Sobetirome prodrug esters with enhanced blood–brain barrier permeability

Placzek, Andrew T.; Ferrara, Skylar J.; Hartley, Meredith D.; Sanford-Crane, Hannah; Meinig, J. Matthew; Scanlan, Thomas S.

doi:10.1016/j.bmc.2016.09.038

Cited by 41 publications

(37 citation statements)

References 43 publications

(50 reference statements)

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“…Following prodrug 6 , the next highest brain/serum ratio is that for prodrug 3 with a value of 0.5, which is ~13-fold higher than the brain/serum ratio of sobetirome, and ~7-fold higher than previously reported 2 . 18 From this biodistribution study, it appears that the prodrugs which can undergo this intramolecular ester-to-amide rearrangement of their promoities display the desired PK-ADME properties for CNS distribution, suggesting that amide prodrugs of sobetirome are the pharmacologically active species of interest. This was confirmed by analyzing prodrug 3 synthesized as an ester (3a) side-by-side with the deliberately prepared amide of 3 (3b) , which gave statistically identical brain levels and brain/serum ratios at equimolar doses (see Supporting Information).…”

Section: Resultsmentioning

confidence: 92%

“…In line with the recently reported successful application of an ethanolamine-based ester prodrug of sobetirome 18 and ethanolamine-based ester prodrugs of dexibuprofen, 19, 20 a drug with structural similarities to sobetirome, a new series of ethanolamine-derived prodrugs of sobetirome were synthesized in an effort to expand upon these findings and improve their pharmacokinetic properties regarding CNS distribution (Scheme 1). Derivatization of the ethanolamine moiety within the series explores varying aspects of steric and electronic parameters with subtle differences in lipophilicity.…”

Section: Resultsmentioning

confidence: 95%

“…22 Generation of the acid chloride of phenol-benzylated sobetirome (Scheme 1, left) is accomplished by treating phenol-benzylated sobetirome with oxalyl chloride in the presence of a catalytic amount of DMF. 18, 23 Coupling of the phenol-protected sobetirome acid chloride with N -protected amino alcohols occurs readily in the presence of DMAP in heated THF. Global deprotection of benzyl ether, N -Cbz, and N -benzyl protected fragments follows with treatment of the protected precursors with 10% Pd/C and triethylsilane in THF/MeOH.…”

Section: Resultsmentioning

confidence: 99%

“…Prodrug 3 delivers 3.6-fold more sobetirome to the brain than an equimolar dose of unmodified sobetirome, and its levels are 1.7-fold higher than the previously reported ethanolamine-derived prodrug of sobetirome 2 in a side-by-side comparison. 18 In addition to BBB penetration, an ideal prodrug would be stable in blood and limit exposure of the parent drug in peripheral tissues. Most prodrugs in this series displayed higher brain/serum ratios than the control dose of sobetirome.…”

Section: Resultsmentioning

confidence: 99%

“…Recently, an in vivo study evaluating the brain exposure of ester-based prodrugs of sobetirome confirmed this strategy to be effective. 18 In this study, a particular ester derivative, an ethanolamino ester (2) , was found to have the greatest CNS penetration with minimized peripheral exposure of the parent drug. Here we report a new series of prodrugs that feature improved CNS distribution compared to the originally reported ethanolamino ester and, in the process, it was discovered that these ester promoieties undergo an intramolecular rearrangement to form the corresponding amides, which were found to be the pharmacologically active forms of the prodrugs.…”

Section: Introductionmentioning

confidence: 86%

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Ester-to-amide rearrangement of ethanolamine-derived prodrugs of sobetirome with increased blood-brain barrier penetration

Ferrara

Meinig

Placzek

et al. 2017

Bioorganic & Medicinal Chemistry

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Current therapeutic options for treating demyelinating disorders such as multiple sclerosis (MS) do not stimulate myelin repair, thus creating a clinical need for therapeutic agents that address axonal remyelination. Thyroid hormone is known to play an important role in promoting developmental myelination and repair, and CNS permeable thyromimetic agents could offer an increased therapeutic index compared to endogenous thyroid hormone. Sobetirome is a clinical stage thyromimetic that has been shown to have promising activity in preclinical models related to MS and X-linked adrenoleukodystrophy (X-ALD), a genetic disease that involves demyelination. Here we report a new series of sobetirome prodrugs containing ethanolamine-based promoieties that were found to undergo an intramolecular O,N acyl migration to form the pharmacologically relevant amide species. Several of these systemically administered prodrugs deliver more sobetirome to the brain compared to unmodified sobetirome. Pharmacokinetic properties of the parent drug sobetirome and amidoalcohol prodrug 3 are described and prodrug 3 was found to be more potent than sobetirome in target engagement in the brain from systemic dosing.

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Section: Resultsmentioning

confidence: 92%

Section: Resultsmentioning

confidence: 95%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 86%

See 3 more Smart Citations

Ester-to-amide rearrangement of ethanolamine-derived prodrugs of sobetirome with increased blood-brain barrier penetration

Ferrara

Meinig

Placzek

et al. 2017

Bioorganic & Medicinal Chemistry

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Discovery and Characterization of Novel Naphthalimide Analogs as Potent Multitargeted Directed Ligands against Alzheimer's Disease

Gao

Chapman

2020

Drug Development Research

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Current therapeutic drugs for Alzheimer's disease (AD) can only offer limited symptomatic benefits and do not halt disease progression. Multitargeted directed ligands (MTDLs) have been considered to be a feasible way to treat AD due to the multiple neuropathological processes in AD. Previous studies proposed that compounds containing two aromatic groups connected by a carbon chain should act as effective amyloid β (Aβ) aggregation inhibitors although the optimal length of the carbon chain has not been explored. In the current study, a series of naphthalimide analogs were designed and synthesized based on the proposed structure and multiple bioactivities beneficial to the AD treatment were reported. In vitro studies showed that compound 8, which has two aromatic groups connected by a two‐carbon chain, exhibited significant inhibition of Aβ aggregation through the prevention of elongation and association of Aβ fibril growth. Furthermore, this compound also displayed antioxidative activities and neuroprotection from Aβ monomer induced toxicity in primary cortical neurons. The results of the present study highlight a novel naphthalimide‐based compound 8 as a promising MTDL against AD. Its structural elements can be further explored for enhanced therapeutic capabilities.

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Imidazo[1,2‐α] azine's esters increase selectivity and anti‐inflammatory activity in microglial cells

Guerrero‐González,

Campos‐Aldrete,

Meraz‐Ríos

2024

Journal of Heterocyclic Chem

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Chronic neuroinflammation is crucial in many neurodegenerative diseases, including AD. Neuroinflammation activates microglia, the CNS's central effector cells, and immune cells. Toxins and neuroinflammatory reactions can kill or damage neurons, activating microglial cells. Inflammatory mediators from activated microglia can kill neurons like cytokines, chemokines, reactive oxygen species, and reactive nitrogen species. Imidazo[1,2‐α]azines with different acid groups in position two of the heterocycle system were synthesized and tested as anti‐inflammatory and cell immunomodulators. We measured the ability of human neuroblastoma (SHSY‐5Y) and microglial (HMC3) cell lines to decrease PGE2 production under pro‐inflammatory conditions. All derivatives reduced PGE2 production. Inhibitory profiles indicate that compounds 8a and 8b are more effective and potent than 9a and 9b, indicating a steric effect of carboxyphenyl on imidazo[1,2‐α]azines, reducing their potency. However, imidazo[1,2α]pyrimidines (8b and 9b) with nitrogen at position 8 were less effective than those observed by other groups (8a, 9a, and 10a). imidazo[1,2‐α]pyrimidines are more polar due to nitrogen at position 8. The synthetically derivative imidazo[1,2‐α]pyridines decreased PGE2 formation in vitro on neural cells, microglia (HMC3), and neuroblastoma (SH‐SY5Y) cells, proving that they are more effective than imidazo[1,2‐α]pyrimidines. Two product esters selectively reduced HMC3 microglial cell PGE2 production. This finding may help develop neurodegenerative disease anti‐inflammatories.

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Sobetirome prodrug esters with enhanced blood–brain barrier permeability

Cited by 41 publications

References 43 publications

Ester-to-amide rearrangement of ethanolamine-derived prodrugs of sobetirome with increased blood-brain barrier penetration

Ester-to-amide rearrangement of ethanolamine-derived prodrugs of sobetirome with increased blood-brain barrier penetration

Discovery and Characterization of Novel Naphthalimide Analogs as Potent Multitargeted Directed Ligands against Alzheimer's Disease

Imidazo[1,2‐α] azine's esters increase selectivity and anti‐inflammatory activity in microglial cells

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