31 The relatively favorable side-effect
profile of pregabalin makes it another useful treatment option in GAD.7 Current treatment guidelines recommend a dose range of 150 to 600 mg/day for adult patients.9 Antipsychotic agents have also been studied as monotherapy in GAD. There is evidence that the atypical antipsychotic quetiapine is more effective than placebo in improving Inhibitors,research,lifescience,medical clinical response and remission rates in patients with GAD.32,33 However, risk:benefit ratio remains a concern given the possibility of adverse events such as metabolic syndrome. On the other hand, these agents may have a role to play in treatment-selleck chemicals refractory patients, with evidence suggesting that various antipsychotic agents may be beneficial as augmentation strategies in those with treatment-refractory
GAD.34,35 Indeed, in clinical practice a significant proportion of patients with GAD fail either to receive appropriate therapy or to respond to first-line pharmacotherapy. An immediate Inhibitors,research,lifescience,medical step in the management of the latter group of patients is to ensure that diagnosis is correct, that psychiatric and medical comorbidity has not been overlooked, and that the trial is of sufficient duration and dosage.36 Next steps include switching to a different agent, or augmentation.8,9,16,37 There are few switch studies in GAD, but the literature on depression suggests that a different SSRI or an agent from a different class Inhibitors,research,lifescience,medical might be Inhibitors,research,lifescience,medical useful in refractory cases. Pharmacotherapy augmentation strategies include the addition to SSRI/SNRI treatment of buspirone,29 pregabalin,38 or low doses of atypical antipsychotics.35,34 Although data on the value of combined pharmacotherapy and psychotherapy in GAD is surprisingly limited,39 psychotherapy
augmentation strategies may also be considered. In addition to the glaring absence of data on how best to approach the treatment-refractory GAD patient, a number of other gaps in the literature deserve to be highlighted. First, most treatment data on GAD derive from trials of GAD patients without comorbidity recruited by academic centers; there are few data Inhibitors,research,lifescience,medical on effectiveness in real-world settings, where the vast majority of patients with GAD present, often with a range of comorbid psychiatric and medical ALOX15 disorders and symptoms. Second, there are relatively few data on “special” populations, including children and adolescents and geriatric patients with GAD,40,41 or on whether early pharmacotherapy of GAD is able to prevent subsequent onset of mood and substance-use disorders.42 Several promising future lines of investigation of GAD have, however, been opened up by ongoing work on the psychobiology of GAD. Work on the role of the glutamate system in fear extinction,43 on the role of neuropeptides in stress responses,44 and on a range of second messenger or other downstream systems,45,46 for example, may ultimately lead to new treatments for GAD.