Bench-top to clinical therapies: A review of melanocortin ligands from 1954 to 2016

Ericson, Mark D.; Lensing, Cody J.; Fleming, Katlyn A.; Schlasner, Katherine N.; Doering, Skye R.; Haskell‐Luevano, Carrie

doi:10.1016/j.bbadis.2017.03.020

Cited by 67 publications

(100 citation statements)

References 290 publications

(498 reference statements)

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“…In addition to melanocortins, the naturally occurring agonists of MCR, many pharmacologic agonists have been synthesized and tested for MCR subtype specificity, for longer half-lives than the rapidly degraded melanocortin peptides, and for reduction in steroidogenic or other side effects [ 4 , 11 , 35 ] (reviews). These include agents targeted to allosteric (extracellular), orthosteric (transmembrane, where ACTH and melanocortins bind) and signal transduction (intracellular) sites on MCR.…”

Section: Melanocortin Receptor Signalingmentioning

confidence: 99%

Melanocortins, Melanocortin Receptors and Multiple Sclerosis

Lisak

Benjamins

2017

Brain Sciences

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The melanocortins and their receptors have been extensively investigated for their roles in the hypothalamo-pituitary-adrenal axis, but to a lesser extent in immune cells and in the nervous system outside the hypothalamic axis. This review discusses corticosteroid dependent and independent effects of melanocortins on the peripheral immune system, central nervous system (CNS) effects mediated through neuronal regulation of immune system function, and direct effects on endogenous cells in the CNS. We have focused on the expression and function of melanocortin receptors in oligodendroglia (OL), the myelin producing cells of the CNS, with the goal of identifying new therapeutic approaches to decrease CNS damage in multiple sclerosis as well as to promote repair. It is clear that melanocortin signaling through their receptors in the CNS has potential for neuroprotection and repair in diseases like MS. Effects of melanocortins on the immune system by direct effects on the circulating cells (lymphocytes and monocytes) and by signaling through CNS cells in regions lacking a mature blood brain barrier are clear. However, additional studies are needed to develop highly effective MCR targeted therapies that directly affect endogenous cells of the CNS, particularly OL, their progenitors and neurons.

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Section: Melanocortin Receptor Signalingmentioning

confidence: 99%

Melanocortins, Melanocortin Receptors and Multiple Sclerosis

Lisak

Benjamins

2017

Brain Sciences

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“…The important role of melanocortin‐4 receptors (MC 4 R) in energy homeostasis, sexual functions, neuroprotection, and neurogenesis (Wikberg and Mutulis, ; Tao, ) has made these G protein‐coupled receptors attractive drug targets in the central nervous system (CNS). Despite being very promising targets for several clinical trials, there is only a limited number of therapeutically approved drugs for MC 4 Rs (Ericson et al, ), mainly because the signal transduction of MC 4 Rs is subject to considerable complexity including conformational adjustments, oligomerization, and effects of different modulators (Biebermann et al, ; Kopanchuk et al, ; Müller, Berkmann, Scheerer, Biebermann, and Kleinau, ). There is increasing evidence that MC 4 R can form homo‐ and heterodimers or higher‐order oligomers (Elsner et al, ; Kopanchuk et al, ; Nickolls and Maki, ; Rediger et al, ; Chapman and Findlay, ) and the ligand binding within MC 4 R homodimers is governed by asymmetric regulation of co‐operative‐binding sites (Kopanchuk et al, , ).…”

Section: Introductionmentioning

confidence: 99%

The constitutive activity of melanocortin‐4 receptors in cAMP pathway is allosterically modulated by zinc and copper ions

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Veikšina

Tahk

et al. 2019

Journal of Neurochemistry

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Melanocortin‐4 receptors (MC4R) are unique among G‐protein‐coupled receptors (GPCRs) as they have endogenous ligands that can exhibit inverse agonistic properties in the case of elevated basal activity. It is known that the constitutive activity of GPCRs strongly affects the ligand‐dependent physiological responses, but little is known about these regulatory mechanisms. Since several metal ions have been shown to be important modulators of the signal transduction of GPCRs, we hypothesized that metal ions regulate the basal activity of MC4Rs. Implementation of a fluorescence anisotropy assay and novel redshifted fluorescent peptides enabled kinetic characterization of ligand binding to MC4R expressed on budded baculoviruses. We show that Ca2+ is required for high‐affinity ligand binding, but Zn2+ and Cu2+ in the presence of Ca2+ behave as negative allosteric modulators of ligand binding to MC4R. FRET‐based cAMP biosensor was used to measure the activation of MC4R stably expressed in CHO‐K1 cells. At low micromolar concentrations, Zn2+ caused MC4R‐dependent activation of the cAMP pathway, whereas Cu2+ reduced the activity of MC4R even below the basal level. These findings indicate that at physiologically relevant concentrations can Zn2+ and Cu2+ function as MC4R agonists or inverse agonists, respectively. This means that depending on the level of constitutive activity induced by Zn2+ ions, the pharmacological effect of orthosteric ligands of MC4R can be switched from a partial to an inverse agonist. Open Science Badges This article has received a badge for *Open Materials* because it provided all relevant information to reproduce the study in the manuscript. More information about the Open Science badges can be found at https://cos.io/our-services/open-science-badges/.

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“…Since melanocortins possess the ability to be pro-resolving molecules, they are attractive options for patients with inflammatory diseases. Synthetic melanocortins have been developed that are characterized by enhanced potency, improved duration of activity compared to endogenous melanocortins, and resistance to proteolytic activity 35. In addition, selective agonist peptides, selective antagonist peptides, and small-molecule ligands have been and are being developed in order to target particular melano-cortin receptors to exert control in particular pathologies; for example, MC 4 R has been the frequent target of development of agonists because of the association between this receptor and obesity 35…”

Section: Discussionmentioning

confidence: 99%

Repository corticotropin injection as adjunctive therapy in patients with rheumatoid arthritis who have failed previous therapies with at least three different modes of action

Gillis¹,

Crane²,

Hinkle³

et al. 2017

OARRR

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ObjectiveMany types of treatment are available for patients with rheumatoid arthritis (RA), however, some patients fail to achieve remission. This report aims to determine the safety and efficacy of using repository corticotropin injection (RCI) as an adjunctive therapy in patients with RA refractory to at least three therapeutics with different mechanisms of action.MethodIn this open-label, interventional, single-group study, patients received 80 U RCI twice weekly via subcutaneous injection over 12 weeks. Changes in the Ritchie–Camp Articular Index and health assessment questionnaire scores were monitored for changes from baseline measures.ResultsEight patients were enrolled and consisted of seven females and one male with an average age of 64.6 years and disease duration of 20.9 years. Use of RCI resulted in significant improvement in swollen and tender joint counts. The disease activity score 28 and the physician and patient visual analog scale scores were significantly reduced at treatment week 12. The reduction in health assessment questionnaire scores did not reach statistical significance after RCI treatment. Once RCI therapy was discontinued, all improvements in disease activity score 28, physician and patient visual analog scale, and tender and swollen joint counts achieved during treatment were lost by the week 16 follow-up visit.ConclusionWhile larger clinical trials are necessary to further confirm the efficacy of RCI in patients with refractory RA, the response of patients with refractory RA in this study suggests that RCI can be an effective add-on therapy for patients who have exhausted several classes of treatments. Furthermore, this study suggests that RCI has an alternative mode of action, compared to other available antirheumatic drugs.

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Bench-top to clinical therapies: A review of melanocortin ligands from 1954 to 2016

Cited by 67 publications

References 290 publications

Melanocortins, Melanocortin Receptors and Multiple Sclerosis

Melanocortins, Melanocortin Receptors and Multiple Sclerosis

The constitutive activity of melanocortin‐4 receptors in cAMP pathway is allosterically modulated by zinc and copper ions

Repository corticotropin injection as adjunctive therapy in patients with rheumatoid arthritis who have failed previous therapies with at least three different modes of action

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