Tetracyclic antidepressant

Tetracyclic antidepressants (TeCAs) are a class of antidepressants that were first introduced in the 1970s. They are named after their tetracyclic chemical structure, containing four rings of atoms, and are closely related to the tricyclic antidepressants (TCAs), which contain three rings of atoms.

List of TeCAs

Maprotiline (Ludiomil) – can also be classified as a TCA and grouped with the secondary amines
Mianserin (Tolvon)
Mirtazapine (Remeron)
Setiptiline (Tecipul)

Drugs that contain four rings not all fused together but are sometimes still classified as TeCAs include:

Amoxapine (Asendin) – often classified as a TCA and grouped with the secondary amines
Quetiapine (Seroquel) - an atypical antipsychotic sometimes used as an adjunct antidepressant

Benzoctamine (Tacitin) – a tetracyclic compound and is closely related to maprotiline, with the two compounds differing only in the length of their side chain, but benzoctamine is not used as an antidepressant and is instead used as an anxiolytic
Loxapine (Adasuve, Loxitane) – a typical antipsychotic that produces amoxapine as a major metabolite and is said to have antidepressant effects, but it is not usually regarded as a TeCA

Drugs that contain four rings not all fused together but could still be classified as tetracyclic include:

Mazindol (Mazanor, Sanorex) – a monoamine reuptake inhibitor used as an appetite suppressant and with potential antidepressant effects, but not classified as a TeCA

Drugs that contain four rings not all fused together but could still be classified as tetracyclic include:

TeCAs have diverse pharmacology and differ from TCAs in a number of ways. With the exception of amoxapine, TeCAs do not inhibit the reuptake of serotonin Template:Citation needed. However, aside from mirtazapine, they do inhibit the reuptake of norepinephrine Template:Citation needed. TeCAs block the serotonin 5-HT₂ receptors similarly to TCAs. Besides mirtazapine, they also block the α₁-adrenergic receptor Template:Citation needed. Conversely, whereas TCAs have relatively low affinity for the α₂-adrenergic receptor, mianserin and mirtazapine potently antagonize this receptor, and this action is thought to be involved in their antidepressant effectsTemplate:Citation needed. TeCAs block the histamine H₁ receptor similarly to the TCAs, but tend to be even stronger antihistamines than TCAsTemplate:Citation needed. On the other hand, in contrast to almost all TCAs, TeCAs have only low affinity for the muscarinic acetylcholine receptors, and for this reason, are associated with few or no anticholinergic side effects Template:Citation needed. Mianserin and mirtazapine are far less toxic than TCAs in overdose.<ref>Template:Cite journal</ref><ref>Template:Cite journal</ref>

The binding profiles of various TeCAs in terms of their affinities (Template:Abbr, Template:Abbr) for various receptors and transporters are as follows:<ref name="PDSP">Template:Cite web</ref>


Compound	Template:Abbrlink	Template:Abbrlink	Template:Abbrlink	5-HT_1A	5-HT_2A	5-HT_2B	5-HT_2C	5-HT₃	5-HT₆	5-HT₇	α₁	α₂	D₂	H₁	H₂	Template:Abbrlink
Amoxapine	58	16	4,310	Template:Abbr	0.5	Template:Abbr	2.0	Template:Abbr	6.0–50	41	50	2,600	3.6–160	7.9–25	Template:Abbr	1,000
Maprotiline	5,800	11–12	1,000	Template:Abbr	51	Template:Abbr	122	ND	Template:Abbr	50	90	9,400	350–665	0.79–2.0	776	570
Mianserin	4,000	71	9,400	400–2,600	1.6–20	1.6–55	0.63–6.5	5.8–300	55–81	48–56	34	3.8–73	≥2,100	0.30–1.7	437	820
Mirtazapine	>10,000	≥4,600	>10,000	≥3,330	6.3–69	200	8.9–39	7.9	Template:Abbr	265	316–1,815	18–88	>5,454	0.14–1.6	>10,000	670
Setiptiline	>10,000	220	>10,000	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr	24	Template:Abbr	Template:Abbr	Template:Abbr	Template:Abbr
Values are Template:Abbr (Template:Abbr). The smaller the value, the more strongly the drug binds to the site. For assay species and references, see the individual drug articles. Most but not all values are for human proteins.

The TeCAs act as antagonists or inverse agonists of the receptors and as inhibitors of the transporters.