Mefway (¹⁸F)

Mefway (¹⁸F)
Clinical data
Pregnancy; category	N/A;
ATC code	none;
Legal status
Legal status	Research compound;
Identifiers
	IUPAC name 4-[(18F)fluoromethyl]-N-{2-[4-(2-methoxyphenyl)piperazin-1-yl]ethyl}-N-(pyridin-2-yl)cyclohexane-1-carboxamide;
JSmol)	Interactive image;
	SMILES COC1=CC=CC=C1N2CCN(CC2)CCN(C3=CC=CC=N3)C(=O)C4CCC(CC4)C[18F];
	InChI InChI=1S/C26H35FN4O2/c1-33-24-7-3-2-6-23(24)30-17-14-29(15-18-30)16-19-31(25-8-4-5-13-28-25)26(32)22-11-9-21(20-27)10-12-22/h2-8,13,21-22H,9-12,14-20H2,1H3/i27-1; Key:BQGLPDFQLBNUGU-FMLNDMEQSA-N;

Mefway is a serotonin

radiotracer.^[1]

Chemistry

Mefway is closely related to the research compound

WAY-100,635. The compound adds a fluoromethyl group to the cyclohexyl ring of WAY-100,635 and it is effectively prepared with automation module.^[2]

There are two

isomers with regard to the cyclohexane ring, of which the trans conformation has the higher 5-HT_1A specificity.^[3]

Animal PET studies

In one study the uptake and retention of mefway (¹⁸F) was found to be similar to that found for ¹¹C-WAY-100,635. Head-to-head comparison of mefway (¹⁸F) and ¹¹C-WAY-100,635 have been evaluated. Since ¹¹C-WAY-100,635 is the current 'gold standard' and difficult to synthesize, a suitable fluorine-18 replacement as in mefway is highly desired.^[4] In addition, mefway (¹⁸F) showed comparable brain uptake and the target-to-reference ratios compared to fcway(¹⁸F)^[5]

The ability to separately measure dissociation constant, K_D and receptor density Bmax has been shown to be of potential value rather than simply comparing binding potential, BP_ND. Multiple injection mefway PET experiments can be used for the in-vivo measurement of 5-HT_1A receptor density.^[6]

Imaging studies of mefway on in vivo and ex vivo rat brains indicate that the substance binds to the known 5-HT_1A receptor regions including the dorsal raphe. These findings support that the dorsal raphe is measurable in rat PET studies.^[7] Mefway (¹⁸F) undergoes in vivo defluorination in rodent brain and this phenomenon was effectively suppressed by cytochrome P450 inhibitor (i.e. fluconazole).^[8] Animal models of Parkinson's disease and the acute physical stress model exhibited significant decrement of binding potential in the hippocampus ^[9]^[10]

Human PET studies

First-in-human studies have shown in vivo stability of mefway (¹⁸F) and its localization to 5-HT_1A receptor-rich regions in the human brain, including the

raphe nucleus.^[11] Mefway (¹⁸F) is highly selective for the human serotonin 5-HT_1A receptor and may therefore may be used to quantify serotonin 5-HT_1A receptor distribution in brain regions for the study of various central nervous system disorders.^[12]

References

PMID 17015907
.

PMID 24285234
.

PMID 21741252
.

PMID 21484878
.

S2CID 23706884
.

PMID 22472611
.

PMID 23504990
.

S2CID 5266871
.

PMID 25064461
.

PMID 24771590
.

PMID 25453045
.

PMID 26509362
.

Retrieved from "https://en.wikipedia.org/w/index.php?title=Mefway_(18F)&oldid=1120553909"

[1] PMID 17015907
.

[2] PMID 24285234
.

[3] PMID 21741252
.

[4] PMID 21484878
.

[5] S2CID 23706884
.

[6] PMID 22472611
.

[7] PMID 23504990
.

[8] S2CID 5266871
.

[9] PMID 25064461
.

[10] PMID 24771590
.

[11] PMID 25453045
.

[12] PMID 26509362
.

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