Anxiety disorders are among the most common mental health conditions in the United States, and for many people, it takes concentrated effort to treat them. About one-third of U.S. adults will experience an anxiety disorder at some point in their lives.
There are many variations in how anxiety manifests and the ways to treat it. Some people improve rapidly once they implement a skill or medication, while others improve steadily over time, and still others try many approaches without finding sustained relief.
Anxiety disorders are chronic conditions shaped by overlapping factors, such as genetic predisposition, early life experiences, and cumulative stress. Because no single cause drives them, treatment response varies, as only 60 to 70 percent of patients respond, and of those, up to two-thirds experience relapse.
Harvard Health explains that the autonomic nervous system, which governs the fight-or-flight response, can generate physical symptoms. This includes headaches, nausea, and shortness of breath, during both acute anxiety and chronic anxiety, and especially in anxiety disorders.
Psychological and environmental factors, such as learned fear responses, financial strain, and relationship difficulties, can also worsen anxiety, keeping the nervous system in a cyclical state of alert that's hard to escape.
It’s also important to set realistic expectations. For some people, “better” doesn’t look like a full elimination of anxiety. It may be a meaningful reduction in symptoms that allows someone to live their daily life with improved function and less distress.
Sometimes treatments don’t work as the patient hopes because other factors may be at play. Anxiety disorders frequently co-occur with major depression, alcohol and other substance-use disorders, and personality disorders. Rule out physical conditions like thyroid, cardiac, or respiratory, as well as substance use or withdrawal, since these can mimic or worsen anxiety symptoms.
Mayo Clinic recommends having a doctor rule out physical causes before assuming it’s anxiety. Treating the wrong problem means treating symptoms that won’t go away.
Chronic stress can also alter how the nervous system responds, making it harder to return to the calm baseline, even when the original stressor is gone. Unresolved trauma is another common driver, as standard anxiety treatments don’t always reach it. Beyond diagnosis, it could also come down to medication mismatch, a poor therapist fit, inconsistent attendance or practice, sleep deprivation, and alcohol or drug dependency, which may limit how much progress is possible.
A 2024 Delphi-method consensus published in World Psychiatry established the first internationally agreed operational criteria: TR-AD is defined by failure to respond to at least one adequate trial of a first-line pharmacological treatment (SSRI or SNRI) and/or one evidence-based psychotherapeutic intervention (such as CBT), at an adequate dose and duration, with anxiety severity remaining above a clinically meaningful threshold. The panel also outlined a staging model to reflect degrees of resistance. This allows professionals to recognize this pattern and use those criteria as a framework for stepping up care.
Anxiety may be considered treatment-resistant when symptoms remain at a clinically significant level despite at least one adequate trial each of a first-line medication and a first-line psychotherapy (e.g., 8+ weeks at an effective dose, or a full course of CBT), rather than simply "symptoms haven't gone away."
Signs worth flagging for further evaluation include:
Research suggests that clinical trials for anxiety disorders show remission rates of only 25 to 35 percent*, meaning that even with adequate treatment, a proportion of people don't achieve full relief.
*These figures include OCD and PTSD, which have since been reclassified as separate diagnostic categories in DSM-5. They're still relevant here because both conditions share significant anxiety symptoms and were treated as anxiety disorders in the research this estimate draws on, but their inclusion means remission rates may vary depending on which specific disorders are examined.
One of the more significant shifts in mental health research over the past two decades has been a renewed scientific interest in psychedelic-assisted therapy. Institutions, including the Johns Hopkins Center for Psychedelic and Consciousness Research, have been conducting rigorous clinical trials examining whether certain compounds, in carefully controlled therapeutic settings, may offer relief for conditions where existing therapies often fall short. This research is still in its early stages
Psilocybin has been the most studied compound in this context. In a randomized double-blind trial at Johns Hopkins, Griffiths and colleagues found that high-dose psilocybin with psychological support produced substantial and sustained decreases in anxiety and depression in cancer patients with life-threatening diagnoses. Roughly 70 to 80 percent of participants maintained clinically significant improvements at six months.
A parallel trial by Ross, Bossis, and colleagues at NYU found similarly rapid and sustained symptom reduction in a study in which participants received both the treatment and a placebo, in random order. These were patients with existential distress tied to terminal illness, not generalized anxiety.
Neuroimaging research suggests that psilocybin may modulate the brain's default mode network, which is associated with rumination and negative mood loops. Some researchers hypothesize that this could support a form of emotional flexibility that is difficult to achieve through conventional therapy alone, though the underlying mechanism remains poorly understood.
Johns Hopkins Medicine has reported improvements in quality of life, sense of meaning, optimism, and acceptance of death among participants in its studies. These findings are notable but preliminary and are based on small samples and still require replication before broader conclusions can be drawn.
MDMA (3,4-Methylenedioxymethamphetamine) has been investigated for PTSD-related anxiety through two Phase 3 trials, which found significant reductions in PTSD symptoms compared to placebo with therapy. In the first trial, 67 percent of participants in the MDMA group no longer met diagnostic criteria for PTSD after three sessions, compared with 32 percent of the placebo group.
The proposed mechanism differs from psilocybin's in that MDMA is thought to enhance fear extinction and modulate fear memory reconsolidation through its combined effects. Researchers hypothesize this creates a window of reduced fear and increased psychological openness that allows patients to engage more fully with trauma-focused therapy.
Ketamine and its derivative, esketamine, are the only compounds in this category that are currently FDA-cleared, though their clearance is specifically for treatment-resistant depression rather than anxiety. SPRAVATO® (prescription nasal spray esketamine) was first approved in 2019 for adults with treatment-resistant depression who had not responded to at least two other antidepressants; in January 2025, the FDA expanded that approval to allow it as a standalone treatment.
Ketamine's antidepressant effects are thought to be mediated by a glutamate surge that initiates a cascade leading to synaptogenesis and reversal of stress-related synaptic loss, particularly in the prefrontal cortex. Research has noted that ketamine’s anti-depressant effects can kick in as soon as four hours after an intravenous dose is administered.
Anxiety that persists despite treatment is usually a signal to take a closer look at what can be done. That means ruling out physical causes, checking for co-occurring conditions like depression or substance use, confirming medications and boses are adequate, and asking whether the therapy modality fits your needs.
Psilocybin, MDMA, and ketamine are in an active area of research and may be a potential path to treatment for those who suffer from treatment-resistant depression, PTSD, and existential distress. Anyone considering these routes should pursue them through a licensed clinical trial or legally sanctioned treatment setting.