to gain a better understanding and analysis of the current state of the biomolecular mechanisms behind the pathogenesis of DN, which will be essential to effectively address every facet of DN, from prevention to treatment. [ABSTRACT FROM AUTHOR]

Published

2024

17. Inhibitory Impact of Quercetin Nanoparticles on Polyol Pathway in Hyperthyroidism Rats.

Author

El-Aal, Yasmin Ali Abd, Tousson, Ehab, El-Dawy, Khalifa, Mohamed, Tarek M., and Abosharaf, Hamed A.

Abstract

The polyol pathway is a primary mechanism for the formation of sorbitol, and its accumulation is a major factor in many diseases' complications. Importantly, there have previously been some indications that there is a relationship between polyol intermediates and thyroid hormones in hyperthyroidism state. Hence, this study aimed to shed light on the therapeutic impact of nano-quercetin (QT-NPs) on hyperthyroidism via inhibiting the polyol pathway. Besides control groups, hyperthyroidism was triggered in the rats by 100 μg/kg of l-thyroxin and further treated with quercetin (QT) and nano-quercetin (10 mg/kg body weight). Additionally, levels of thyroid hormones (T3 and T4), oxidative markers, and the antioxidant system were monitored. Besides histological investigation of thyroid gland, the level of aldose reductase was estimated by qPCR. The obtained findings indicated an elevation of T3 and T4 which indicated hyperthyroidism. This hyperthyroid state was accompanied by an elevation in oxidative stress and a decline in antioxidant status. Importantly, the expression level of aldose reductase was elevated, as was the level of sorbitol. The treatment with QT and QT-NPs potentially reduced the expression level of aldose reductase and the concentration of sorbitol, indicating the inhibition capability of QT and QT-NPs on the polyol pathway key enzyme. Furthermore, rat groups treated with QT and QT-NPs showed an elevation in the antioxidant system (GSH, GPx) with a notable decline in the oxidative stress marker MDA. Furthermore, histopathological examination of the thyroid tissue of hyperthyroidism group treated with QT-NPs confirms the potential effect of QT-NPs on the thyroid tissue. In conclusion, QT-NPs showed therapeutic superiority over QT in hyperthyroidism treatment through inhibition of aldose reductase, which is the key enzyme in the polyol pathway. [ABSTRACT FROM AUTHOR]

Published

2024

18. Aldose Reductase as a Key Target in the Prevention and Treatment of Diabetic Retinopathy: A Comprehensive Review.

Author

Dănilă, Alexandra-Ioana, Ghenciu, Laura Andreea, Stoicescu, Emil Robert, Bolintineanu, Sorin Lucian, Iacob, Roxana, Săndesc, Mihai-Alexandru, and Faur, Alexandra Corina

Subjects

DIABETIC retinopathy, ALDOSE reductase, VISION disorders, CILIARY body, HYPERTENSION risk factors, REDUCTASE inhibitors

Abstract

The escalating global prevalence of diabetes mellitus (DM) over the past two decades has led to a persistent high incidence of diabetic retinopathy (DR), necessitating screening for early symptoms and proper treatment. Effective management of DR aims to decrease vision impairment by controlling modifiable risk factors including hypertension, obesity, and dyslipidemia. Moreover, systemic medications and plant-based therapy show promise in advancing DR treatment. One of the key mechanisms related to DR pathogenesis is the polyol pathway, through which aldose reductase (AR) catalyzes the conversion of glucose to sorbitol within various tissues, including the retina, lens, ciliary body and iris. Elevated glucose levels activate AR, leading to osmotic stress, advanced glycation end-product formation, and oxidative damage. This further implies chronic inflammation, vascular permeability, and angiogenesis. Our comprehensive narrative review describes the therapeutic potential of aldose reductase inhibitors in treating DR, where both synthetic and natural inhibitors have been studied in recent decades. Our synthesis aims to guide future research and clinical interventions in DR management. [ABSTRACT FROM AUTHOR]

Published

2024

19. Metabolic Alterations in NADSYN1-Deficient Cells.

Author

Meijer, Nils W. F., Gerrits, Johan, Zwakenberg, Susan, Zwartkruis, Fried J. T., Verhoeven-Duif, Nanda M., and Jans, Judith J. M.

Subjects

NICOTINAMIDE, NIACIN, PENTOSE phosphate pathway, PHENOTYPIC plasticity, TRYPTOPHAN, METABOLITES

Abstract

NAD synthetase 1 (encoded by the gene NADSYN1) is a cytosolic enzyme that catalyzes the final step in the biosynthesis of nicotinamide adenine dinucleotide (NAD+) from tryptophan and nicotinic acid. NADSYN1 deficiency has recently been added to the spectrum of congenital NAD+ deficiency disorders. To gain insight into the metabolic consequences of NADSYN1 deficiency, the encoding gene was disrupted in A549 and HEK293T cells, and the metabolome was profiled in the presence of different NAD+ precursors, including tryptophan, nicotinamide and nicotinic acid. We demonstrate that when precursors of the NAD+ salvage pathway in the form of nicotinamide become limiting, NADSYN1 deficiency results in a decline in intracellular NAD+ levels even in the presence of other potential NAD+ sources such as tryptophan and nicotinic acid. As a consequence, alterations in 122 and 69 metabolites are observed in NADSYN1-deficient A549 and HEK293T cells compared to the wild-type cell line (FC > 2 and p < 0.05). We thus show that NADSYN1 deficiency results in a metabolic phenotype characterized by alterations in glycolysis, the TCA cycle, the pentose phosphate pathway, and the polyol pathway. [ABSTRACT FROM AUTHOR]

Published

2023

20. Aldose Reductase (AR) Mediates and Perivascular Adipose Tissue (PVAT) Modulates Endothelial Dysfunction of Short-Term High-Fat Diet Feeding in Mice.

Author

Conklin, Daniel J., Haberzettl, Petra, MacKinlay, Kenneth G., Murphy, Daniel, Jin, Lexiao, Yuan, Fangping, Srivastava, Sanjay, and Bhatnagar, Aruni

Subjects

ALDOSE reductase, FAT, HIGH-fat diet, ADIPOSE tissues, ENDOTHELIUM diseases, DIABETIC neuropathies, MICE, CARDIOVASCULAR diseases

Abstract

Increased adiposity of both visceral and perivascular adipose tissue (PVAT) depots is associated with an increased risk of diabetes and cardiovascular disease (CVD). Under healthy conditions, PVAT modulates vascular tone via the release of PVAT-derived relaxing factors, including adiponectin and leptin. However, when PVAT expands with high-fat diet (HFD) feeding, it appears to contribute to the development of endothelial dysfunction (ED). Yet, the mechanisms by which PVAT alters vascular health are unclear. Aldose reductase (AR) catalyzes glucose reduction in the first step of the polyol pathway and has been long implicated in diabetic complications including neuropathy, retinopathy, nephropathy, and vascular diseases. To better understand the roles of both PVAT and AR in HFD-induced ED, we studied structural and functional changes in aortic PVAT induced by short-term HFD (60% kcal fat) feeding in wild type (WT) and aldose reductase-null (AR-null) mice. Although 4 weeks of HFD feeding significantly increased body fat and PVAT mass in both WT and AR-null mice, HFD feeding induced ED in the aortas of WT mice but not of AR-null mice. Moreover, HFD feeding augmented endothelial-dependent relaxation in aortas with intact PVAT only in WT and not in AR-null mice. These data indicate that AR mediates ED associated with short-term HFD feeding and that ED appears to provoke 'compensatory changes' in PVAT induced by HFD. As these data support that the ED of HFD feeding is AR-dependent, vascular-localized AR remains a potential target of temporally selective intervention. [ABSTRACT FROM AUTHOR]

Published

2023

21. Biochemical Mechanisms of Vascular Complications in Diabetes

Author

Flores, Margarita Díaz, del Carmen Cortés Ginez, María, Gutman, Luis Arturo Baiza, and Rodriguez-Saldana, Joel, editor

Published

2023

22. Recent Advances in Biomolecular Patho-Mechanistic Pathways behind the Development and Progression of Diabetic Neuropathy

Author

Yashumati Ratan, Aishwarya Rajput, Ashutosh Pareek, Aaushi Pareek, Ranjeet Kaur, Sonia Sonia, Rahul Kumar, and Gurjit Singh

Subjects

diabetic neuropathy, molecular mechanism, pathogenesis, polyol pathway, Schwann cells, neuropathic pain, Biology (General), QH301-705.5

Abstract

Diabetic neuropathy (DN) is a neurodegenerative disorder that is primarily characterized by distal sensory loss, reduced mobility, and foot ulcers that may potentially lead to amputation. The multifaceted etiology of DN is linked to a range of inflammatory, vascular, metabolic, and other neurodegenerative factors. Chronic inflammation, endothelial dysfunction, and oxidative stress are the three basic biological changes that contribute to the development of DN. Although our understanding of the intricacies of DN has advanced significantly over the past decade, the distinctive mechanisms underlying the condition are still poorly understood, which may be the reason behind the lack of an effective treatment and cure for DN. The present study delivers a comprehensive understanding and highlights the potential role of the several pathways and molecular mechanisms underlying the etiopathogenesis of DN. Moreover, Schwann cells and satellite glial cells, as integral factors in the pathogenesis of DN, have been enlightened. This work will motivate allied research disciplines to gain a better understanding and analysis of the current state of the biomolecular mechanisms behind the pathogenesis of DN, which will be essential to effectively address every facet of DN, from prevention to treatment.

Published

2024

23. 13C Metabolic Flux Analysis Indicates Endothelial Cells Attenuate Metabolic Perturbations by Modulating TCA Activity

Author

Moiz, Bilal, Garcia, Jonathan, Basehore, Sarah, Sun, Angela, Li, Andrew, Padmanabhan, Surya, Albus, Kaitlyn, Jang, Cholsoon, Sriram, Ganesh, and Clyne, Alisa Morss

Subjects

Biological Sciences, Industrial Biotechnology, Prevention, metabolic flux analysis, fluxomics, endothelial metabolism, cardiovascular disease, polyol pathway, pentose phosphate pathway, hexosamine biosynthetic pathway, aldose reductase inhibitors, Analytical Chemistry, Biochemistry and Cell Biology, Clinical Sciences, Biochemistry and cell biology, Medical biochemistry and metabolomics, Analytical chemistry

Abstract

Disrupted endothelial metabolism is linked to endothelial dysfunction and cardiovascular disease. Targeted metabolic inhibitors are potential therapeutics; however, their systemic impact on endothelial metabolism remains unknown. In this study, we combined stable isotope labeling with 13C metabolic flux analysis (13C MFA) to determine how targeted inhibition of the polyol (fidarestat), pentose phosphate (DHEA), and hexosamine biosynthetic (azaserine) pathways alters endothelial metabolism. Glucose, glutamine, and a four-carbon input to the malate shuttle were important carbon sources in the baseline human umbilical vein endothelial cell (HUVEC) 13C MFA model. We observed two to three times higher glutamine uptake in fidarestat and azaserine-treated cells. Fidarestat and DHEA-treated HUVEC showed decreased 13C enrichment of glycolytic and TCA metabolites and amino acids. Azaserine-treated HUVEC primarily showed 13C enrichment differences in UDP-GlcNAc. 13C MFA estimated decreased pentose phosphate pathway flux and increased TCA activity with reversed malate shuttle direction in fidarestat and DHEA-treated HUVEC. In contrast, 13C MFA estimated increases in both pentose phosphate pathway and TCA activity in azaserine-treated cells. These data show the potential importance of endothelial malate shuttle activity and suggest that inhibiting glycolytic side branch pathways can change the metabolic network, highlighting the need to study systemic metabolic therapeutic effects.

Published

2021

24. Endogenous Fructose Production and Metabolism Drive Metabolic Dysregulation and Liver Disease in Mice with Hereditary Fructose Intolerance.

Author

Andres-Hernando, Ana, Orlicky, David J., Kuwabara, Masanari, Cicerchi, Christina, Pedler, Michelle, Petrash, Mark J., Johnson, Richard J., Tolan, Dean R., and Lanaspa, Miguel A.

Abstract

Excessive intake of sugar, and particularly fructose, is closely associated with the development and progression of metabolic syndrome in humans and animal models. However, genetic disorders in fructose metabolism have very different consequences. While the deficiency of fructokinase, the first enzyme involved in fructose metabolism, is benign and somewhat desirable, missense mutations in the second enzyme, aldolase B, causes a very dramatic and sometimes lethal condition known as hereditary fructose intolerance (HFI). To date, there is no cure for HFI, and treatment is limited to avoiding fructose and sugar. Because of this, for subjects with HFI, glucose is their sole source of carbohydrates in the diet. However, clinical symptoms still occur, suggesting that either low amounts of fructose are still being consumed or, alternatively, fructose is being produced endogenously in the body. Here, we demonstrate that as a consequence of consuming high glycemic foods, the polyol pathway, a metabolic route in which fructose is produced from glucose, is activated, triggering a deleterious mechanism whereby glucose, sorbitol and alcohol induce severe liver disease and growth retardation in aldolase B knockout mice. We show that generically and pharmacologically blocking this pathway significantly improves metabolic dysfunction and thriving and increases the tolerance of aldolase B knockout mice to dietary triggers of endogenous fructose production. [ABSTRACT FROM AUTHOR]

Published

2023

25. Expression of aldose reductase in mouse endometrial epithelial cells and its role in sperm capacitation.

Author

Lei, Yi, Nie, Li, Long, Yun, Zhao, Dan, Liu, Min, Wang, Yi-cheng, Zhang, Xue-qin, Xu, Miao-miao, Liu, Huan, Zhang, Jin-hu, Yuan, Dong-zhi, and Yue, Li-min

Subjects

*ALDOSE reductase, *EPITHELIAL cells, *ENDOMETRIUM, *SPERMATOZOA, *GENITALIA, *SORBITOL, *SPERM motility, *HORMONE regulation

Abstract

The survival, motility and capacitation of sperm in the female reproductive tract are important prerequisites for fertilization. The uterus is the main location for sperm capacitation. One of the most important physiological functions of the endometrial epithelium is to create a suitable uterine environment under the regulation of ovarian hormones, to ensure sperm capacitation. The composition of uterine fluid directly affects sperm capacitation. Fructose is an important component of semen that supports sperm viability and motility. Aldose reductase, a rate-limiting enzyme in the polyol pathway, metabolizes sorbitol and fructose, thereby supplying cells with necessary energy for functional activities. Existing studies have reported the presence aldose reductase in the endometrium, leading us to hypothesize that its expression in endometrial epithelium might promote sperm capacitation by maintaining the uterine environment. Yet, the mechanism of regulation has not been clarified. In this study, we investigated the expression of aldose reductase in mouse endometrial epithelium and its potential role in sperm capacitation. We initially investigated the periodic characteristics of glucose, fructose and sorbitol in uterine fluid. We then studied the temporal and spatial characteristics of aldose reductase in the endometrial epithelium. Next, we examined the effect of aldose reductase on glucose, fructose and sorbitol in uterine fluid. Finally, we explored the effect of aldose reductase on sperm capacitation and fertilization. The results showed that glucose and fructose content in uterine fluid and the expression of aldose reductase fluctuated periodically during physiological periods. Inhibition of aldose reductase in the endometrial epithelium interfered with sperm capacitation and fertilization by reducing the fructose levels in the uterine fluid. To conclude, the aldose reductase-mediated polyol pathway in endometrial epithelial cells is essential to maintain an appropriate fructose environment in the uterine fluid for sperm capacitation and fertilization. [ABSTRACT FROM AUTHOR]

Published

2023

26. Insight into the Molecular Mechanism of Diabetic Kidney Disease and the Role of Metformin in Its Pathogenesis.

Author

Kleibert, Marcin, Zygmunciak, Przemysław, Łakomska, Klaudia, Mila, Klaudia, Zgliczyński, Wojciech, and Mrozikiewicz-Rakowska, Beata

Subjects

*DIABETIC nephropathies, *METFORMIN, *BLOOD sugar, *PATHOGENESIS, *ENDOTHELIAL cells

Abstract

Diabetic kidney disease (DKD) is one of the leading causes of death among patients diagnosed with diabetes mellitus. Despite the growing knowledge about the pathogenesis of DKD, we still do not have effective direct pharmacotherapy. Accurate blood sugar control is essential in slowing down DKD. It seems that metformin has a positive impact on kidneys and this effect is not only mediated by its hypoglycemic action, but also by direct molecular regulation of pathways involved in DKD. The molecular mechanism of DKD is complex and we can distinguish polyol, hexosamine, PKC, and AGE pathways which play key roles in the development and progression of this disease. Each of these pathways is overactivated in a hyperglycemic environment and it seems that most of them may be regulated by metformin. In this article, we summarize the knowledge about DKD pathogenesis and the potential mechanism of the nephroprotective effect of metformin. Additionally, we describe the impact of metformin on glomerular endothelial cells and podocytes, which are harmed in DKD. [ABSTRACT FROM AUTHOR]

Published

2023

27. Pre-hyperglycemia immune cell trafficking underlies subclinical diabetic cataractogenesis

Author

Ehsan Ranaei Pirmardan, Yuanlin Zhang, Aliaa Barakat, Marzieh Naseri, Christoph Russmann, and Ali Hafezi-Moghadam

Subjects

Diabetic complications, Polyol pathway, Paradigm shift, Insulin resistance, Medicine

Abstract

Abstract Background This work elucidates the first cellular and molecular causes of cataractogenesis. Current paradigm presupposes elevated blood glucose as a prerequisite in diabetic cataractogenesis. Novel evidence in our model of diabetic cataract challenges this notion and introduces immune cell migration to the lens and epithelial-mesenchymal transformation (EMT) of lens epithelial cells (LECs) as underlying causes. Methods Paucity of suitable animal models has hampered mechanistic studies of diabetic cataract, as most studies were traditionally carried out in acutely induced hyperglycemic animals. We introduced diabetic cataract in the Nile grass rat (NGR) that spontaneously develops type 2 diabetes (T2D) and showed its closeness to the human condition. Specialized stereo microscopy with dual bright-field illumination revealed novel hyperreflective dot-like microlesions in the inner cortical regions of the lens. To study immune cell migration to the lens, we developed a unique in situ microscopy technique of the inner eye globe in combination with immunohistochemistry. Results Contrary to the existing paradigm, in about half of the animals, the newly introduced hyper reflective dot-like microlesions preceded hyperglycemia. Even though the animals were normoglycemic, we found significant changes in their oral glucose tolerance test (OGTT), indicative of the prediabetic stage. The microlesions were accompanied with significant immune cell migration from the ciliary bodies to the lens, as revealed in our novel in situ microscopy technique. Immune cells adhered to the lens surface, some traversed the lens capsule, and colocalized with apoptotic nuclei of the lens epithelial cells (LECs). Extracellular degradations, amorphous material accumulations, and changes in E-cadherin expressions showed epithelial-mesenchymal transformation (EMT) in LECs. Subsequently, lens fiber disintegration and cataract progression extended into cortical, posterior, and anterior subcapsular cataracts. Conclusions Our results establish a novel role for immune cells in LEC transformation and death. The fact that cataract formation precedes hyperglycemia challenges the prevailing paradigm that glucose initiates or is necessary for initiation of the pathogenesis. Novel evidence shows that molecular and cellular complications of diabetes start during the prediabetic state. These results have foreseeable ramifications for early diagnosis, prevention and development of new treatment strategies in patients with diabetes.

Published

2023

28. Role of SERCA and AQP-5 in Diabetes Mellitus-Induced Xerostomia in Adult Male Albino Rat and The Potential Therapeutic Effect of Aldose Reductase Inhibitors: Histological Study.

Author

Farag, Eman Abas, Yousry, Marwa Mohamed, and Omar, Abeer Ibraheem

Subjects

ALDOSE reductase, XEROSTOMIA, TREATMENT effectiveness, ANIMAL models of diabetes, REDUCTASE inhibitors, BIOMOLECULES, AMYLASES

Abstract

Background: Saliva plays essential roles in different biological processes. Autonomic receptors stimulation is the main regulator of its secretion. Ca2+ acts as a 2nd messenger via increasing its cytoplasmic-level (i-Ca2+) &decreasing its endoplasmic reticulum-level (ER-Ca2+) with subsequent protein synthesis as a-amylase and water flow through aquaporin-5 channels (AQP-5). Sarco-ER Ca2+-ATPase (SERCA) pumps i-Ca2+ back to ER-Ca2+ maintaining low i-Ca2+ during rest and allowing its increase during salivary activation. Polyol-pathway overactivity with biological molecules glycation and oxidative-stress is the main mechanism of diabetic complications as xerostomia. As aldose-reductase (AR) is its key-enzyme, multiple ARinhibitors (ARIs) were newly explored to cure diabetic complications. Aim of work: Investigating SERCA &AQP-5 roles in diabetes-induced xerostomia molecular mechanism in adult male albino rats &the potential ARIs therapeutic effect. Materials &Methods: 32 rats were divided into 2 groups: control &experimental [received 55mg/kg streptozotocin to induce diabetes]. 18 hyperglycemic rats were divided into 3 subgroups: diabetic, diabetic/recovery &diabetic/ARIs [received daily oral 57 mg/kg Epalrestat for 4 weeks]. Serum glucose measurement, saliva collection &biochemical, histological, immunohistochemical [for active SERCA, AQP-5, inactive SERCA &caspase-3] and morphometric studies were done. Results: All serological, biochemical &histological manifestations of diabetes &xerostomia deteriorated from diabetic subgroup to diabetic/recovery subgroup. However, Epalrestat use evidently improved xerostomia manifestations but not diabetic manifestations. Conclusion: The main molecular mechanism of diabetesinduced xerostomia is polyol-pathway overactivity and consequent SERCA inactivation, i-Ca2+ overload, ER-stress, AQP-5 reduction, &a-amylase improper folding. Epalrestat, an ARI, ameliorates such xerostomia by blocking this pathway and preventing these changes with no effect on diabetes itself. [ABSTRACT FROM AUTHOR]

Published

2023

29. Aldose Reductase as a Key Target in the Prevention and Treatment of Diabetic Retinopathy: A Comprehensive Review

Author

Alexandra-Ioana Dănilă, Laura Andreea Ghenciu, Emil Robert Stoicescu, Sorin Lucian Bolintineanu, Roxana Iacob, Mihai-Alexandru Săndesc, and Alexandra Corina Faur

Subjects

diabetic retinopathy, aldose reductase, polyol pathway, aldose reductase inhibitor, Biology (General), QH301-705.5

Abstract

The escalating global prevalence of diabetes mellitus (DM) over the past two decades has led to a persistent high incidence of diabetic retinopathy (DR), necessitating screening for early symptoms and proper treatment. Effective management of DR aims to decrease vision impairment by controlling modifiable risk factors including hypertension, obesity, and dyslipidemia. Moreover, systemic medications and plant-based therapy show promise in advancing DR treatment. One of the key mechanisms related to DR pathogenesis is the polyol pathway, through which aldose reductase (AR) catalyzes the conversion of glucose to sorbitol within various tissues, including the retina, lens, ciliary body and iris. Elevated glucose levels activate AR, leading to osmotic stress, advanced glycation end-product formation, and oxidative damage. This further implies chronic inflammation, vascular permeability, and angiogenesis. Our comprehensive narrative review describes the therapeutic potential of aldose reductase inhibitors in treating DR, where both synthetic and natural inhibitors have been studied in recent decades. Our synthesis aims to guide future research and clinical interventions in DR management.

Published

2024

30. Osthole Prevents Heart Damage Induced by Diet-Induced Metabolic Syndrome: Role of Fructokinase (KHK).

Author

García-Arroyo, Fernando E., Gonzaga-Sánchez, Guillermo, Silva-Palacios, Alejandro, Roldán, Francisco Javier, Loredo-Mendoza, María L., Alvarez-Alvarez, Yamnia Quetzal, de los Santos Coyotl, Jesus A., Vélez Orozco, Kevin A., Tapia, Edilia, Osorio-Alonso, Horacio, Arellano-Buendía, Abraham S., Sánchez-Gloria, José L., Lanaspa, Miguel A., Johnson, Richard J., and Sánchez-Lozada, Laura Gabriela

Subjects

METABOLIC syndrome, HEART failure, CARDIAC hypertrophy, FRUCTOSE, WESTERN diet, LABORATORY rats, URIC acid

Abstract

There is increasing evidence that either ingested or produced fructose may have a role in metabolic syndrome. While not commonly considered a criterion for metabolic syndrome, cardiac hypertrophy is often associated with metabolic syndrome, and its presence carries increased cardiovascular risk. Recently it has been shown that fructose and fructokinase C (KHK) can be induced in cardiac tissue. Here we tested whether diet-induced metabolic syndrome causes heart disease associated with increased fructose content and metabolism and whether it can be prevented with a fructokinase inhibitor (osthole). Male Wistar rats were provided a control diet (C) or high fat/sugar diet for 30 days (MS), with half of the latter group receiving osthol (MS+OT, 40 mg/kg/d). The Western diet increased fructose, uric acid, and triglyceride concentrations in cardiac tissue associated with cardiac hypertrophy, local hypoxia, oxidative stress, and increased activity and expression of KHK in cardiac tissue. Osthole reversed these effects. We conclude that the cardiac changes in metabolic syndrome involve increased fructose content and its metabolism and that blocking fructokinase can provide cardiac benefit through the inhibition of KHK with modulation of hypoxia, oxidative stress, hypertrophy, and fibrosis. [ABSTRACT FROM AUTHOR]

Published

2023

31. A compressive review on novel molecular target of diabetic nephropathy

Author

Jaiswal, Astha, Semwal, Bhupesh Chandra, and Singh, Sonia

Published

2022

32. Assessing the risk factors for myocardial infarction in diet-induced prediabetes: myocardial tissue changes

Author

Nompumelelo Gumede, Phikelelani Ngubane, and Andile Khathi

Subjects

Polyol pathway, NADH oxidase, Oxidative stress, Myocardial injury, Antioxidant, Prediabetes, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Hyperglycaemia is known to result in oxidative stress tissue injury and dysfunction. Interestingly, studies have reported hepatic and renal oxidative stress injury during prediabetes; however, any injury to the myocardium during prediabetes has not been investigated. Hence this study aims to assess changes in the myocardial tissue in an HFHC diet-induced model of prediabetes. Methods Male Sprague Dawley rats were randomly grouped into non-prediabetes and prediabetes (n = 6 in each group) and consumed a standard rat chow or fed a high-fat-high-carbohydrate diet respectively for a 20-week prediabetes induction period. Post induction, prediabetes was confirmed using the ADA criteria. Aldose reductase, NADH oxidase 1, superoxide dismutase, glutathione peroxide, cardiac troponins were analysed in cardiac tissue homogenate using specific ELISA kits. Lipid peroxidation was estimated by determining the concentration of malondialdehyde in the heart tissue homogenate according to the previously described protocol. Myocardial tissue sections were stained with H&E stain and analysed using Leica microsystem. All data were expressed as means ± SEM. Statistical comparisons were performed with Graph Pad instat Software using the Student's two-sided t-test. Pearson correlation coefficient was calculated to assess the association. Value of p

Published

2022

33. Selectivity challenges for aldose reductase inhibitors: A review on comparative SAR and interaction studies.

Author

Kumari, Preety, Kohal, Rupali, Bhavana, Gupta, Ghanshyam Das, and Verma, Sant Kumar

Subjects

*ALDOSE reductase, *ALCOHOL dehydrogenase, *DIABETES complications, *STRUCTURE-activity relationships, *REDUCTASE inhibitors, *HYPERGLYCEMIA

Abstract

• ALR2, 1st enzyme of polyol pathway, overactives in diabetics, driving complications. • Strategies for managing diabetic complications via ALR2 targeting are exemplified. • Target-level selectivity challenges hindering ALR2 inhibition have been discussed. • Comparative SAR investigations for selectively targeting ALR2 inhibitors over ALR1. • In-depth interaction analysis to illustrate the target selective binding features. Chronic hyperglycemia initiates multiple pathways that contribute to developing complications in individuals with diabetes, ultimately leading to significant health problems and mortality. The extensive research elucidated the pathophysiological role of aldose reductase (ALR2) in the polyol pathway, which significantly contributes to these diabetic complications. ALR2, a rate-limiting enzyme in this pathway, becomes overactive in hyperglycemic conditions and plays a central role in developing diabetic complications. As a result, inhibiting ALR2 has emerged as a promising approach for managing these complications. Despite numerous ALR2 inhibitors, only epalrestat is currently marketed, mainly due to challenges related to their limited selectivity for ALR2 over aldehyde reductase (ALR1). This selectivity issue arises because ALR2 shares 65 % structural similarity with ALR1, leading to concerns about potential toxicity. This article provides a detailed overview of the advancements made in the last decade (2012–2023) in developing ALR2 and ALR1 inhibitors, addressing the selectivity challenges between ALR2 and ALR1 through comparative structure-activity relationship (SAR) analyses. It also explores the intricate interactions of potent ligands within the catalytic sites of both ALR2 and ALR1, offering innovative strategies for designing target-specific ALR2 inhibitors to minimize off-target toxicity. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

34. Advanced Glycation End-Products and Diabetic Neuropathy of the Retina.

Author

Oshitari, Toshiyuki

Subjects

*DIABETIC retinopathy, *ADVANCED glycation end-products, *DIABETIC neuropathies, *TYPE 1 diabetes, *TYPE 2 diabetes, *REACTIVE oxygen species, *RETINA

Abstract

Diabetic retinopathy is a tissue-specific neurovascular impairment of the retina in patients with both type 1 and type 2 diabetes. Several pathological factors are involved in the progressive impairment of the interdependence between cells that consist of the neurovascular units (NVUs). The advanced glycation end-products (AGEs) are one of the major pathological factors that cause the impairments of neurovascular coupling in diabetic retinopathy. Although the exact mechanisms for the toxicities of the AGEs in diabetic retinopathy have not been definitively determined, the AGE-receptor of the AGE (RAGE) axis, production of reactive oxygen species, inflammatory reactions, and the activation of the cell death pathways are associated with the impairment of the NVUs in diabetic retinopathy. More specifically, neuronal cell death is an irreversible change that is directly associated with vision reduction in diabetic patients. Thus, neuroprotective therapies must be established for diabetic retinopathy. The AGEs are one of the therapeutic targets to examine to ameliorate the pathological changes in the NVUs in diabetic retinopathy. This review focuses on the basic and pathological findings of AGE-induced neurovascular abnormalities and the potential therapeutic approaches, including the use of anti-glycated drugs to protect the AGE-induced impairments of the NVUs in diabetic retinopathy. [ABSTRACT FROM AUTHOR]

Published

2023

35. Rationale and design of the Aldose Reductase Inhibition for Stabilization of Exercise Capacity in Heart Failure Trial (ARISE-HF) in patients with high-risk diabetic cardiomyopathy.

Author

Januzzi, James L., Butler, Javed, Del Prato, Stefano, Ezekowitz, Justin A., Ibrahim, Nasrien E., Lam, Carolyn S.P., Lewis, Gregory D., Marwick, Thomas H., Rosenstock, Julio, Tang, W.H. Wilson, Zannad, Faiez, Lawson, Francesca, Perfetti, Riccardo, Urbinati, Alessia, Januzzi, James L Jr, Prato, Stefano Del, Lam, Carolyn Sp, and Tang, Wh Wilson

Abstract

Background: Diabetic cardiomyopathy (DbCM) is a specific form of heart muscle disease that may result in substantial morbidity and mortality in individuals with type 2 diabetes mellitus (T2DM). Hyperactivation of the polyol pathway is one of the primary mechanisms in the pathogenesis of diabetic complications, including development of DbCM. There is an unmet need for therapies targeting the underlying metabolic abnormalities that drive this form of Stage B heart failure (HF).Methods: Aldose reductase (AR) catalyzes the first and rate-limiting step in the polyol pathway, and AR inhibition has been shown to reduce diabetic complications, including DbCM in animal models and in patients with DbCM. Previous AR inhibitors (ARIs) were limited by poor specificity resulting in unacceptable tolerability and safety profile. AT-001 is a novel investigational highly specific ARI with higher binding affinity and greater selectivity than previously studied ARIs. ARISE-HF (NCT04083339) is an ongoing Phase 3 randomized, placebo-controlled, double blind, global clinical study to investigate the efficacy of AT-001 (1000 mg twice daily [BID] and 1500 mg BID) in 675 T2DM patients with DbCM at high risk of progression to overt HF. ARISE-HF assesses the ability of AT-001 to improve or prevent decline in exercise capacity as measured by functional capacity (changes in peak oxygen uptake [peak VO2]) over 15 (and possibly 27) months of treatment. Additional endpoints include percentage of patients progressing to overt HF, health status metrics, echocardiographic measurements, and changes in cardiacbiomarkers.Results: The ARISE-HF Trial is fully enrolled.Conclusions: This report describes the rationale and study design of ARISE-HF. [ABSTRACT FROM AUTHOR]

Published

2023

36. Pre-hyperglycemia immune cell trafficking underlies subclinical diabetic cataractogenesis.

Author

Ranaei Pirmardan, Ehsan, Zhang, Yuanlin, Barakat, Aliaa, Naseri, Marzieh, Russmann, Christoph, and Hafezi-Moghadam, Ali

Subjects

GLUCOSE tolerance tests, PREDIABETIC state, CRYSTALLINE lens, TYPE 2 diabetes, BLOOD sugar, CELL death

Abstract

Background: This work elucidates the first cellular and molecular causes of cataractogenesis. Current paradigm presupposes elevated blood glucose as a prerequisite in diabetic cataractogenesis. Novel evidence in our model of diabetic cataract challenges this notion and introduces immune cell migration to the lens and epithelial-mesenchymal transformation (EMT) of lens epithelial cells (LECs) as underlying causes. Methods: Paucity of suitable animal models has hampered mechanistic studies of diabetic cataract, as most studies were traditionally carried out in acutely induced hyperglycemic animals. We introduced diabetic cataract in the Nile grass rat (NGR) that spontaneously develops type 2 diabetes (T2D) and showed its closeness to the human condition. Specialized stereo microscopy with dual bright-field illumination revealed novel hyperreflective dot-like microlesions in the inner cortical regions of the lens. To study immune cell migration to the lens, we developed a unique in situ microscopy technique of the inner eye globe in combination with immunohistochemistry. Results: Contrary to the existing paradigm, in about half of the animals, the newly introduced hyper reflective dot-like microlesions preceded hyperglycemia. Even though the animals were normoglycemic, we found significant changes in their oral glucose tolerance test (OGTT), indicative of the prediabetic stage. The microlesions were accompanied with significant immune cell migration from the ciliary bodies to the lens, as revealed in our novel in situ microscopy technique. Immune cells adhered to the lens surface, some traversed the lens capsule, and colocalized with apoptotic nuclei of the lens epithelial cells (LECs). Extracellular degradations, amorphous material accumulations, and changes in E-cadherin expressions showed epithelial-mesenchymal transformation (EMT) in LECs. Subsequently, lens fiber disintegration and cataract progression extended into cortical, posterior, and anterior subcapsular cataracts. Conclusions: Our results establish a novel role for immune cells in LEC transformation and death. The fact that cataract formation precedes hyperglycemia challenges the prevailing paradigm that glucose initiates or is necessary for initiation of the pathogenesis. Novel evidence shows that molecular and cellular complications of diabetes start during the prediabetic state. These results have foreseeable ramifications for early diagnosis, prevention and development of new treatment strategies in patients with diabetes. [ABSTRACT FROM AUTHOR]

Published

2023

37. Insight into polyol pathway for diabetic wound care supported by applications of scaffolds.

Author

Ramachandran, Vadivelan, Mohanasundaram, Tharani, Gunasekaran, Monika, Karnakaran, Darshan, and Tiwari, Ruchi

Subjects

*DIABETIC foot, *WOUND care, *DIABETIC neuropathies, *PROTEIN kinase C, *SORBITOL, *NITRIC-oxide synthases

Abstract

Diabetes foot ulcer (DFU) affects around one-third of diabetic patients, which are mostly caused by peripheral neurovascular disease or peripheral neuropathy. Since diabetic foot ulcers are persistent and difficult to cure, the present study contains a literature review for a better understanding of the neuropathic and ischemic characteristics of diabetes, their control, prevention, and treatment. The researchers discovered that the inhibitors of sorbitol dehydrogenase, AR, Protein Kinase C (PKC) activation, activators of myo-inositol bisphosphatase, nitric oxide synthase and many other enzymes were found to play salient roles in the polyol pathway of diabetic neuropathy. It can be concluded that key elements of the polyol pathway play a vital role in the control, prevention, management, and treatment of diabetic foot ulcers. [ABSTRACT FROM AUTHOR]

Published

2023

38. N‐substituted phthalazine sulfonamide derivatives as non‐classical aldose reductase inhibitors.

Author

Türkeş, Cüneyt, Arslan, Mustafa, Demir, Yeliz, Çoçaj, Liridon, Nixha, Arleta Rifati, and Beydemir, Şükrü

Subjects

*ALDOSE reductase, *REDUCTASE inhibitors, *PHTHALAZINE, *SULFONAMIDES, *MOLECULAR docking, *BINDING sites

Abstract

Aldose reductase (AR, AKR1B1; EC 1.1.1.21) is an aldo‐keto reductase that has been widely investigated as an enzyme crucially involved in the pathogenesis of several chronic complications, including nephropathy, neuropathy, retinopathy, and cataracts associated with diabetes mellitus. Although sulfonamides have been reported to possess many other biological activities, in continuation of our interest in designing and discovering potent inhibitors of AR, herein, we have evaluated the AR inhibitory potential of N‐substituted phthalazine sulfonamide derivatives 5a‐l. The biological studies revealed that all the derivatives show excellent activity against AR, with KI constants ranging from 67.73 to 495.20 nM. Among these agents, 4‐(6‐nitro‐1,4‐dioxo‐1,2,3,4‐tetrahydrophthalazine‐2‐carbonyl)benzenesulfonamide (5e) and 1,4‐dioxo‐3‐(4‐sulfamoylbenzoyl)‐1,2,3,4‐tetrahydrophthalazine‐6‐carboxylic acid (5f) showed prominent inhibitory activity with KI values of 67.73 and 148.20 nM, respectively, vs AR and were found to be more potent than epalrestat (KI = 852.50 nM), the only AR inhibitor currently used in the therapy. Moreover, molecular docking studies were also performed to rationalize binding site interactions of these sulfonamides (5a‐l) with the target enzyme AR. According to ADME‐Tox, predicts were also determined that these derivatives be ARIs displaying suitable drug‐like properties. The sulfonamides identified in this study may be used to develop lead therapeutic agents inhibiting diabetic complications. [ABSTRACT FROM AUTHOR]

Published

2022

39. Genotype and phenotype spectrum of Charcot-Marie-Tooth disease due to mutations in SORD.

Author

Cortese A, Dohrn MF, Curro R, Negri S, Lassuthova P, Pisciotta C, Tozza S, Al-Ajmi A, Feng C, Tomaselli PJ, Fernandez-Eulate G, Haddad S, Laurà M, Rossor AM, Vegezzi E, Facchini S, Sleigh JN, Rebelo A, Beijer D, Raposo J, Saporta M, Lauerova B, Pernice HF, Achenbach P, Schöne U, Alon T, Deschauer M, Cordts I, Obermaier CD, Winter N, Creigh PD, Sowden JE, Rehbein T, Magri S, Bertini A, Saveri P, Ripellino P, Huang J, Nadaj-Pakleza A, Ross A, Holt JKL, Brennan KM, Sukenik-Halevy R, Bizaoui V, Parman Y, Battaloglu E, Cakar A, Alrohaif H, Hammans S, Kumar KR, Kennerson ML, Kayserili H, Amado DA, Hahn K, Valentino P, Cavalcanti F, Gaetano C, Taroni F, Braathen GJ, Houlden H, Stojkovic T, Peric S, Bolino A, Previtali SC, Lee YC, Başak AN, Hamed SA, Rojas-Garcia R, Claeys KG, Marques W, Sevilla T, Schlotter-Weigel B, Manganelli F, Zhang R, Herrmann DN, Scherer SS, Seeman P, Pareyson D, Reilly MM, Shy ME, and Züchner S

Abstract

Biallelic loss-of-function mutations in the sorbitol dehydrogenase (SORD) gene cause the most common recessive type of Charcot-Marie-Tooth disease (CMT), CMT-SORD. However, the full genotype-phenotype spectrum and progression of the disease remain to be defined. Notably, a multicenter phase 2/3 study to test the efficacy of govorestat (NCT05397665), a new aldose reductase inhibitor, is currently ongoing. Diagnosing CMT-SORD will become imperative when disease-modifying therapies become available. In this cross-sectional multicentre study, we identified 144 patients from 126 families, including 99 males (69%) and 45 females (31%). Patients represented multiple ancestries, including European, Hispanic, Chinese, Near Eastern, and Northern African. We confirmed c.757delG (p.Ala253GlnfsTer27) as the most common pathogenic allele, followed by c.458C>A (p.Ala153Asp), while other variants were identified mostly in single cases. The average sorbitol level in CMT-SORD patients was significantly higher compared to controls and heterozygous carriers, independently from serum storage duration, sex, or variant type. Two-thirds of cases were diagnosed with CMT2 while one-third had distal hereditary motor neuropathy (dHMN). Disease onset was usually in the second decade of life. Although foot dorsiflexion was the most affected muscle group, dorsal and plantar flexion had a similar degree of weakness in most cases (difference of Medical Research Council score ≤ 1). One fourth of patients used ankle foot orthoses, usually in their 30s, but most patients maintained independent ambulation later in life. Nerve conduction studies (NCS) were suggestive of a motor predominant axonal neuropathy, with reduced conduction velocities in the intermediate range in one fourth of the cases. Sensory conductions in the upper limbs appeared more frequently affected than in the lower limbs. Foot dorsiflexion and plantar flexion decreased significantly with age. Male sex was significantly associated with the severity of distal lower limb weakness (plantar flexion) and a larger change over time (dorsiflexion). In conclusion, CMT-SORD is a frequent recessive form of axonal, motor predominant CMT, with prominent foot dorsiflexion and plantar flexion involvement. Fasting serum sorbitol is a reliable biomarker of the condition that can be utilized for pathogenicity assessment of identified rare SORD variants., (© The Author(s) 2025. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2025

40. Perioperative cerebrospinal fluid sorbitol and fructose concentrations in patients undergoing thoracic aortic surgery.

Author

van Zuylen, Mark L., Peters van Ton, Annemieke M., Duindam, Harmke B., Scholten, Erik, van Dongen, Eric P.A., ten Hoope, Werner, Plummer, Mark P., DeVries, J. Hans, Preckel, Benedikt, Scheffer, Gert-Jan, Abdo, Wilson F., and Hermanides, Jeroen

Subjects

*CEREBROSPINAL fluid, *SORBITOL, *FRUCTOSE, *THORACIC surgery, *CEREBROSPINAL fluid shunts, *GLUCOSE

Published

2022

41. Role of the Polyol Pathway in Locomotor Recovery and Wallerian Degeneration after Spinal Cord Contusion Injury

Author

Richard J. Zeman, Xialing Wen, Nengtai Ouyang, Abraham M. Brown, and Joseph D. Etlinger

Subjects

glucose uptake, glucotoxicity, hyperglucosis, locomotor function, polyol pathway, spinal cord injury, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Spinal cord contusion injury leads to Wallerian degeneration of axonal tracts, resulting in irreversible paralysis. Contusion injury causes perfusion loss by thrombosis and vasospasm, resulting in spinal cord ischemia. In several tissues, including heart and brain, ischemia activates polyol pathway enzymes?aldose reductase (AR) and sorbitol dehydrogenase (SDH)?that convert glucose to sorbitol and fructose in reactions, causing oxidative stress and tissue loss. We sought to determine whether activation of this pathway, which has been termed glucotoxicity, contributes to tissue loss after spinal cord contusion injury. We tested individual treatments with AR inhibitors (sorbinil or ARI-809), SDH inhibitor (CP-470711), superoxide dismutase mimetic (tempol), or combined sorbinil and tempol. Each treatment significantly increased locomotor recovery and reduced loss of spinal cord tissue in a standard model of spinal cord contusion in rats. Tissue levels of sorbitol and axonal AR (AKR1B10) expression were increased after contusion injury, consistent with activation of the polyol pathway. Sorbinil treatment inhibited the above changes and also decreased axonal swelling and loss, characteristic of Wallerian degeneration. Treatment with tempol induced recovery of locomotor function that was similar in magnitude, but non-additive to sorbinil, suggesting a shared mechanism of action by reactive oxygen species (ROS). Exogenous induction of hyperglycemia further increased injury-induced axonal swelling, consistent with glucotoxicity. Unexpectedly, contusion increased spinal cord levels of glucose, the primary polyol pathway substrate. These results support roles for spinal glucose elevation and tissue glucotoxicity by the polyol pathway after spinal cord contusion injury that results in ROS-mediated axonal degeneration.

Published

2021

42. Assessing the risk factors for myocardial infarction in diet-induced prediabetes: myocardial tissue changes.

Author

Gumede, Nompumelelo, Ngubane, Phikelelani, and Khathi, Andile

Abstract

Background: Hyperglycaemia is known to result in oxidative stress tissue injury and dysfunction. Interestingly, studies have reported hepatic and renal oxidative stress injury during prediabetes; however, any injury to the myocardium during prediabetes has not been investigated. Hence this study aims to assess changes in the myocardial tissue in an HFHC diet-induced model of prediabetes.Methods: Male Sprague Dawley rats were randomly grouped into non-prediabetes and prediabetes (n = 6 in each group) and consumed a standard rat chow or fed a high-fat-high-carbohydrate diet respectively for a 20-week prediabetes induction period. Post induction, prediabetes was confirmed using the ADA criteria. Aldose reductase, NADH oxidase 1, superoxide dismutase, glutathione peroxide, cardiac troponins were analysed in cardiac tissue homogenate using specific ELISA kits. Lipid peroxidation was estimated by determining the concentration of malondialdehyde in the heart tissue homogenate according to the previously described protocol. Myocardial tissue sections were stained with H&E stain and analysed using Leica microsystem. All data were expressed as means ± SEM. Statistical comparisons were performed with Graph Pad instat Software using the Student's two-sided t-test. Pearson correlation coefficient was calculated to assess the association. Value of p < 0.05 was considered statistically significant.Results: The prediabetes group showed a markedly high oxidative stress as indicated by significantly increased NADH oxidase 1 and malondialdehyde while superoxide dismutase and glutathione peroxide were decreased compared to non-prediabetes group. There was no statistical difference between cardiac troponin I and T in the non-prediabetes and prediabetes groups. Cardiac troponins had a weak positive association with glycated haemoglobin.Conclusion: The findings of this study demonstrate that prediabetes is associated with myocardial injury through oxidative stress. Future studies are to investigate cardiac contractile function and include more cardiac biomarkers. [ABSTRACT FROM AUTHOR]

Published

2022

43. Elevated cerebrospinal fluid glucose levels and diabetes mellitus are associated with activation of the neurotoxic polyol pathway.

Author

Tigchelaar, Celien, van Zuylen, Mark L., Hulst, Abraham H., Preckel, Benedikt, van Beek, André P., Kema, Ido P., Hermanides, Jeroen, and Absalom, Anthony R.

Abstract

Aims/hypothesis: During hyperglycaemia, some glucose bypasses glycolysis and is metabolised via the potentially neurotoxic polyol pathway, in which glucose is metabolised to sorbitol and fructose. Increased polyol concentrations have been demonstrated in the cerebrospinal fluid (CSF) of neurological patients with and without diabetes mellitus. However, polyol levels in patients without evident neurological abnormalities have not been investigated so far. The aim of this study was to determine CSF polyol concentrations in patients without major neurological disease with normal or elevated CSF glucose concentrations. Methods: This observational cohort study used CSF and plasma analyses, as well as clinical data, from 30 participants of the Anaesthetic Biobank of Cerebrospinal Fluid study. Biomaterial was collected from adult patients scheduled for elective surgery under spinal anaesthesia. CSF polyol concentrations were measured by GC/flame ionisation detector in ten patients with normal CSF glucose levels (group 1), ten patients with elevated CSF glucose levels (group 2) and ten patients with elevated CSF glucose levels and type 2 diabetes (group 3). We compared the concentrations of plasma glucose, CSF glucose, sorbitol and fructose, and CSF polyol/glucose ratios between the three groups, and determined the correlation between plasma glucose levels and CSF glucose, sorbitol and fructose levels. Results: Groups 2 and 3 had significantly higher CSF fructose levels compared with group 1 (p=0.036 and p<0.001, respectively). Group 3 showed significant differences compared with groups 1 and 2 for CSF sorbitol (p<0.001 and 0.036, respectively). Moreover, patients with diabetes had a significantly higher CSF sorbitol/glucose ratio compared with patients without diabetes. There was a strong positive correlation between plasma glucose and CSF glucose, sorbitol and fructose. Finally, age, sex, CSF/plasma albumin ratio and preoperative cognitive function scores were significantly correlated with plasma glucose and CSF glucose, sorbitol and fructose levels. Conclusions/interpretation: Hyperglycaemia causes a proportional increase in polyol concentrations in CSF of patients without major neurological disease. Furthermore, this study provides the first indication of upregulation of the cerebral polyol pathway in patients with diabetes without evident neurological abnormalities. [ABSTRACT FROM AUTHOR]

Published

2022

44. Systematic Investigations on the Metabolic and Transcriptomic Regulation of Lactate in the Human Colon Epithelial Cells.

Author

Huang, Chongyang, Xu, Huanzhou, Zhou, Xin, Liu, Maili, Li, Jing, and Liu, Chaoyang

Subjects

*METABOLIC regulation, *EPITHELIAL cells, *LACTATES, *LACTATION, *COLON (Anatomy)

Abstract

Lactate, primarily produced by the gut microbiota, performs as a necessary "information transmission carrier" between the gut and the microbiota. To investigate the role of lactate in the gut epithelium cell–microbiota interactions as a metabolic signal, we performed a combinatory, global, and unbiased analysis of metabolomic and transcriptional profiling in human colon epithelial cells (Caco-2), using a lactate treatment at the physiological concentration (8 mM). The data demonstrated that most of the genes in oxidative phosphorylation were significantly downregulated in the Caco-2 cells due to lactate treatment. Consistently, the levels of fumarate, adenosine triphosphate (ATP), and creatine significantly decreased, and these are the metabolic markers of OXPHOS inhibition by mitochondria dysfunction. The one-carbon metabolism was affected and the polyol pathway was activated at the levels of gene expression and metabolic alternation. In addition, lactate significantly upregulated the expressions of genes related to self-protection against apoptosis. In conclusion, lactate participates in gut–gut microbiota communications by remodeling the metabolomic and transcriptional signatures, especially for the regulation of mitochondrial function. This work contributes comprehensive information to disclose the molecular mechanisms of lactate-mediated functions in human colon epithelial cells that can help us understand how the microbiota communicates with the intestines through the signaling molecule, lactate. [ABSTRACT FROM AUTHOR]

Published

2022

45. Potential molecular mechanism of action of sodium-glucose co-transporter 2 inhibitors in the prevention and management of diabetic retinopathy.

Author

Zaini, Lia Meuthia, Kartasasmita, Arief S, Gondhowiardjo, Tjahjono D, Syukri, Maimun, and Lesmana, Ronny

Subjects

MOLECULAR biology, TREATMENT effectiveness, CELLULAR signal transduction, OXIDATIVE stress, DIABETIC retinopathy

Abstract

Sodium glucose co-transporter 2 (SGLT2) inhibitors are a new class of drugs for the treatment of type 2 diabetes mellitus (T2DM), which have cardio-renal protective activity. Some studies have also found that this drug may have an eye-protective effect, especially in preventing diabetic retinopathy (DR). A search was conducted on PubMed and Google Scholar for all articles published from January 2007 to May 2022. This paper provides a new insight into how new emerging diabetic therapy may be beneficial in the case of DR. SGLT2 inhibitors have been proven to delay DR progression. However, the drug mechanism in the pathophysiology of diabetic retinopathy has not yet been established. In clinical practice, using SGLT2 inhibitors is beneficial as it offers multiple advantages. They can control blood sugar levels while simultaneously suppressing the progression of DR and DME. There is potential that the use of other expensive and prolonged therapeutic modalities may no longer be necessary, reducing the burden of treatment for patients. [ABSTRACT FROM AUTHOR]

Published

2022

46. Silymarin from Milk Thistle Fruits Counteracts Selected Pathological Changes in the Lenses of Type 1 Diabetic Rats.

Author

Borymska, Weronika, Zych, Maria, Dudek, Sławomir, and Kaczmarczyk-Sedlak, Ilona

Abstract

Diabetes is a metabolic disease affecting many tissues and organs. The main etiological factor for diabetic complications is hyperglycemia and subsequent pathologies, such as oxidative stress. One of the organs susceptible to the development of diabetic complications is the eye with all of its elements, including the lens. The aim of this study was to evaluate the effect of silymarin, an extract obtained from milk thistle fruit husks, on the oxidative stress markers in the lenses of type 1 diabetic rats. The study was performed on male rats in which type 1 diabetes was induced with 60 mg/kg streptozotocin injection. Diabetic animals were treated via an intragastric tube with silymarin at 50 and 100 mg/kg doses for four weeks. Multiple oxidative stress and polyol pathway-related parameters were measured in the lenses, and auxiliary biochemical tests in the serum were conducted. Diabetes induced severe pathological changes both in the lenses and the serum, and silymarin counteracted several of them. Nevertheless, the qualitative analyses encompassing all tested parameters indicate that silymarin slightly improved the overall state of diabetic animals. Upon the obtained results, it can be concluded that silymarin reveals a faint positive effect on the lenses in type 1 diabetic rats. [ABSTRACT FROM AUTHOR]

Published

2022

47. Cytotoxicity and polyol pathway inhibitory activities of chemical constituents isolated from the pericarp of Toona sinensis.

Author

Wang, Rongshen, Liu, Di, Liu, Xiaoxiao, Liu, Fan, Xuan, Lulu, Tang, Ying, and Li, Wanzhong

Subjects

TOONA, PERICARP, EDIBLE plants, SILICA gel, TRITERPENOIDS

Abstract

Toona sinensis is a medicinal and edible plant that belongs to the genus Toona of family Meliaceae. Phytochemical investigations carried out on this plant, seven apotirucallane-type triterpenoids (1–7), two cycloartane-type triterpenoids (8–9), four sterols (10–13), two sesquiterpenes (14–15), four phenols (16–19), and one lignin (20) were isolated from the pericarp of T. sinensis by silica gel column and preparative middle pressure liquid chromatography. Their structures were identified by interpretation of NMR and comparison with those reported in the literature. Compounds 11–12, 15–16, and 18 were isolated from the family Meliaceae, compounds 13–14 were obtained from the genus Toona, and compound 19 was obtained from T. sinensis for the first time. Additionally, the cytotoxicity and polyol pathway (PP) inhibitory activities of active constituents were evaluated in rat glomerular mesangial cells cultured under high glucose conditions, suggesting their potential application for a PP inhibitor. [ABSTRACT FROM AUTHOR]

Published

2022

48. Effective fraction of Teucrium polium suppressed polyol pathway through inhibiting the aldose reductase enzyme: strategy to reduce retinopathy

Author

Somayeh Amraee, Seifollah Bahramikia, and Abdelnasser Mohammadi

Subjects

teucrium polium, aldose reductase, ethyl acetate fraction, polyol pathway, Therapeutics. Pharmacology, RM1-950, Toxicology. Poisons, RA1190-1270

Abstract

Background: Several metabolic pathways are involved in the complications of diabetes like polyol pathway. Aldose reductase (AR) is a key enzyme in the polyol pathway, which catalyzes the conversion of glucose to sorbitol. AR inhibitors are appropriate to prevent and treat the diabetes complications. Objective: This study was designed to investigate the effect of different fractions of Teucrium polium on the AR activity. Methods: Fifty cow’s eye lenses were prepared and AR enzyme was purified according to the Hyman-Kinoshita method. The enzyme activity in the presence of the crude extract and different fractions of Teucrium polium (1, 5, 10, 20 and 100 μg/ml) was measured. In addition, IC50 content of fractions was also measured for the neutralization of DPPH free radical. Since some AR inhibitors are phenolic compounds, the phenolic and flavonoid contents have been investigated. Results: Results showed that the highest phenol and flavonoid content and the lowest IC50 value (3.67 µg/ml) for AR inhibition were related to the ethyl acetate fraction. Line weaver-Burk plot showed that ethyl acetate fraction acts as a non-competitive enzyme inhibition. Conclusion: Thus, T. polium can be proposed as a therapy to prevent or treat chronic complications of diabetes in the future.

Published

2020

49. SORBITOL DEHYDROGENASE OF CATS BLOOD UNDER DIABETES MELLITUS

Author

I. Chala and V. Rusak

Subjects

polyol pathway, liver, enzymes, osmolality, hyperglycemia., Agriculture

Abstract

Diabetes mellitus is one of the most widely spread non-infectious cats and dogs diseases and in modern times it is reaching epidemic levels. The purpose of the research was to determine enzymes activity, which is a marker of liver’s functional activity: alanine aminotransferase, asparagine aminotransferase, alkaline phosphatase and sorbitol dehydrogenase in cats suffering from diabetes mellitus, and another purpose was to study the dynamics of sorbitol dehydrogenase activity. Two groups of cats aged 5–7 years old (males and females) 10 cats in each group were formed for the research. A control group comprised clinically healthy animals, experimental group comprised animals diagnosed with diabetes mellitus. The results of the research showed that in cats of the experimental group the glucose content was 3.31 times as high as in cats of a control group. Fructosamine characterizes the duration of hyperglycemia and in cats diagnosed with diabetes mellitus its content overshot the control indices by 32 %, that testifies to a long-standing increase in glucose amount. Because of diabetes mellitus, water-salt metabolism is damaged, for instance blood osmolality is increased. The determination of enzymes activity showed that transaminase activity doubled, whereas the alkaline phosphatase activity increased by 25 %. The concentration of total bilirubin increased more than three-fold as compared to the control. The sorbitol dehydrogenase activity in cats diagnosed with diabetes mellitus was in 2.25 times higher as compared to the animals in a control group. The activity of this enzyme, contrary to transaminase activity, is increased during the first days after hepatic dysfunction symptoms. Thus, in cats diagnosed with diabetes mellitus, liver function abnormality is developed which is manifested in activity changes of alanine aminotransferase, asparagine aminotransferase, alkaline phosphatase in the increase in bilirubin concentration as well as in the increase of sorbitol dehydrogenase activity. This enzyme is a valuable biochemical marker of liver function abnormality on the early stages of pathology development.

Published

2020

50. Osthole Prevents Heart Damage Induced by Diet-Induced Metabolic Syndrome: Role of Fructokinase (KHK)

Author

Fernando E. García-Arroyo, Guillermo Gonzaga-Sánchez, Alejandro Silva-Palacios, Francisco Javier Roldán, María L. Loredo-Mendoza, Yamnia Quetzal Alvarez-Alvarez, Jesus A. de los Santos Coyotl, Kevin A. Vélez Orozco, Edilia Tapia, Horacio Osorio-Alonso, Abraham S. Arellano-Buendía, José L. Sánchez-Gloria, Miguel A. Lanaspa, Richard J. Johnson, and Laura Gabriela Sánchez-Lozada

Subjects

cardiac hypertrophy, polyol pathway, hyperuricemia, Therapeutics. Pharmacology, RM1-950

Abstract

There is increasing evidence that either ingested or produced fructose may have a role in metabolic syndrome. While not commonly considered a criterion for metabolic syndrome, cardiac hypertrophy is often associated with metabolic syndrome, and its presence carries increased cardiovascular risk. Recently it has been shown that fructose and fructokinase C (KHK) can be induced in cardiac tissue. Here we tested whether diet-induced metabolic syndrome causes heart disease associated with increased fructose content and metabolism and whether it can be prevented with a fructokinase inhibitor (osthole). Male Wistar rats were provided a control diet (C) or high fat/sugar diet for 30 days (MS), with half of the latter group receiving osthol (MS+OT, 40 mg/kg/d). The Western diet increased fructose, uric acid, and triglyceride concentrations in cardiac tissue associated with cardiac hypertrophy, local hypoxia, oxidative stress, and increased activity and expression of KHK in cardiac tissue. Osthole reversed these effects. We conclude that the cardiac changes in metabolic syndrome involve increased fructose content and its metabolism and that blocking fructokinase can provide cardiac benefit through the inhibition of KHK with modulation of hypoxia, oxidative stress, hypertrophy, and fibrosis.

Published

2023