Your search keyword '"enkephalins"' showing total 10,383 results

1. Modification and Delivery of Enkephalins for Pain Modulation

Author

Hohenwarter, Lukas, Böttger, Roland, and Li, Shyh-Dar

Published

2023

2. The Role of Endogenous Beta-Endorphin and Enkephalins in the Crosstalk Between Ethanol and Morphine.

Author

Tseng, Andy, Ahmad, Syed Muzzammil, Hamid, Abdul, and Lutfy, Kabirullah

Subjects

*ENKEPHALINS, *KNOCKOUT mice, *OPIOID receptors, *MORPHINE, *MICE, *NARCOTICS, *OPIOID peptides, *NALTREXONE

Abstract

Background: There is clinical concern about the combined use of alcohol and opiates. Several lines of evidence support an interaction between alcohol and the endogenous opioid system. Thus, we hypothesized that ethanol, by causing the release of opioid peptides, may sensitize the system to the action of exogenous opioids such as morphine. Objectives: In this study, using the place conditioning paradigm, a model of reward, we determined whether a morphine challenge would alter the pre-established preference induced by ethanol conditioning in mice, and whether this response was mediated by the mu opioid receptor (MOP). Given that ethanol exposure stimulates the release of opioid peptides, we also assessed the role of beta-endorphin (β-END) and enkephalins (ENKs) in this response. Methods: Mice lacking MOPs, β-END, and/or ENKs, and their respective wild-type controls were tested for preconditioning place preference on day 1. Mice were then conditioned with ethanol (2 g/kg) versus saline on days 2 to 4 and then tested under a drug-free state for postconditioning place preference on day 5. On day 8, mice received a single injection of morphine (5 mg/kg) and were tested for place preference. On the test days, mice were placed in the central chamber and allowed to explore the chambers. The amount of time that mice spent in the drug-paired chamber was recorded. Results: We found that a challenge dose of morphine given on day 8 enhanced the conditioned place preference (CPP) response in mice previously conditioned with ethanol. This response was abolished in MOP-null mice, confirming the role of MOPs in this response. Although this enhanced response was not altered in mice lacking either β-END or ENKs compared to their wild-type littermates/controls, it was completely blunted in mice lacking both β-END and enkephalins. Conclusions: Together, these results suggest that these opioid peptides jointly mediate the crosstalk between the rewarding actions of morphine and ethanol. [ABSTRACT FROM AUTHOR]

Published

2025

3. Furosemide stress test to predict acute kidney injury progression in critically ill children.

Author

Krishnasamy, Sudarsan, Sinha, Aditi, Lodha, Rakesh, Sankar, Jhuma, Tarik, Mohamad, Ramakrishnan, Lakshmy, Bagga, Arvind, and Hari, Pankaj

Subjects

*ENKEPHALINS, *FUROSEMIDE, *CRITICALLY ill, *PATIENTS, *CARRIER proteins, *HEART function tests, *NEUTROPHILS, *ACUTE kidney failure, *TERTIARY care, *DESCRIPTIVE statistics, *PEDIATRICS, *INTRAVENOUS therapy, *INTENSIVE care units, *CONFIDENCE intervals, *DISEASE progression, *BIOMARKERS, *CHILDREN

Abstract

Background: Furosemide stress test (FST) is a novel functional biomarker for predicting severe acute kidney injury (AKI); however, pediatric studies are limited. Methods: Children 3 months to 18 years of age admitted to the intensive care unit (ICU) of a tertiary care hospital from Nov 2019 to July 2021 were screened and those who developed AKI stage 1 or 2 within 7 days of admission underwent FST (intravenous furosemide 1 mg/kg). Urine output was measured hourly for the next 6 h; a value > 2 ml/kg within the first 2 h was deemed furosemide responsive. Other biomarkers like plasma neutrophil gelatinase-associated lipocalin (NGAL) and proenkephalin (PENK) were also evaluated. Results: Of the 480 admitted patients, 51 developed AKI stage 1 or 2 within 7 days of admission and underwent FST. Nine of these patients were furosemide non-responsive. Thirteen (25.5%) patients (eight of nine from FST non-responsive group) developed stage 3 AKI within 7 days of FST, nine (17.6%) of whom (seven from non-responsive group) required kidney support therapy (KST). FST emerged as a good biomarker for predicting stage 3 AKI and need for KST with area-under-the-curve (AUC) being 0.93 ± 0.05 (95% CI 0.84–1.0) and 0.96 ± 0.03 (95% CI 0.9–1.0), respectively. FST outperformed NGAL and PENK in predicting AKI stage 3 and KST; however, the combination did not improve the diagnostic accuracy. Conclusions: Furosemide stress test is a simple, inexpensive, and robust biomarker for predicting stage 3 AKI and KST need in critically ill children. Further research is required to identify the best FST cut-off in children. [ABSTRACT FROM AUTHOR]

Published

2025

4. Inflammatory pain resolution by mouse serum-derived small extracellular vesicles.

Author

Lin, Zhucheng, Luo, Xuan, Wickman, Jason R., Reddy, Deepa, DaCunza, Jason T., Pande, Richa, Tian, Yuzhen, Kasimoglu, Ezgi E., Triana, Vivian, Lee, Jingyun, Furdui, Cristina M., Pink, Desmond, Sacan, Ahmet, and Ajit, Seena K.

Subjects

*DORSAL root ganglia, *EXTRACELLULAR vesicles, *CELL populations, *INTRATHECAL injections, *ENKEPHALINS

Abstract

• Extensively characterized sEVs from SNI model mice serum. • Detected endogenous leu-enkephalin in serum sEVs. • Prophylactic sEVs accelerated recovery from inflammatory pain. • Immune cell alterations probed by ChipCytometry and flow cytometry. Current treatments for chronic pain have limited efficacy and significant side effects, warranting research on alternative strategies for pain management. One approach involves using small extracellular vesicles (sEVs), or exosomes, to transport beneficial biomolecular cargo to aid pain resolution. Exosomes are 30–150 nm sEVs that can be beneficial or harmful depending on their source and cargo composition. We report a comprehensive multi-modal analysis of different aspects of sEV characterization, miRNAs, and protein markers across sEV sources. To investigate the short- and long-term effects of mouse serum-derived sEVs in pain modulation, sEVs from naïve control or spared nerve injury (SNI) model male donor mice were injected intrathecally into naïve male recipient mice. These sEVs transiently increased basal mechanical thresholds, an effect mediated by opioid signaling as this outcome was blocked by naltrexone. Mass spectrometry of sEVs detected endogenous opioid peptide leu-enkephalin. sEVs from naïve female mice have higher levels of leu-enkephalin compared to male, matching the analgesic onset of leu-enkephalin in male recipient mice. In investigating the long-term effect of sEVs, we observed that a single prophylactic intrathecal injection of sEVs two weeks prior to induction of the pain model in recipient mice accelerated recovery from inflammatory pain after complete Freund's adjuvant (CFA) injection. Our exploratory studies examining immune cell populations in spinal cord and dorsal root ganglion using ChipCytometry suggested alterations in immune cell populations 14 days post-CFA. Flow cytometry confirmed increases in CD206+ macrophages in the spinal cord in sEV-treated mice. Collectively, these studies demonstrate multiple mechanisms by which sEVs can attenuate pain. [ABSTRACT FROM AUTHOR]

Published

2025

5. Proenkephalin plasma levels as a predictor of acute kidney injury in adult septic subjects.

Author

Ampulembang, Diana Tangdan, Mangarengi, Fitriani, Widaningsih, Yuyun, Patellongi, Ilham Jaya, Muchtar, Faisal, and Kadir, Nursin Abd

Subjects

ENKEPHALINS, PREDICTIVE tests, DATA analysis, ENZYME-linked immunosorbent assay, ACUTE kidney failure, MANN Whitney U Test, DESCRIPTIVE statistics, LONGITUDINAL method, SEPSIS, STATISTICS, BIOMARKERS, DISEASE risk factors, DISEASE complications, ADULTS

Abstract

Background: Sepsis is a leading cause of increased morbidity and mortality rates in hospitalized patients and is the most common cause of acute kidney injury (AKI). A potential biomarker that can predict the occurrence of AKI in septic patients is proenkephalin (PENK), an endogenous precursor of opioids. Methods: This prospective cohort study included 40 septic patients at Wahidin Sudirohusodo Hospital, Makassar, from March to May 2024. Plasma levels of PENK were measured using the enzyme-linked immunosorbent assay (ELISA) method. Data were analyzed statistically using the Shapiro-Wilk, Mann-Whitney, Wilcoxon, and Spearman correlation tests. Results: The study included 23 men (57.5%) and 17 women (42.5%). Patients predominantly required ventilators as respiratory aids (35%). The average length of stay was 23.5 days. The mean . Sequential Organ Failure Assessment (SOFA) score was 5.03±2.6. The mean procalcitonin level was 38.6±56.2, with a range of 0.12-249.26. The mean PENK level on day 7 was lower (294.67 pg/ml) than the initial level (402.02 pg/ml) in septic patients who did not experience AKI. In septic patients who experienced AKI, the mean PENK level on day 7 was higher (421.56 pg/ml) than the initial level (191.78 pg/ml). A plasma PENK level >194.65 pg/ml can indicate AKI in adult septic patients with a sensitivity of 62.5% and a specificity of 82.25%, with a positive likelihood ratio of 3.33. Conclusion: There was a significant difference between the initial PENK levels and the PENK levels on day 7 in septic patients who did not experience AKI and those who did. Plasma PENK levels in septic patients could be used as a predictive marker for the likelihood of acute kidney injury. [ABSTRACT FROM AUTHOR]

Published

2024

6. Plasma proenkephalin A and incident chronic kidney disease and albuminuria in the REasons for Geographic And Racial Differences in Stroke (REGARDS) cohort.

Author

Bullen, Alexander, Katz, Ronit, Poursadrolah, Sayna, Short, Samuel, Long, D, Cheung, Katharine, Sharma, Shilpa, Al-Rousan, Tala, Fregoso, Alma, Schulte, Janin, Gutierrez, Orlando, Shlipak, Michael, Cushman, Mary, Ix, Joachim, and Rifkin, Dena

Subjects

albuminuria, biomarker, chronic kidney disease, proenkephalin A, Humans, Female, Middle Aged, Male, Albuminuria, Race Factors, Renal Insufficiency, Chronic, Stroke, Enkephalins, Protein Precursors

Abstract

BACKGROUND: Plasma proenkephalin A (PENK-A) is a precursor of active enkephalins. Higher blood concentrations have been associated with estimated glomerular filtration rate (eGFR) decline in European populations. Due to the significant disparity in incident chronic kidney disease (CKD) between White and Black people, we evaluated the association of PENK-A with incident CKD and other kidney outcomes among a biracial cohort in the U.S. METHODS: In a nested cohort of 4,400 participants among the REasons for Geographic And Racial Differences in Stroke, we determined the association between baseline PENK-A concentration and incident CKD using the creatinine-cystatin C CKD-EPI 2021 equation without race coefficient, significant eGFR decline, and incident albuminuria between baseline and a follow-up visit 9.4 years later. We tested for race and sex interactions. We used inverse probability sampling weights to account for the sampling design. RESULTS: At baseline, mean (SD) age was 64 (8) years, 49% were women, and 52% were Black participants. 8.5% developed CKD, 21% experienced ≥ 30% decline in eGFR and 18% developed albuminuria. There was no association between PENK-A and incident CKD and no difference by race or sex. However, higher PENK-A was associated with increased odds of progressive eGFR decline (OR: 1.12; 95% CI 1.00, 1.25). Higher PENK-A concentration was strongly associated with incident albuminuria among patients without diabetes mellitus (OR: 1.29; 95% CI 1.09, 1.53). CONCLUSION: While PENK-A was not associated with incident CKD, its associations with progression of CKD and incident albuminuria, among patients without diabetes, suggest that it might be a useful tool in the evaluation of kidney disease among White and Black patients.

Published

2024

7. Opiorphin: an endogenous human peptide with intriguing application in diverse range of pathologies.

Author

Tiwari, Chanchal, Khan, Heena, Grewal, Amarjot Kaur, Dhankhar, Sanchit, Chauhan, Samrat, Dua, Kamal, Gupta, Gaurav, and Singh, Thakur Gurjeet

Subjects

*OPIOID peptides, *PEPTIDES, *PAIN perception, *ENKEPHALINS, *CARDIOVASCULAR system, *OPIOID receptors

Abstract

Mammalian zinc ectopeptidases have significant functions in deactivating neurological and hormonal peptide signals on the cell surface. The identification of Opiorphin, a physiological inhibitor of zinc ectopeptidases that inactivate enkephalin, has revealed its strong analgesic effects in both chemical and mechanical pain models. Opiorphin achieves this by increasing the transmission of endogenous opioids, which are dependent on the body's own opioid system. The function of opiorphin is closely linked to the rat sialorphin peptide, which inhibits pain perception by enhancing the activity of naturally occurring enkephalinergic pathways that depend on μ- and δ-opioid receptors. Opiorphin is highly intriguing in terms of its physiological implications within the endogenous opioidergic pathways, particularly in its ability to regulate mood-related states and pain perception. Opiorphin can induce antidepressant-like effects by influencing the levels of naturally occurring enkephalin, which are released in response to specific physical and/or psychological stimuli. This effect is achieved through the modulation of delta-opioid receptor-dependent pathways. Furthermore, research has demonstrated that opiorphin's impact on the cardiovascular system is facilitated by the renin–angiotensin system (RAS), sympathetic ganglia, and adrenal medulla, rather than the opioid system. Hence, opiorphin shows great potential as a solitary candidate for the treatment of several illnesses such as neurodegeneration, pain, and mood disorders. [ABSTRACT FROM AUTHOR]

Published

2024

8. Effects of Neonatal Administration of Non-Opiate Analogues of Leu-Enkephalin on the Delayed Cardiac Consequences of Intrauterine Hypoxia.

Author

Gusev, I. A., Malofey, Yu. B., and Sazonova, E. N.

Subjects

*PEPTIDES, *NITRIC-oxide synthases, *MAST cells, *HEART cells, *ENKEPHALINS

Abstract

Intrauterine hypoxia (gestation days 15-19, pO2 65 mm Hg, duration 4 h) led to an increase in the expression of p53, beclin-1, endothelial NO synthase (eNOS), and caspase-3 proteins in cardiomyocytes and reduced the number of mast cells in the heart of 60-day-old albino rats. Administration of a non-opiate analogue of leu-enkephalin (NALE peptide: Phe–D-Ala–Gly–Phe–Leu–Arg, 100 μg/kg) on days 2-6 of the neonatal period decreased the severity of delayed posthypoxic myocardial reaction. The content of eNOS+ cardiomyocytes and the total number of mast cells of these animals did not differ from the control parameters; the content of p53+ cardiomyocytes was significantly lower than in animals exposed to intrauterine hypoxia. The cardioprotective activity of NALE was partially neutralized by co-administration with the NO synthase inhibitor (L-NAME, 50 mg/kg). Correction of the delayed posthypoxic changes, similar to the effects of NALE peptide, was observed after neonatal administration of its arginine-free analogue, G peptide (Phe–D-Ala–Gly–Phe–Leu–Gly; 100 μg/kg). Non-opiate analogues of leu-enkephalin NALE and G peptides can be considered as promising substances capable of preventing long-term cardiac consequences of intrauterine hypoxia. [ABSTRACT FROM AUTHOR]

Published

2024

9. A nanomedicine approach for the treatment of long-lasting pain.

Author

Hazam, Hadjer, Prades, Lucas, Cailleau, Catherine, Mougin, Julie, Feng, Jiao, Benhamou, Dan, Gobeaux, Frédéric, Hamdi, Leïla, Couvreur, Patrick, Sitbon, Philippe, and Lepetre-Mouelhi, Sinda

Subjects

*LABORATORY rats, *POSTOPERATIVE pain, *CENTRAL nervous system, *PAIN management, *ENKEPHALINS

Abstract

This study explores the potential of a nanomedicine approach, using Leu-enkephalin-squalene nanoparticles (LENK-SQ NPs) for managing long-lasting pain. It was observed that the nanomedicine significantly improved the pharmacological efficacy of the Leu-enkephalin, a fast metabolized neuropeptide, in a rat model of acute inflammatory pain, providing local analgesic effect, while minimizing potential systemic side effects by circumventing central nervous system. The LENK-SQ NPs were tested in a rat model of postoperative pain (Brennan's rodent plantar incision model) using continuous infusion via Alzet® pump, with an additional bolus injection. The analgesic activity was assessed through stimulus-evoked methods, such as the von Frey and Hargreaves tests. Both mechanical and thermal hyperalgesia were significantly reduced at days 2 and 3 post-incision. An additional pharmacokinetic study was conducted, showing that LENK-SQ NPs allowed a sustained circulation of the neuropeptide under its prodrug form. On the other hand, the biodistribution of fluorescently labelled LENK-SQ NPs revealed their selective accumulation in the incised paw within the first hour post administration, followed by a disassembly of the NPs, starting 24 h later. The study proposes the following multi-step mechanism for the anti-nociceptive pharmacological activity of LENK-SQ NPs: (i) protection of the neuropeptide from metabolization into the bloodstream, (ii) targeted accumulation of the nanoparticles within the incised painful tissue and (iii) gradual release of LENK at the onset of the inflammatory process, leading to the observed analgesic activity. [Display omitted] • Continuous L-enkephalin-squalene nanoparticles infusion relieves postoperative pain. • The long-lasting analgesia is obtained via in situ targeting of nanoparticles. • L-enkephalin-squalene nanoparticles increase the plasma half-life of the neuropeptide. • The accumulation of nanoparticles into painful tissues does not require transcytosis. [ABSTRACT FROM AUTHOR]

Published

2024

10. Enkephalins and Pain Modulation: Mechanisms of Action and Therapeutic Perspectives.

Author

García-Domínguez, Mario

Subjects

*OPIOID peptides, *ENKEPHALINS, *PERIPHERAL nervous system, *OPIOID receptors, *PEPTIDES

Abstract

Enkephalins, a subclass of endogenous opioid peptides, play a pivotal role in pain modulation. Enkephalins primarily exert their effects through opioid receptors located widely throughout both the central and peripheral nervous systems. This review will explore the mechanisms by which enkephalins produce analgesia, emotional regulation, neuroprotection, and other physiological effects. Furthermore, this review will analyze the involvement of enkephalins in the modulation of different pathologies characterized by severe pain. Understanding the complex role of enkephalins in pain processing provides valuable insight into potential therapeutic strategies for managing pain disorders. [ABSTRACT FROM AUTHOR]

Published

2024

11. Disparate Effects of Stressors on Met-Enkephalin System Parameters and on Plasma Concentrations of Corticosterone in Young Female Chickens.

Author

Scanes, Colin Guy and Pierzchala-Koziec, Krystyna

Subjects

*ANTERIOR pituitary gland, *ENKEPHALINS, *CORTICOSTERONE, *NALTREXONE, *CHICKENS

Abstract

Simple Summary: There are multiple physiological changes in response to stress across vertebrate species. These shift metabolism and organ functioning such that the animals can withstand the stress. Ours results show that nutritional deprivation and crowding stimulate both the activities of the opioid system and the adrenocortical axis stress response in chickens. The effects of stressors were examined on Met-enkephalin-related parameters and plasma concentrations of corticosterone in 14-week-old female chickens. Water deprivation for 24 h was accompanied by a tendency for increased plasma concentration of Met-enkephalin while plasma concentrations of corticosterone were elevated in water-deprived birds. Concentrations of Met-enkephalin were reduced in the anterior pituitary gland and adrenal gland in water-deprived pullets while proenkephalin (PENK) expression was increased in both tissues. There were changes in the plasma concentrations of Met-enkephalin and corticosterone in pullets subjected to either feed withholding or crowding. Concentrations of Met-enkephalin were increased in the anterior pituitary gland but decreased in adrenal glands in pullets subjected to crowding stress. The increase in the plasma concentrations of Met-enkephalin was ablated when the chickens were pretreated with naltrexone. However, naltrexone did not influence either basal or crowding on plasma concentrations of corticosterone. In vitro release of Met-enkephalin from the anterior pituitary or adrenal tissues was depressed in the presence of naltrexone. It was concluded that Met-enkephalin was part of the neuroendocrine response to stress in female chickens. It was concluded that stress influenced the release of both Met-enkephalin and corticosterone, but there was not complete parallelism. [ABSTRACT FROM AUTHOR]

Published

2024

12. Organization of enkephalinergic neuronal system in the central nervous system of the gecko Hemidactylus frenatus.

Author

Ganeyan, Ananya and Ganesh, C. B.

Subjects

*CENTRAL nervous system, *PREOPTIC area, *HEMIDACTYLUS, *GECKOS, *THALAMIC nuclei, *ENKEPHALINS

Abstract

Enkephalins are endogenous opioid pentapeptides that play a role in neurotransmission and pain modulation in vertebrates. However, the distribution pattern of enkephalinergic neurons in the brains of reptiles has been understudied. This study reports the organization of the methionine-enkephalin (M-ENK) and leucine-enkephalin (L-ENK) neuronal systems in the central nervous system of the gecko Hemidactylus frenatus using an immunofluorescence labeling method. Although M-ENK and L-ENK-immunoreactive (ir) fibers extended throughout the pallial and subpallial subdivisions, including the olfactory bulbs, M-ENK and L-ENK-ir cells were found only in the dorsal septal nucleus. Enkephalinergic perikarya and fibers were highly concentrated in the periventricular and lateral preoptic areas, as well as in the anterior and lateral subdivisions of the hypothalamus, while enkephalinergic innervation was observed in the hypothalamic periventricular nucleus, infundibular recess nucleus and median eminence. The dense accumulation of enkephalinergic content was noticed in the pars distalis of the hypophysis. In the thalamus, the nucleus rotundus and the dorsolateral, medial, and medial posterior thalamic nuclei contained M-ENK and L-ENK-ir fibers, whereas clusters of M-ENK and L-ENK-ir neurons were observed in the pretectum, mesencephalon, and rhombencephalon. The enkephalinergic fibers were also seen in the area X around the central canal, as well as the dorsal and ventral horns. The widespread distribution of enkephalin-containing neurons within the central nervous system implies that enkephalins regulate a variety of functions in the gecko, including sensory, behavioral, hypophysiotropic, and neuroendocrine functions. [ABSTRACT FROM AUTHOR]

Published

2024

13. Endogenous Opioids and Exercise-Related Hypoalgesia: Modern Models, Measurement, and Mechanisms of Action

Author

Goldfarb, Allan H., Kraemer, Robert R., Baiamonte, Brandon A., Schousboe, Arne, Series Editor, Kerr, Patrick L., editor, Sirbu, Cristian, editor, and Gregg, John M., editor

Published

2024

14. Neuropeptide Expression During the Ovarian Cycle and in Patients With PCOS (PCO-NP)

Author

Sandro Gerli, Associate Professor of Obstetrics and Gynecology

Published

2023

15. Dopamine D2 receptors bidirectionally regulate striatal enkephalin expression: Implications for cocaine reward.

Author

Dai, Kathy, Choi, In, Levitt, Ryan, Blegen, Mariah, Kaplan, Alanna, Matsui, Aya, Shin, J, Bocarsly, Miriam, Simpson, Eleanor, Kellendonk, Christoph, Alvarez, Veronica, and Dobbs, Lauren

Subjects

CP: Neuroscience, D2-receptor, GABA, addiction, cocaine, dopamine, enkephalin, reward, striatum, synaptic, withdrawal, Analgesics, Opioid, Animals, Cocaine, Cocaine-Related Disorders, Corpus Striatum, Enkephalin, Methionine, Enkephalins, Mice, Narcotic Antagonists, RNA, Messenger, Receptors, Dopamine D1, Receptors, Dopamine D2, Reward, gamma-Aminobutyric Acid

Abstract

Low dopamine D2 receptor (D2R) availability in the striatum can predispose for cocaine abuse; though how low striatal D2Rs facilitate cocaine reward is unclear. Overexpression of D2Rs in striatal neurons or activation of D2Rs by acute cocaine suppresses striatal Penk mRNA. Conversely, low D2Rs in D2-striatal neurons increases striatal Penk mRNA and enkephalin peptide tone, an endogenous mu-opioid agonist. In brain slices, met-enkephalin and inhibition of enkephalin catabolism suppresses intra-striatal GABA transmission. Pairing cocaine with intra-accumbens met-enkephalin during place conditioning facilitates acquisition of preference, while mu-opioid receptor antagonist blocks preference in wild-type mice. We propose that heightened striatal enkephalin potentiates cocaine reward by suppressing intra-striatal GABA to enhance striatal output. Surprisingly, a mu-opioid receptor antagonist does not block cocaine preference in mice with low striatal D2Rs, implicating other opioid receptors. The bidirectional regulation of enkephalin by D2R activity and cocaine offers insights into mechanisms underlying the vulnerability for cocaine abuse.

Published

2022

16. Highly sensitive in vivo detection of dynamic changes in enkephalins following acute stress (Updated September 25, 2024)

Subjects

Physical fitness, Enkephalins

Abstract

2024 OCT 12 (NewsRx) -- By a News Reporter-Staff News Editor at Obesity, Fitness & Wellness Week -- According to news reporting based on a preprint abstract, our journalists obtained [...]

Published

2024

17. The Effect of Dalargin on the Level of Corticosterone in Rats with Different Individual Typological Features of Behavior in the PTSD Model.

Author

Semenova, O. G., Vyushina, A. V., Pritvorova, A. V., Pivina, S. G., and Ordyan, N. E.

Subjects

*RATS, *CORTICOSTERONE, *POST-traumatic stress disorder, *ADRENAL glands, *SALINE solutions, *ENKEPHALINS

Abstract

The effect of the synthetic analogue of leu-enkephalin (dalargin) on the level of corticosterone in the blood and the mass of the adrenal glands in rats with various typological features of behavior in the model of post-traumatic stress disorder (PTSD) was studied. Groups were formed: active low-anxiety (ALA) and high-anxiety (AHA), as well as passive low-anxiety (PLA) and high-anxiety (PHA) rats. Each of the four groups of rats was divided into three subgroups, where subgroup 1 is an intact control. Twenty days after the first stressful exposure, rats from subgroup 3 were injected intramuscularly with dalargin for seven days, and rats from subgroup 2 were injected with saline solution. It was found that the course of injections of dalargin into rats in the PTSD model had a positive effect on the studied indicators only in the group of active high-anxiety animals. [ABSTRACT FROM AUTHOR]

Published

2024

18. Stapling of leu-enkephalin analogs with bifunctional reagents for prolonged analgesic activity.

Author

Kijewska, Monika, Wołczański, Grzegorz, Kosson, Piotr, Wieczorek, Robert, Lisowski, Marek, and Stefanowicz, Piotr

Subjects

*ENKEPHALINS, *ACID derivatives, *HEXAFLUOROBENZENE, *GLYCINE, *ANALGESICS, *RING formation (Chemistry), *OPIOID analgesics

Abstract

The design and synthesis of leu-enkephalin analogs by replacing the glycine residues with N-(2-thioethyl)glycines and opening the cyclisation potential is presented. The cyclization (stapling) was achieved using bifunctional reagents (hexafluorobenzene and trithiocyanuric acid derivatives). The CD conformational studies of the stapled analogs suggest that the peptides adopt the type I β-turn conformation, which is in agreement with the theoretical analysis. The analog containing a trithiocyanuric acid derivative with a benzyl substituent shows potent analgesic activity. [ABSTRACT FROM AUTHOR]

Published

2024

19. Synergistic effect of combining dual enkephalinase inhibitor PL37 and sumatriptan in a preclinical model of migraine.

Author

Rossignol, Jeanne, Ouimet, Tanja, Poras, Hervé, Dallel, Radhouane, and Luccarini, Philippe

Subjects

*ENKEPHALINS, *ISOSORBIDE dinitrate (Drug), *SUMATRIPTAN, *RESEARCH funding, *NITRIC oxide, *DATA analysis, *DESCRIPTIVE statistics, *DRUG efficacy, *ANIMAL experimentation, *NARCOTICS, *ANALYSIS of variance, *ONE-way analysis of variance, *STATISTICS, *DATA analysis software, *CONFIDENCE intervals, *MIGRAINE

Abstract

Objective: The aim of this study was to test whether a combination of sumatriptan with dual enkephalinase inhibitor PL37 would result in an additive or a synergistic effect. Background: Combination treatment is frequently used to improve the therapeutic efficacy of drugs. The co‐administration of two drugs may result in efficacy at lower doses than those needed for either drug alone, thus minimizing side effects. Here, we tested the effect of the co‐administration of two drugs on cutaneous mechanical hypersensitivity (MH), a symptom often affecting cephalic regions in patients with migraine: dual enkephalinase inhibitor PL37, a small molecule that protects enkephalins from rapid degradation, and sumatriptan, a serotonin 5‐HT1B/1D receptor agonist. Methods: We investigated the effects of oral administrations of sumatriptan, PL37, or their combination on changes in cutaneous mechanical sensitivity induced by a single intraperitoneal administration of the nitric oxide donor, isosorbide dinitrate (ISDN) in male rats. Mechanical sensitivity was assessed using von Frey filaments applied to the face of animals to determine pain thresholds. Isobolographic analysis was performed to determine the nature of the interaction between sumatriptan and PL37. Results: Sumatriptan as well as PL37 each produced a dose‐dependent inhibition of ISDN‐induced cephalic MH. Median effective dose (ED50) values were 0.3 and 1.1 mg/kg for sumatriptan and PL37, respectively. An isobolographic analysis of the effect of combined doses of sumatriptan and PL37 based on their calculated ED50 values demonstrated a synergistic effect of the combination on cephalic MH, with an interaction index of 0.14 ± 0.04. Conclusion: These results suggest that PL37 acts synergistically with sumatriptan to produce an anti‐allodynic effect in a rat model of migraine. Thus, combining PL37 and sumatriptan may be a useful therapeutic strategy in the management of migraine. Plain Language Summary: There have been many advances in migraine treatment, but we still need more options that are effective and have few side effects. Sumatriptan is one available drug for acute treatment of migraine, but it does not work for every patient and is not suitable for some people. We tested a new drug called PL37 (that blocks enkephalinases) together with sumatriptan and the combination minimized side effects and allowed lower doses of the drugs for effective migraine treatment in an animal model. [ABSTRACT FROM AUTHOR]

Published

2024

20. Enkephalin-mediated modulation of basal somatic sensitivity by regulatory T cells in mice

Author

Nicolas Aubert, Madeleine Purcarea, Julien Novarino, Julien Schopp, Alexis Audibert, Wangtianrui Li, Marie Fornier, Léonie Cagnet, Marie Naturel, Armanda Casrouge, Marie-Caroline Dieu-Nosjean, Nicolas Blanchard, Gilles Dietrich, Cedric Peirs, and Gilles Marodon

Subjects

pain, enkephalins, skin, immunoregulation, Medicine, Science, Biology (General), QH301-705.5

Abstract

CD4+CD25+Foxp3+ regulatory T cells (Treg) have been implicated in pain modulation in various inflammatory conditions. However, whether Treg cells hamper pain at steady state and by which mechanism is still unclear. From a meta-analysis of the transcriptomes of murine Treg and conventional T cells (Tconv), we observe that the proenkephalin gene (Penk), encoding the precursor of analgesic opioid peptides, ranks among the top 25 genes most enriched in Treg cells. We then present various evidence suggesting that Penk is regulated in part by members of the Tumor Necrosis Factor Receptor (TNFR) family and the transcription factor Basic leucine zipper transcription faatf-like (BATF). Using mice in which the promoter activity of Penk can be tracked with a fluorescent reporter, we also show that Penk expression is mostly detected in Treg and activated Tconv in non-inflammatory conditions in the colon and skin. Functionally, Treg cells proficient or deficient for Penk suppress equally well the proliferation of effector T cells in vitro and autoimmune colitis in vivo. In contrast, inducible ablation of Penk in Treg leads to heat hyperalgesia in both male and female mice. Overall, our results indicate that Treg might play a key role at modulating basal somatic sensitivity in mice through the production of analgesic opioid peptides.

Published

2024

21. Basic Science Prize Award 2023.

Author

Szabo, Edina and Olson, Patricia A.

Subjects

*HEADACHE treatment, *SERIAL publications, *CAFFEINE, *ENKEPHALINS, *HEADACHE, *FACIAL pain, *INTRACRANIAL pressure, *AWARDS, *CEREBROSPINAL fluid, *OPIOID receptors

Abstract

The article focuses on Headache's annual Basic Science Prize Award, recognizing outstanding research published in the journal, particularly in preclinical studies aimed at advancing understanding and treatment of headaches. Topics include studies on caffeine's impact on intracranial pressure in rats, the role of enkephalins in stress-induced migraine-like behavior in mice, and mitochondrial metabolism during migraine attacks in pediatric patients.

Published

2024

22. The History and Evolution of Intrathecal Drug Delivery: From the 1950s to the Present

Author

Penn, Richard D., Yaksh, Tony L., Yaksh, Tony, editor, and Hayek, Salim, editor

Published

2023

23. Ultrafast vibrational dynamics of the tyrosine ring mode and its application to enkephalin insertion into phospholipid membranes as probed by two-dimensional infrared spectroscopy

Author

Vinogradov, Ilya, Feng, Yuan, Kumar, SK Karthick, Guo, Chenxu, Udagawa, Nina Saki, and Ge, Nien-Hui

Subjects

Bioengineering, Density Functional Theory, Enkephalins, Lipid Bilayers, Molecular Conformation, Phospholipids, Spectroscopy, Fourier Transform Infrared, Temperature, Tyrosine, Vibration, Physical Sciences, Chemical Sciences, Engineering, Chemical Physics

Abstract

Enkephalins are small opioid peptides whose binding conformations are catalyzed by phospholipid membranes. Binding to opioid receptors is determined by the orientation of tyrosine and phenylalanine side chains. In this work, we investigate the effects of different charged phospholipid headgroups on the insertion of the tyrosine side chain into a lipid bilayer using a combination of 2D IR spectroscopy, anharmonic DFT calculations, and third order response function modeling. The insertion is probed by using the ∼1515 cm-1 tyrosine ring breathing mode, which we found exhibits rich vibrational dynamics on the picosecond timescale. These dynamics include rapid intramolecular vibrational energy redistribution (IVR), where some of the energy ends up in a dark state that shows up as an anharmonically shifted combination band. The waiting-time dependent 2D IR spectra also show an unusual line shape distortion that affects the extraction of the frequency-frequency correlation function (FFCF), which is the dynamic observable of interest that reflects the tyrosine side chain's insertion into the lipid bilayer. We proposed three models to account for this distortion: a hot-state exchange model, a local environment dependent IVR model, and a coherence transfer model. A qualitative analysis of these models suggests that the local environment dependent IVR rate best explains the line shape distortion, while the coherence transfer model best reproduced the effects on the FFCF. Even with these complex dynamics, we found that the tyrosine ring mode's FFCF is qualitatively correlated with the degree of insertion expected from the different phospholipid headgroups.

Published

2021

24. Proenkephalin deletion in hematopoietic cells induces intestinal barrier failure resulting in clinical feature similarities with irritable bowel syndrome in mice.

Author

Mas-Orea, Xavier, Rey, Lea, Battut, Louise, Bories, Cyrielle, Petitfils, Camille, Abot, Anne, Gheziel, Nadine, Wemelle, Eve, Blanpied, Catherine, Motta, Jean-Paul, Knauf, Claude, Barreau, Frederick, Espinosa, Eric, Aloulou, Meryem, Cenac, Nicolas, Serino, Matteo, Mouledous, Lionel, Fazilleau, Nicolas, and Dietrich, Gilles

Subjects

*IRRITABLE colon, *OPIOID receptors, *NOCICEPTORS, *HOMEOSTASIS, *OPIOID peptides, *BONE marrow cells, *ENKEPHALINS, *VISCERAL pain

Abstract

Opioid-dependent immune-mediated analgesic effects have been broadly reported upon inflammation. In preclinical mouse models of intestinal inflammatory diseases, the local release of enkephalins (endogenous opioids) by colitogenic T lymphocytes alleviate inflammation-induced pain by down-modulating gut-innervating nociceptor activation in periphery. In this study, we wondered whether this immune cell-derived enkephalin-mediated regulation of the nociceptor activity also operates under steady state conditions. Here, we show that chimeric mice engrafted with enkephalin-deficient bone marrow cells exhibit not only visceral hypersensitivity but also an increase in both epithelial paracellular and transcellular permeability, an alteration of the microbial topography resulting in increased bacteria-epithelium interactions and a higher frequency of IgA-producing plasma cells in Peyer's patches. All these alterations of the intestinal homeostasis are associated with an anxiety-like behavior despite the absence of an overt inflammation as observed in patients with irritable bowel syndrome. Thus, our results show that immune cell-derived enkephalins play a pivotal role in maintaining gut homeostasis and normal behavior in mice. Because a defect in the mucosal opioid system remarkably mimics some major clinical symptoms of the irritable bowel syndrome, its identification might help to stratify subgroups of patients. The study shows, by using hematopoietic chimeric mice, that mucosal immune cell-derived enkephalins play a pivotal role in maintaining gut homeostasis including visceral sensitivity and normal behavior in mice. [ABSTRACT FROM AUTHOR]

Published

2023

25. Proenkephalin Levels and Its Determinants in Patients with End-Stage Kidney Disease Treated with Hemodialysis and Peritoneal Dialysis.

Author

Grycuk, Wiktoria, Jakubowska, Zuzanna, and Małyszko, Jolanta

Subjects

*CHRONIC kidney failure, *PERITONEAL dialysis, *ACUTE kidney failure, *HEMODIALYSIS, *KIDNEY physiology, *URINE

Abstract

Recently, proenkephalin A (PENK A) has been shown to reflect glomerular dysfunction and to predict new-onset acute kidney injury and heart failure. While previous studies have investigated PENK A as a biomarker in individuals with preserved renal function, PENK A concentration in patients with end-stage kidney disease (ESKD) was not investigated. Plasma PENK A concentration was assessed in 88 patients with ESKD treated with hemodialysis (HD) or peritoneal dialysis (PD), and its associations with kidney function and heart failure indicators were investigated. In HD patients, the difference in PENK A levels before and after hemodialysis, was measured and further assessed for an association with the type of HD membrane used. PENK A levels did not differ significantly between HD and PD patients. In HD patients, the median PENK A concentration was significantly higher before than after hemodialysis (1.368 vs. 2.061, p = 0.003). No correlation was found between PENK A level and urea (p = 0.192), eGFR (p = 0.922), dialysis vintage (p = 0.637), and residual urine output (p = 0.784). Heart failure (p = 0.961), EF (p = 0.361), and NT-proBNP (p = 0.949) were not associated with increased PENK A concentration. PENK A does not reflect renal function and cardiac status in patients with ESKD. Further research is required to establish the clinical utility of the new biomarker in patients with impaired kidney function. [ABSTRACT FROM AUTHOR]

Published

2023

26. Five decades of research on opioid peptides: Current knowledge and unanswered questions

Author

Fricker, Lloyd D, Margolis, Elyssa B, Gomes, Ivone, and Devi, Lakshmi A

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Brain Disorders, Substance Misuse, Neurosciences, Biotechnology, Drug Abuse (NIDA only), 1.1 Normal biological development and functioning, Underpinning research, Animals, Brain, Carboxypeptidase H, Enkephalins, Humans, Opioid Peptides, Pro-Opiomelanocortin, Proprotein Convertases, Protein Precursors, Receptors, Opioid, Biochemistry and Cell Biology, Pharmacology & Pharmacy, Biochemistry and cell biology, Pharmacology and pharmaceutical sciences

Abstract

In the mid-1970s, an intense race to identify endogenous substances that activated the same receptors as opiates resulted in the identification of the first endogenous opioid peptides. Since then, >20 peptides with opioid receptor activity have been discovered, all of which are generated from three precursors, proenkephalin, prodynorphin, and proopiomelanocortin, by sequential proteolytic processing by prohormone convertases and carboxypeptidase E. Each of these peptides binds to all three of the opioid receptor types (μ, δ, or κ), albeit with differing affinities. Peptides derived from proenkephalin and prodynorphin are broadly distributed in the brain, and mRNA encoding all three precursors are highly expressed in some peripheral tissues. Various approaches have been used to explore the functions of the opioid peptides in specific behaviors and brain circuits. These methods include directly administering the peptides ex vivo (i.e., to excised tissue) or in vivo (in animals), using antagonists of opioid receptors to infer endogenous peptide activity, and genetic knockout of opioid peptide precursors. Collectively, these studies add to our current understanding of the function of endogenous opioids, especially when similar results are found using different approaches. We briefly review the history of identification of opioid peptides, highlight the major findings, address several myths that are widely accepted but not supported by recent data, and discuss unanswered questions and future directions for research. SIGNIFICANCE STATEMENT: Activation of the opioid receptors by opiates and synthetic drugs leads to central and peripheral biological effects, including analgesia and respiratory depression, but these may not be the primary functions of the endogenous opioid peptides. Instead, the opioid peptides play complex and overlapping roles in a variety of systems, including reward pathways, and an important direction for research is the delineation of the role of individual peptides.

Published

2020

27. Modulation of endogenous opioid signaling by inhibitors of puromycin sensitive aminopeptidase

Subjects

Physical fitness, Enkephalins

Abstract

2024 APR 20 (NewsRx) -- By a News Reporter-Staff News Editor at Obesity, Fitness & Wellness Week -- According to news reporting based on a preprint abstract, our journalists obtained [...]

Published

2024

28. Deletion of arrestin-3 does not improve compulsive drug- seeking behavior in a longitudinal paradigm of oral morphine self-administration (Updated March 22, 2024)

Subjects

Physical fitness, Opioid abuse, Morphine, Enkephalins

Abstract

2024 APR 13 (NewsRx) -- By a News Reporter-Staff News Editor at Obesity, Fitness & Wellness Week -- According to news reporting based on a preprint abstract, our journalists obtained [...]

Published

2024

29. Role of enkephalin derivative in promoting wound healing and scar remodeling via increased epidermal growth factor in a mouse model

Author

Sun Eung Kim, Yu Jin Kim, and Young Woo Cheon

Subjects

enkephalins, wound healing, cicatrix, epidermal growth factor, Surgery, RD1-811

Abstract

Background Enkephalin, an endogenous neuropeptide, binds to the delta (δ) opioid receptor and exerts an antinociceptive effect. Recent studies have suggested that neuropeptides might effectuate cutaneous wound healing. Therefore, we investigated the effects of an enkephalin derivative on wound healing and scar formation in vivo. Methods Enkephalin derivatives (leucine-enkephalin) were synthesized using the alanine scan method, and the most promising derivative (E10) was selected for further testing. In 15 C57BL/6N mice, two full-thickness skin defects (10 mm in diameter) were made on both sides of the back (left side, enkephalin group; right side, control group). The enkephalin group was administered 100 μL of E10 (AGGFL, 200 μg/mL), and the control group received phosphate-buffered saline. The wound size was digitally analyzed on days 2, 4, 7, and 10. After 21 days, the scar tissues were histologically evaluated for the scar depression index (SDI), and the epidermal growth factor (EGF) concentration was assessed using an enzyme-linked immunosorbent assay. Results The skin defect percentages were 98.4%±17.9% (day 2), 83.2%±24.0% (day 4), 39.7%±17.4% (day 7), and 16.2%±10.0% (day 10) in the control group and 86.1%±15.0% (day 2), 61.4%±11.6% (day 4), 26.6%±8.8% (day 7), and 16.4%±8.8% (day 10) in the enkephalin group. The SDI values were significantly lower in the enkephalin group (0.06±0.19) than in the control group (0.22±0.13, P

Published

2023

30. Effects of Non-Opiate Analogue of Leu-Enkephalin on the Ion Currents, Number of Nucleoli, and p53 Expression in Isolated Cardiomyocytes of Albino Rats.

Author

Sazonova, E. N., Gusev, I. A., and Filatova, T. S.

Subjects

*ENKEPHALINS, *NUCLEOLUS, *PEPTIDES, *P53 protein, *RATS

Abstract

Acute exposure of isolated ventricular cardiomyocytes to non-opiate analogue of leu-enkephalin (NALE peptide: Phe-D-Ala-Gly-Phe-Leu-Arg) in a concentration of 100 μg/liter and 6-h incubation in NALE solution did not significantly change ATP-dependent K+ current, L-type Ca2+ current, p53 protein expression, and number of nucleoli in the cardiomyocyte nuclei. Incubation of cardiomyocytes with NALE (100 μg/liter) in combination with NOP receptor blocker J-113397 (1 mg/liter) was followed by an increase in Ca2+ L-type current and the number of p53+ cells. The exposure of cardiomyocytes to NALE in a concentration 1000 μg/liter induced similar changes in the studied parameters (increase in Ca2+ L-type current and number of p53+ cardiomyocytes); an increase in the mean number of nucleoli was also observed. Our findings suggest that NALE peptide has direct effect on cardiomyocytes and NOP receptors are involved in this effect. [ABSTRACT FROM AUTHOR]

Published

2023

31. Endogenous Opioids in Crohn's Disease.

Author

Martyniak, Adrian, Wędrychowicz, Andrzej, and Tomasik, Przemysław J.

Subjects

OPIOID peptides, CROHN'S disease, INFLAMMATORY bowel diseases, DYNORPHINS, ENKEPHALINS, DISEASE remission

Abstract

Caring for patients with Crohn's disease (CD) is a serious challenge in modern medicine. The increasing incidence of CD among adolescents and the severe course of the disease create the need for new methods of diagnosis and therapy. Endogenous opioids are a group of low molecular weight chemical compounds with analgesic and anti-inflammatory properties. Endorphins, enkephalins, and dynorphins may have potentially beneficial effects on the course of CD. Previous research data on this topic are inconsistent. Some authors have reported an increase in the concentration of leukocytes during the course of inflammatory bowel disease (IBD) while others have described a downward trend, explained by DPP-IV enzyme activity. Even fewer data are available on plasma endo-opioid level. There is also a lack of comprehensive studies that have assessed the endo-opioid system in patients with IBD. Therefore, the objective of this study was to measure the serum concentrations of human β-endorphin, human proenkephalin (A), and human big dynorphin in CD patients in the acute phase of the disease, during hospital treatment, and in the remission state. All determinations were performed using ELISA kits. The results of our study showed that the concentrations of all the tested endo-opioids, especially β-endorphin and proenkephalin (A), were reduced in adolescents with CD compared to those in the healthy control group, during the acute phase of the disease, and in the remission state. Modulation of the endogenous opioid system and the use of selective nonnarcotic agonists of opioid receptors seems to be promising goals in the future treatment of CD. [ABSTRACT FROM AUTHOR]

Published

2023

32. Transmitters and Peptides: Basic Principles

Author

Devi, Lakshmi A., Fricker, Lloyd D., Pfaff, Donald W., editor, Volkow, Nora D., editor, and Rubenstein, John L., editor

Published

2022

33. Reports from Birla Institute of Technology and Science Pilani Advance Knowledge in Cardiorenal Disease [A Perspective On the Development of Small Molecular Neprilysin Inhibitors (Nepi) With Emphasis On Cardiorenal Disease]

Subjects

Diseases -- India, Valsartan, Angiotensin II, Medical research, Sacubitril, Enkephalins, Natriuretic peptides, Medicine, Experimental

Abstract

2024 DEC 20 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- A new study on Diseases and Conditions - Cardiorenal Disease is now available. [...]

Published

2024

34. Speeding up sustainable solution-phase peptide synthesis using T3P® as a green coupling reagent: methods and challenges.

Author

Mattellone, Alexia, Corbisiero, Dario, Ferrazzano, Lucia, Cantelmi, Paolo, Martelli, Giulia, Palladino, Chiara, Tolomelli, Alessandra, and Cabri, Walter

Subjects

*PEPTIDE synthesis, *RACEMIZATION, *ENKEPHALINS, *OLIGOPEPTIDES, *PROOF of concept, *PRODUCTION standards

Abstract

In peptide synthesis, the issues related to poor sustainability, long reaction times and high process mass intensity (PMI) are necessary to promote actions aimed at redefining procedural aspects projected towards more sustainable synthetic processes. Herein, we report a fast, widely applicable and green solution-phase peptide synthesis (GSolPPS) via a continuous protocol using propylphosphonic anhydride T3P® as the coupling reagent and N-benzyloxycarbonyl-protecting group (Z), which is easily removed by hydrogenation. Because N,N-dimethylformamide (DMF) replacement was a priority, the iterative process was performed in EtOAc, pushing further on overall sustainability. The efficiency of the synthetic protocol in terms of conversion, racemization and reaction times allowed extending the scope of the work to the synthesis of the standard peptide Leu-enkephalin as a proof of concept. Among the various explored procedures, the one-pot protocol (Acont plus), avoiding work-ups, intermediate purification and any dispersion effect, allowed the achievement of PMI = 30 for each deprotection/coupling sequence necessary to introduce a single amino acid in the iterative process, without considering the possibility of solvent and base recovery. This value is the lowest reported for an oligopeptide synthesis protocol to date. [ABSTRACT FROM AUTHOR]

Published

2023

35. Endogenous Opioid Imbalance as a Potential Factor Involved in the Pathogenesis of Chronic Kidney Disease-Associated Pruritus in Dialysis Patients.

Author

Wala-Zielińska, Kamila, Świerczyńska-Mróz, Karolina, Krajewski, Piotr K., Nowicka-Suszko, Danuta, Krajewska, Magdalena, and Szepietowski, Jacek C.

Subjects

*ITCHING, *HEMODIALYSIS patients, *OPIOID peptides, *CHRONIC kidney failure, *ENKEPHALINS, *OPIOIDS

Abstract

Chronic pruritus is one of the most common symptoms of dermatological diseases. It may occur in the course of other disorders, such as kidney disease. Chronic kidney disease-associated pruritus (CKD-aP) most often affects people with end-stage renal disease. The etiology of this condition is still not fully understood, but researchers are currently focusing on a thorough analysis of the association between disturbed opioid balance and increased neuronal signaling leading to pruritus. The aim of this study is to assess the concentration of endogenous opioids in dialysis patients with and without pruritus and in the control group, and to determine the correlation between the concentration of these substances and the occurrence and severity of itching. The study involved 126 dialysis patients and 50 healthy controls. Patients were divided into groups with pruritus (n = 62) and without pruritus (n = 64). The severity of pruritus was assessed using the NRS scale. The concentration of endogenous opioids was determined using the ELISA. The concentration of met-enkephalin was higher in the group of patients with pruritus compared to the control group. Moreover, significantly lower levels of β-endorphin and dynorphin A were observed in the group of dialysis patients compared to the control group. In addition, a statistically significant difference was seen between the β-endorphin concentration in the group of dialysis patients with pruritus compared to the group without pruritus. The ratio of β-endorphin/dynorphin A concentrations was significantly lower in the group of patients with pruritus compared to patients without pruritus and the control group. No correlations were found between serum level of studied opioids and the severity of pruritus. The concentrations of the studied opioids did not correlate with the severity of pruritus. Observed opioid imbalance may affect the occurrence of CKD-aP in dialysis patients, but a thorough understanding of the mechanism of action of these substances in the sensation of pruritus is necessary to assess the possibility of finding a new therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2023

36. The inhibition of enkephalin catabolism by dual enkephalinase inhibitor: A novel possible therapeutic approach for opioid use disorders.

Author

Alvarez‐Perez, Beltran, Poras, Hervé, and Maldonado, Rafael

Subjects

*OPIOID abuse, *OPIOID receptors, *THERAPEUTICS, *OPIOID peptides, *OPIOID epidemic, *ENKEPHALINS

Abstract

Despite the increasing impact of opioid use disorders on society, there is a disturbing lack of effective medications for their clinical management. An interesting innovative strategy to treat these disorders consists in the protection of endogenous opioid peptides to activate opioid receptors, avoiding the classical opioid‐like side effects. Dual enkephalinase inhibitors (DENKIs) physiologically activate the endogenous opioid system by inhibiting the enzymes responsible for the breakdown of enkephalins, protecting endogenous enkephalins and increasing their half‐lives and physiological actions. The activation of opioid receptors by the increased enkephalin levels, and their well‐demonstrated safety, suggests that DENKIs could represent a novel analgesic therapy and a possible effective treatment for acute opioid withdrawal, as well as a promising alternative to opioid substitution therapy minimizing side effects. This new pharmacological class of compounds could bring effective and safe medications avoiding the major limitations of exogenous opioids, representing a novel approach to overcome the problem of opioid use disorders. LINKED ARTICLES: This article is part of a themed issue on Advances in Opioid Pharmacology at the Time of the Opioid Epidemic. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v180.7/issuetoc [ABSTRACT FROM AUTHOR]

Published

2023

37. Characterization of the enzymatic properties of human RNPEPL1/aminopeptidase Z.

Author

Ohnishi, Atsushi and Tsujimoto, Masafumi

Subjects

*PEPTIDES, *OPIOID peptides, *AMINO acid sequence, *AMINO acids, *ENKEPHALINS, *AMINOPEPTIDASES

Abstract

It is now evident that the M1 family of aminopeptidases play important roles in many pathophysiological processes. Among them, the enzymatic properties of arginyl aminopeptidase-like 1 (RNPEPL1) are characterized only by its truncated form. No peptide substrate has been identified. To characterize the enzymatic properties of RNPEPL1 in more detail, the full-length protein was expressed in Escherichia coli and purified to homogeneity. The full-length RNPEPL1 showed rather restricted substrate specificity and basic amino acid preference towards synthetic substrates, which was different from the previously reported specificity characterized by the truncated form. Searching for peptide substrates, we found that several peptides, such as Met-enkephalin and kallidin, were cleaved. RNPEPL1 cleaved bradykinin to de-[Arg]-bradykinin despite the presence of proline at the P2'-position. The enzyme cleaved Met-enkephalin but not dynorphin A1–17. Similar to aminopeptidase B, the full-length RNPEPL1 showed basic amino acid preference towards both synthetic and peptide substrates. In addition to the unusual cleavage of bradykinin, this enzyme shows chain length-dependent cleavage of peptide substrates sharing N-terminal amino acid sequence. This is the first study to report the enzymatic properties of the full-length human RNPEPL1 as an aminopeptidase enzyme. [ABSTRACT FROM AUTHOR]

Published

2023

38. Enkephalin-δ Opioid Receptor Signaling Mediates Glucoprivic Suppression of LH Pulse and Gluconeogenesis in Female Rats.

Author

Tsuchida, Hitomi, Nonogaki, Miku, Takizawa, Marina, Inoue, Naoko, Uenoyama, Yoshihisa, and Tsukamura, Hiroko

Subjects

ENKEPHALINS, GLUCONEOGENESIS, LABORATORY rats

Abstract

Energy availability is an important regulator of reproductive function at various reproductive phases in mammals. Glucoprivation induced by 2-deoxy-D-glucose (2DG), an inhibitor of glucose utilization, as an experimental model of malnutrition suppresses the pulsatile release of GnRH/LH and induces gluconeogenesis. The present study was performed with the aim of examining whether enkephalin-δ-opioid receptor (DOR) signaling mediates the suppression of pulsatile GnRH/LH release and gluconeogenesis during malnutrition. The administration of naltrindole hydrochloride (NTI), a selective DOR antagonist, into the third ventricle blocked the suppression of LH pulses and part of gluconeogenesis induced by IV 2DG administration in ovariectomized rats treated with a negative feedback level of estradiol-17 β (OVX + low E2). The IV 2DG administration significantly increased the number of Penk (enkephalin gene)-positive cells coexpressing fos (neuronal activation marker gene) in the paraventricular nucleus (PVN), but not in the arcuate nucleus (ARC) in OVX + low E2 rats. Furthermore, double in situ hybridization for Penk / Pdyn (dynorphin gene) in the PVN revealed that approximately 35% of the PVN Penk -expressing cells coexpressed Pdyn. Double in situ hybridization for Penk / Crh (corticotropin-releasing hormone gene) in the PVN and Penk / Kiss1 (kisspeptin gene) in the ARC revealed that few Penk -expressing cells coexpressed Crh and Kiss1. Taken together, these results suggest that central enkephalin-DOR signaling mediates the suppression of pulsatile LH release during malnutrition. Moreover, the current study suggests that central enkephalin-DOR signaling is also involved in gluconeogenesis during malnutrition in female rats. [ABSTRACT FROM AUTHOR]

Published

2023

39. The Involvement of Endogenous Enkephalins in Glucose Homeostasis †.

Author

Escolero, Vanessa, Tolentino, Laica, Muhammad, Abdul Bari, Hamid, Abdul, and Lutfy, Kabirullah

Subjects

ENKEPHALINS, TYPE 2 diabetes, HOMEOSTASIS, BLOOD sugar, GLUCOSE tolerance tests

Abstract

Obesity has nearly tripled since 1975 and is predicted to continue to escalate. The surge in obesity is expected to increase the risk of diabetes type 2, hypertension, coronary artery disease, and stroke. Therefore, it is essential to better understand the mechanisms that regulate energy and glucose homeostasis. The opioid system is implicated in regulating both aspects (hedonic and homeostatic) of food intake. Specifically, in the present study, we investigated the role of endogenous enkephalins in changes in food intake and glucose homeostasis. We used preproenkephalin (ppENK) knockout mice and their wildtype littermates/controls to assess changes in body weight, food intake, and plasma glucose levels when mice were fed a high-fat diet for 16 weeks. Body weight and food intake were measured every week (n = 21–23 mice per genotype), and at the end of the 16-week exposure period, mice were tested using the oral glucose tolerance test (OGTT, n = 9 mice per genotype) and insulin tolerance test (n = 5 mice per genotype). Our results revealed no difference in body weight or food intake between mice of the two genotypes. However, HFD-exposed enkephalin-deficient mice demonstrated impaired OGTT associated with reduced insulin sensitivity compared to their wildtype controls. The impaired insulin sensitivity is possibly due to the development of peripheral insulin resistance. Our results reveal a potential role of enkephalins in the regulation of glucose homeostasis and in the pathophysiology of diabetes type 2. [ABSTRACT FROM AUTHOR]

Published

2023

40. A Caged Enkephalin Optimized for Simultaneously Probing Mu and Delta Opioid Receptors

Author

Banghart, Matthew R, He, Xinyi J, and Sabatini, Bernardo L

Subjects

Neurosciences, Animals, Enkephalin, Ala(2)-MePhe(4)-Gly(5)-, Enkephalins, Hippocampus, Neurons, Potassium Channels, Rats, Sprague-Dawley, Receptors, Opioid, delta, Receptors, Opioid, mu, Synaptic Transmission, Caged compounds, neuropeptides, opioid receptors, potassium channels, synaptic transmission, neurophysiology, Medicinal and Biomolecular Chemistry

Abstract

Physiological responses to the opioid neuropeptide enkephalin often involve both mu and delta opioid receptors. To facilitate quantitative studies into opioid signaling, we previously developed a caged [Leu5]-enkephalin that responds to ultraviolet irradiation, but its residual activity at delta receptors confounds experiments that involve both receptors. To reduce residual activity, we evaluated side-chain, N-terminus, and backbone caging sites and further incorporated the dimethoxy-nitrobenzyl moiety to improve sensitivity to ultraviolet light-emitting diodes (LEDs). Residual activity was characterized using an in vitro functional assay, and the power dependence and kinetics of the uncaging response to 355 nm laser irradiation were assayed using electrophysiological recordings of mu opioid receptor-mediated potassium currents in brain slices of rat locus coeruleus. These experiments identified N-MNVOC-LE as an optimal compound. Using ultraviolet LED illumination to photoactivate N-MNVOC-LE in the CA1 region of hippocampus, we found that enkephalin engages both mu and delta opioid receptors to suppress inhibitory synaptic transmission.

Published

2018

41. Influence of Mutations of Conserved Arginines on Neuropeptide Binding in the DPP III Active Site.

Author

Tomić, Antonija, Karačić, Zrinka, and Tomić, Sanja

Subjects

*MOLECULAR dynamics, *ENKEPHALINS, *OPIOID peptides, *PROTEOLYSIS, *NEUROPEPTIDES, *BINDING energy

Abstract

Dipeptidyl peptidase III (DPP III), a zinc exopeptidase, is involved in the final steps of intercellular protein degradation and has a marked affinity for opioid peptides such as enkephalins and endomorphins. Recently, we characterized a number of neuropeptides as potential substrates and inhibitors of human DPP III and provided an explanation for their differential behavior. These studies prompted us to investigate the influence of the conserved R399 and R669 on neuropeptides binding to DPP III. Measuring kinetic parameters in inhibitory assays, we found that mutation of R669 to Ala or Met significantly reduced the inhibitory properties of the slow substrates tynorphin and valorphin, whereas the effects on binding of the good substrates Arg2-2NA and Leu-enkephalin were small. Molecular dynamics simulations of wild-type (WT) and mutant DPP III complexes with Leu-enkephalin, tynorphin, valorphin, and Arg2-2NA in conjunction with calculations of binding free energies revealed that the lower inhibitory potency of slow substrates in the R669A mutant can be explained by the lower binding affinity of tynorphin and the higher propensity of valorphin to hydrolyze in the mutant than in WT. The R399A mutation was shown to affect the binding and/or hydrolysis of both good and slow substrates, with the effects on Leu-enkephalin being the most pronounced. [ABSTRACT FROM AUTHOR]

Published

2023

42. Morphology and immunohistochemical characteristics of the otic ganglion in the chinchilla (Chinchilla laniger Molina).

Author

Sienkiewicz, Waldemar, Kuchinka, Jacek, Dudek, Agnieszka, Nowak, Elżbieta, Kaleczyc, Jerzy, Radzimirska, Małgorzata, and Szczurkowski, Aleksander

Subjects

AUTONOMIC ganglia, MORPHOGENESIS, RODENTS, NEUROSCIENCES, ACETYLCHOLINESTERASE, NEURONS, STAINS & staining (Microscopy), NITRIC-oxide synthases, IMMUNOHISTOCHEMISTRY, ANIMAL experimentation, NEUROPEPTIDES, NEUROTRANSMITTERS, COMPARATIVE studies, CELLS, HISTOLOGICAL techniques, FLUORESCENT antibody technique, DESCRIPTIVE statistics, ENKEPHALINS, DRUGS, SOMATOSTATIN, ACETYLTRANSFERASES

Abstract

Introduction. The available literature provides relatively little information on the morphology of the autonomic head ganglia in rodents including their neurochemical codding. Material and methods. Morphological investigations of the otic ganglion of the chinchilla were performed using the modified acetylcholinesterase method. The cellular structure was investigated with histological techniques and neurochemical properties were studied with the double-labelling immunofluorescence method. Results. Macromorphological investigations allowed the otic ganglion to be identified as a compact, oval agglomeration of neurons and nerve fibers. Multidimensional cross-sections revealed densely arranged neuronal perikarya and two populations of nerve cells differing in size were distinguished. The large cells (40–50 μm) accounted for about 80% of the neurons in the cross-sections. Moreover, a small number of intraganglionic nerve fibers was observed. Immunohistochemical staining revealed that over 85% of the neuronal cell bodies in the otic ganglion contained immunoreactivity to VAChT or ChAT. VIP-immunoreactive perikarya comprised approximately 10% of the ganglionic cells. Double staining revealed the presence of VAChT+ and NOS+ neurons which amounted to about 45% of the nerve cells in the otic ganglion. NOS+ only perikarya comprised approx. 15% of all the neurons. Immunoreactivity to enkephalins, substance P, somatostatin, and galanin was expressed in single nerve cell bodies and nerve fibers except numerous substance P+ intraganglionic nerve fibers. Some of them were stained also for CGRP. Single neurons stained for tyroxine hydroxylase. Conclusions. Our results, compared with findings in other rodent species suggest the existence of interspecies differences in the morphology, cellular structure, and immunohistochemical properties of the head autonomic ganglia in mammals. [ABSTRACT FROM AUTHOR]

Published

2023

43. Increased Serum Met-enkephalin Level in Patients with Intrahepatic Cholestasis of Pregnancy.

Author

Çaypınar, Sema Süzen and Ekin, Murat

Subjects

ENKEPHALINS, CHOLESTASIS, PREGNANCY complications, GESTATIONAL age, BODY mass index

Abstract

Copyright of Bagcilar Medical Bulletin / Bağcılar Tıp Bülteni is the property of Galenos Yayinevi Tic. LTD. STI and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

44. Plasma concentration of thyroid hormones and corticosterone in hypothyroid rats and its correction with synthetic enkephalin.

Author

Garmaeva, D. V., Adushinov, D. S., Kuznetsov, A. I., and Mirvaliyev, F. S.

Subjects

*THYROID hormones, *CORTICOSTERONE, *RATS, *ENKEPHALINS, *OPIOID receptors, *HYPOTHYROIDISM, *THYROID hormone receptors

Abstract

The aim of the research is to study the possibility of correcting hypothyroidism with a synthetic analogue of the opioid leu-enkephalin (dalargin). The research was carried out on 70 white outbred male rats. The animals were simulated experimental hypothyroidism by the introduction of a synthetic thyreostatic which is called mercazolil. The positive long-term corrective effect of dalargin on the production of thyroid hormones has been shown. Dalargin lowers corticosterone level and protects the body from the damaging effects of stress. [ABSTRACT FROM AUTHOR]

Published

2022

45. Remote Ischemic Preconditioning Attenuates Ischemia-Reperfusion Injury Induced Reductions in Vascular Function through Release of Endogenous Opioids.

Author

Rosenberg AJ, Fernandez A, Moody AW, and Sprick JD

Abstract

Remote Ischemic Preconditioning (RIPC) is a therapy characterized by repeated bouts of limb ischemia and reperfusion. RIPC protects against ischemia-reperfusion injury (IRI), and preclinical studies suggest that this is mediated through release of endogenous opioids. We aimed to interrogate the role of endogenous opioids in RIPC-signaling in humans, using an arm model of IRI. We hypothesized that RIPC would attenuate IRI-induced reductions in brachial artery flow mediated dilation (FMD), and that this would be prevented by systemic opioid receptor blockade. 11 healthy adults (8M/3F, age=28±8y) completed three experimental visits in which IRI was induced via 20-min upper arm ischemia and 20-min reperfusion achieved via upper arm cuff inflation to 250mmHg. FMD was measured at rest and again following IRI. During the control condition, RIPC was not performed. During the RIPC condition, RIPC was performed on the contralateral arm via 4 cycles of 5-min cuff inflation (250mmHg) with 5-min reperfusion. During the opioid receptor blockade condition (Naloxone), RIPC was performed in the presence of systemic opioid receptor blockade via intranasal naloxone (4mg) which was administered during the first 5-min cycle of RIPC. The change in FMD from baseline vs post-IRI were compared between visits via a two-way repeated measures ANOVA (factor 1: time , factor 2, condition ) followed by Tukey post-hoc tests. IRI reduced FMD during the Control (Pre=6.1±2.4%, Post=3.5±2.8%, P<0.001) and Naloxone (Pre=6.6±2.7%, Post=3.5±1.9%, P<0.001) conditions but not during the RIPC condition (Pre=5.9±2.2%, Post=4.9±2.8%, P=0.14). These findings demonstrate that RIPC provides vascular protection from IRI in humans through an opioid-dependent mechanism.

Published

2025

46. N -Terminally Lipidated Sialorphin Analogs—Synthesis, Molecular Modeling, In Vitro Effect on Enkephalins Degradation by NEP and Treatment of Intestinal Inflammation in Mice.

Author

Sobocińska, Małgorzata, Fichna, Jakub, Giełdoń, Artur, Skowron, Piotr, and Kamysz, Elżbieta

Subjects

*ENKEPHALINS, *NEPRILYSIN, *INFLAMMATORY bowel diseases, *PEPTIDES, *STEARIC acid, *LUTEINIZING hormone releasing hormone

Abstract

Pharmacotherapy for inflammatory bowel disease (IBD) is difficult, and some patients do not respond to currently available treatments. Therefore, the discovery of novel anti-IBD agents is imperative. Our aim was the synthesis of lipidated analogs of sialorphin and the in vitro characterization of their effect on the degradation of Met-enkephalin by neutral endopeptidase (NEP). We also investigated in vivo whether the most active inhibitor (peptide VIII) selected in the in vitro studies could be a potential candidate for the treatment of colitis. Peptides were synthesized by the solid-phase method. Molecular modeling technique was used to explain the effect of fatty acid chain length in sialorphin analogs on the ligand–enzyme interactions. The anti-inflammatory effect was evaluated in the dextran sulphate sodium (DSS)-induced model of colitis in mice. Peptide VIII containing stearic acid turned out to be in vitro the strongest inhibitor of NEP. We have also shown that the length of the chain of stearic acid fits the size of the grove of NEP. Peptides VII and VIII exhibited in vivo similar anti-inflammatory activity. Our results suggest that lipidation of sialorphin molecule is a promising direction in the search for NEP inhibitors that protect enkephalins. [ABSTRACT FROM AUTHOR]

Published

2022

47. Laparoendoscopic two-site myomectomy (LETS-M) using conventional laparoscopic instruments and the glove-port technique.

Author

Wu, Pei-Chi, Sheu, Bor-Ching, Huang, Kuan-Ju, Huang, Su-Cheng, and Chang, Wen-Chun

Subjects

MYOMECTOMY, SURGICAL blood loss, LAPAROSCOPIC surgery, MUSCLE tumors, UTERINE tumors, RETROSPECTIVE studies, GYNECOLOGIC surgery, LAPAROSCOPY, ENKEPHALINS

Abstract

Purpose: To evaluate the perioperative outcome of laparoendoscopic two-site myomectomy (LETS-M).Methods: The medical records of 204 women receiving LETS-M in a tertiary referral center, including 183 surgeries performed by the experienced surgeon and 21 surgeries performed by 3 well-supervised trainees were retrospectively reviewed.Results: The age of the participants was 39.3 ± 6.4 years. The mean diameter of the largest myoma and the mean number of myomas were 8.5 ± 2.2 cm and 1.7 ± 1.1, respectively. Thirty-one (15%) operations removed more than 2 myomas larger than 5 cm in diameter. The mean weight of the myomas was 281.1 ± 183.1 g. The operation time was 97.6 ± 40.2 min, and the intraoperative blood loss was 99.3 ± 115.2 mL. There were 3 (1%) cases of excessive blood loss (more than 500 mL) and 2 (1%) of postoperative hematoma. The only significant difference between the experienced surgeon and trainees was the operation time (92.3 ± 32.2 min vs. 141.2 ± 54 min, p < .001), while the myoma number, myoma diameter, myoma weight, and intraoperative blood loss were not significantly different. The operation time did not differ among different myoma locations. In multivariate analysis, virginity, myoma number, more than 2 large myomas, and myoma size were independent variables for longer operation times. No patient experienced any major complications.Conclusion: LETS-M using conventional laparoscopic equipment is a minimally invasive surgical method that is safe, effective, and easy to learn for managing uterine myoma. It is useful to achieve a favorable perioperative outcome with acceptable operation time. [ABSTRACT FROM AUTHOR]

Published

2022

48. HDAC6 Inhibition Reverses Cisplatin-Induced Mechanical Hypersensitivity via Tonic Delta Opioid Receptor Signaling.

Author

Jixiang Zhang, Junigan, Jazzmine M., Trinh, Ronnie, Kavelaars, Annemieke, Heijnen, Cobi J., and Grace, Peter M.

Subjects

*OPIOID receptors, *ALLERGIES, *HISTONE deacetylase, *SENSORY neurons, *ENKEPHALINS, *CISPLATIN

Abstract

Peripheral neuropathic pain induced by the chemotherapeutic cisplatin can persist for months to years after treatment. Histone deacetylase 6 (HDAC6) inhibitors have therapeutic potential for cisplatin-induced neuropathic pain since they persistently reverse mechanical hypersensitivity and spontaneous pain in rodent models. Here, we investigated the mechanisms underlying reversal of mechanical hypersensitivity in male and female mice by a 2 week treatment with an HDAC6 inhibitor, administered 3 d after the last dose of cisplatin. Mechanical hypersensitivity in animals of both sexes treated with the HDAC6 inhibitor was temporarily reinstated by a single injection of the neutral opioid receptor antagonist 6b-naltrexol or the peripherally restricted opioid receptor antagonist naloxone methiodide. These results suggest that tonic peripheral opioid ligand-receptor signaling mediates reversal of cisplatin-induced mechanical hypersensitivity after treatment with an HDAC6 inhibitor. Pointing to a specific role for δ opioid receptors (DORs), Oprd1 expression was decreased in DRG neurons following cisplatin administration, but normalized after treatment with an HDAC6 inhibitor. Mechanical hypersensitivity was temporarily reinstated in both sexes by a single injection of the DOR antagonist naltrindole. Consistently, HDAC6 inhibition failed to reverse cisplatin-induced hypersensitivity when DORs were genetically deleted from advillin+ neurons. Mechanical hypersensitivity was also temporarily reinstated in both sexes by a single injection of a neutralizing antibody against the DOR ligand met-enkephalin. In conclusion, we reveal that treatment with an HDAC6 inhibitor induces tonic enkephalin-DOR signaling in peripheral sensory neurons to suppress mechanical hypersensitivity. [ABSTRACT FROM AUTHOR]

Published

2022

49. Fentanyl induces autism-like behaviours in mice by hypermethylation of the glutamate receptor gene Grin2b.

Author

Sheng, Zhihao, Liu, Qidong, Cheng, Chun, Li, Mengzhu, Barash, Jed, Kofke, W. Andrew, Shen, Yuan, and Xie, Zhongcong

Subjects

*GLUTAMIC acid, *NARCOTIC antagonists, *CELL receptors, *FENTANYL, *NALOXONE, *AUTISM, *ENKEPHALINS, *OPIOID analgesics, *MICE, *ANIMALS, *PHARMACODYNAMICS

Abstract

Background: Environmental factors contribute to autism spectrum disorder. Fentanyl, one of the most widely used opioid analgesics in anaesthesia, can induce neurotoxicity, but its role in autism remains unknown. We determined whether fentanyl induced autism-like behaviours in young mice and the underlying mechanisms.Methods: Young male and female mice received fentanyl at postnatal days 6, 8, and 10, and performed behavioural tests, including three-chamber social preference, elevated plus maze, grooming behaviour, and open-field test, from postnatal days 30-32. Expression of Grin2b, the gene encoding the GluN2B subunit of the N-methyl-d-aspartate receptor, was assessed in the anterior cingulate cortex of male mice using fluorescence in situ hybridisation histochemistry. We used bisulfite target sequencing to determine Grin2b hypermethylation sites after fentanyl treatment. In the specific activation and rescue experiments, we injected the mu opioid receptor agonist [D-Ala,2 N-MePhe,4 Gly-ol]-enkephalin (DAMGO) or Grin2b overexpression lentivirus into the anterior cingulate cortex of male mice.Results: Fentanyl induced autism-like behaviours in both young male and female mice, and downregulated Grin2b expression (0.49-fold [0.08] vs 1.00-fold [0.09]; P<0.01) and GluN2B protein amounts (0.38-fold [0.07] vs 1.00-fold [0.12]; P<0.01) in the anterior cingulate cortex through hypermethylation of Grin2b. The mu-opioid receptor antagonist naloxone and overexpression of Grin2b in anterior cingulate cortex attenuated the fentanyl-induced effects, whereas DAMGO injection into the anterior cingulate cortex induced autism-like behaviours.Conclusions: These data suggest that fentanyl induces autism-like behaviours in young mice via an epigenetic mechanism. Further research is required to determine possible clinical relevance to autism risk. [ABSTRACT FROM AUTHOR]

Published

2022

50. Enkephalin loaded and RGD decorated PLGA–poloxamer nanoparticles for effective targeting in cancer cells.

Author

Kaur, Sarabjit, Pandey, Satish K., Sharma, Deepika, Sharma, Rohit K., and Wangoo, Nishima

Subjects

*LIVER cells, *NANOMEDICINE, *CANCER cells, *TARGETED drug delivery, *NANOPARTICLES, *ENKEPHALINS, *PEPTIDES, *TUMOR markers

Abstract

Enkephalins have been shown to retard cell proliferation in various human cancer cell lines, including breast, soft tissue, gastrointestinal, brain, pancreatic, and liver cell cultures. In this study, we have synthesized polymeric PLGA [poly (lactide-co-glycolic acid)]–poloxamer nanoparticles loaded with enkephalins in order to achieve a consistent release of these neuropeptides. In order to provide targeting abilities toward cancerous cells, these nanoparticles were functionalized with RGD (Arg-Gly-Asp-amide, a cancer cell marker). The synthesized nanoparticles (NPs) were further thoroughly characterized for biological activity including cytotoxicity, anticancer activity as well as cancer cell uptake abilities. Interestingly, it was observed that the fluorescent marker containing cancer cell-targeting peptide (RGD) conjugated nano-formulation(s) exhibited good uptake and internalization into cancer cells. The results indicate that the developed enkephalin-RGD-PLGA nanoparticles can serve as suitable targeted drug delivery vehicle/system for existing conventional drugs as well as in increasing the efficacy of drugs. [ABSTRACT FROM AUTHOR]

Published

2022