The topic of what qualifies as psychedelic is a massive can of worms and I don't think it's really in the spirit of this thread to open it i.e. if well known drugs like ketamine and saliva are what the OP considers to be psychedelic they wouldn't have asked the question. 5HT2a agonism is a practical criterion that helps focus discussion, and even though there's lots of experiential variability between them, there's no doubt that to most people most current psychedelics that agonize the receptor feel more alike than most any of the class does compared to dissociatives and CB-1 agonists (granted, aMT and 5-MeO-DMT are odd, but that probably has a lot to do with their respective monoamine releasing capabilities and highly disproportionate 5HT-1a agonism). I'm certain even rats trained to discriminate DOM won't press a lever if you give them a dissociative or CB-1 agonist or serotonin, yet we know they do mistake LSD for DOM. Hell, rats don't even mistake 5-MeO-DMT for DOM. If even rodents can acknowledge the differences and similarities I don't think we should pretend jwh-018 is anything like ayahuasca just because for some people there is some narrow overlap subjectively speaking.
Serotonin would be, but it doesn't cross the blood-brain barrier.
All the examples mentioned in the OP are 5HT2a agonists (in general). It's probably safe to assume the author already knew about dissociatives and deliriants. 5HT2a agonists, NMDA antagonists, and acetylcholine inhibitors are all definitely hallucinogens, however.
