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Ocd
Introduction
Obsessive-compulsive disorder is one of the more common serious mental illnesses. The shame and secrecy associated with it, as well as lack of recognition of its characteristic symptoms, can lead to delay in diagnosis and treatment. Effective psychological and drug treatments are available for the distressing, time consuming, repetitive thoughts and rituals and the associated functional impairment. This article reviews the presentation and assessment of obsessive-compulsive disorder and discusses the current best treatment options, as well as directions for the future.
Methods
We searched for the term "obsessive compulsive disorder" in electronic databases and referred to published systematic reviews, including the recently published guideline from the National Institute for Health and Clinical Excellence (NICE).
Who gets it and why does it matter?
Obsessive-compulsive disorder occurs throughout the life span, and children as young as 6 or 7 present with the characteristic impairing symptoms . At the other end of the age range, patients may present for the first time in old age. Most adults with the disorder report onset in childhood or adolescence. The condition can result in considerable disability; for example, children may drop out of education and adults can become housebound. The World Health Organization rates obsessive-compulsive disorder as one of the top 20 most disabling diseases. If untreated, it generally persists,yet effective, evidence based psychological and drug treatments are available.
Recent epidemiological studies report prevalence rates of 0.8% in adults and 0.25% in 5-15 year old children, although earlier studies suggested rates as high as 1-3% in adults and 1-2% in children and adolescents.
Why do clinicians need to know about it?
People of all ages with obsessive-compulsive disorder understand the senseless nature of their repetitive, unwanted behaviours and intrusive, recurrent thoughts. This may lead to shame, reluctance to seek help, and poor recognition by health professionals. People with the disorder have long delays in accessing effective treatments—17 years on average in one study. They frequently present to non-psychiatrists for treatment, and psychiatric symptoms go undetected. Greater awareness of the condition is needed in a range of non-psychiatric healthcare settings, and clinicians need to be confident about recognising it.
What are the symptoms?
Obsessions are unwanted ideas, images, or impulses that repeatedly enter a person's mind. Although recognised as being self generated, they are experienced as "egodystonic" (out of character, unwanted, and distressing). Compulsions are repetitive stereotyped behaviours or mental acts driven by rules that must be applied rigidly. They are often intended to neutralise anxiety provoked by the obsessions. They are not inherently enjoyable and do not result in the completion of any useful task. To qualify for the diagnosis, the symptoms must be disabling. Even among children, in whom diagnostic criteria allow less insight, most patients acknowledge the senselessness of the thoughts and behaviours, as well as the wish to be rid of them. Box 2 summarises the ICD-10 (international classification of diseases, 10th revision) criteria for diagnosing the condition.
What happens in cognitive behaviour therapy?
NICE reviewed 17 trials in adults and concluded that cognitive behaviour therapy was an efficacious treatment for obsessive-compulsive disorder. The best randomised controlled trials in the younger age group showed that delivering cognitive behaviour therapy within a family setting was highly effective.
In both adults and children, the specific psychological technique most strongly associated with good outcome in studies of cognitive behaviour therapy is exposure and response prevention, which has response rates of up to 85% in patients who complete the therapy. The patient generates a hierarchy of feared situations and then practises facing the fear (exposure), while monitoring the anxiety and experiencing that it lessens without the need to carry out a ritual (response prevention). Engaging the person by helping them to design a graded programme of exposure and response prevention, and working collaboratively on easiest challenges first, is essential. Careful education about mechanisms of anxiety, understanding that repeated exposure leads to reduced anxiety, as well as reduction in obsessions, is important for success. Practice is needed, as patients will have been reinforcing their behaviours by avoiding feared situations or carrying out rituals to deal with their fears for some time.
The cognitive model of obsessive-compulsive disorder emphasises remedying faulty reasoning that may have developed with the disorder. Increasingly, therapists use cognitive strategies in combination with exposure and response prevention. Cognitive approaches encourage patients to re-evaluate overvalued beliefs about risk or personal responsibility, to regain a more realistic perspective, and to carry out "behavioural experiments" to test the validity of their beliefs.Whether the addition of cognitive techniques significantly improves the efficacy of exposure and response prevention is as yet unclear.
No evidence exists to support the efficacy of psychodynamic psychotherapy in OCD. NICE therefore does not recommend its use.
Do drug treatments work, and who should get them?
Obsessive-compulsive disorder responds specifically to drugs that inhibit the synaptic reuptake of serotonin—that is, the tricyclic antidepressant clomipramine and the more highly selective serotonin reuptake inhibitors (SSRIs). SSRIs are effective at all ages. Both the effect size and side effect profiles seem to be similar across the life span.
All the SSRIs have been subject to large scale clinical trials (33 in adults,18 in children).Dose finding studies have been carried out only in adults. Higher doses of SSRIs than those used for depression may be needed to effectively treat obsessive-compulsive disorder.
SSRIs have largely superseded clomipramine for treating obsessive-compulsive disorder because of their lesser toxicity in overdose and more favourable side effect profile. This is especially important for children, in whom cardiac toxicity may be a risk. Head to head studies show equivalent efficacy and better tolerability for SSRIs relative to clomipramine. Clomipramine remains a useful option but is usually reserved for patients in whom trials of SSRIs have been ineffective.
The therapeutic response to drug treatment in obsessive-compulsive disorder increases gradually over weeks and months; studies show that the benefits continue to accrue for at least six months and probably longer. Patients should be warned that side effects such as nausea and agitation tend to emerge early, often before the therapeutic response is consolidated, but usually abate. A trial of at least 12 weeks at the maximum tolerated dose is advisable before effectiveness is judged.
Several studies have shown that people with obsessive-compulsive disorder continue to benefit from long term drug treatment and that a large number relapse if the drug is discontinued or switched to placebo under trial conditions. Possibly, patients with greater comorbidity are at most risk of relapse. For at least some cases, therefore, treatment may need to be continued indefinitely.
Drugs, psychological therapies, or both?
On the available evidence, for children, adolescents, and adults, psychological and drug treatments seem to be equally effective. According to NICE guidance, cognitive behaviour therapy is recommended as the first line treatment for children and adolescents, because of the assumption that it has fewer risks than SSRIs.6 For adults, cognitive behaviour therapy or pharmacotherapy can be offered first. Currently, in the United Kingdom, provision of evidence based psychological therapies, such as cognitive behaviour therapy, is inadequate, and expansion of these services is needed.18
Uncertainty remains as to whether the two forms of treatment combined are superior to psychological or drug monotherapy. Several studies in adults have looked at this; some suggest that addition of drugs increases the efficacy of cognitive behaviour therapy, whereas others show no additional benefit. In a recent trial in young people, a placebo pill was compared with sertraline alone, cognitive behaviour therapy alone, and cognitive behaviour therapy plus sertraline. All three active treatments were better than placebo and not significantly different from each other. Cognitive behaviour therapy, either alone or in combination with drug treatment, might help to prolong remission and prevent relapse on discontinuation of the drug, but this remains to be tested in long term studies.
Do additional treatments help?
Up to 40% of patients who present to psychiatrists fail to respond adequately to either cognitive behaviour therapy, drugs, or a combination of the two. Careful reassessment with detection and treatment of related problems may improve outcomes. For example, young people with developmental difficulties on the autism spectrum may be susceptible to obsessive-compulsive disorder as teenagers or young adults, and these patients may need specifically tailored cognitive behaviour therapy packages.
Some evidence exists to support various drug strategies in resistant cases, including increasing the dose of the SSRI to the maximum tolerated dose and switching to an alternative, as response may be idiosyncratic. SSRI and clomipramine have been combined in some studies; this needs careful monitoring and should be done in a specialist setting. Obsessive-compulsive disorder does not respond to antipsychotic drugs given as monotherapy. Evidence from children and adults shows that adding first generation and second generation antipsychotics, in low dose, to SSRIs may benefit resistant cases and obsessive-compulsive disorder with comorbid tics. This intervention should be initiated by specialists in obsessive-compulsive disorder and monitored closely for effectiveness and side effects.
Can further research help us?
Debate is ongoing about whether obsessive-compulsive disorder is appropriately classified as an anxiety disorder. Research studies in a range of modalities (neuropsychological, neuroimaging, genetics, psychopharmacology) suggest that the disorder has a heritability and neurobiology distinct from the other anxiety disorders. Whether or not obsessive-compulsive disorder has a distinct neurobiology, it is highly responsive to psychological treatments that involve cognitive and behavioural modification of anxiety symptoms.
Altered functioning of specific brain regions (basal ganglia and orbitofrontal cortex) is implicated in the disorder. Evidence for this includes high rates of obsessive-compulsive disorder in diseases that affect these brain regions, such as Tourette's syndrome, Huntington's chorea, and Sydenham's chorea. A fluctuating form of obsessive-compulsive disorder, tics, or both (paediatric autoimmune neuropsychiatric disorders associated with streptococcal infection—PANDAS) has been recently described and is thought to be secondary to streptococcal infection and mediated by autoantibodies binding to basal ganglia. Furthermore, research into subtypes, such as compulsive hoarding, have suggested that neurobiologically distinct forms of obsessive-compulsive disorder may exist. Research is also needed on early environmental and family risk factors that may, in complex interaction with genes, be implicated in the genesis of the disorder.
Several disorders seem to be related to obsessive-compulsive disorder, either by the nature of their symptoms, which show similarities to obsessions or compulsions, or by their frequent co-occurrence. These have been termed obsessive-compulsive disorder spectrum disorders, although whether all of these disorders are causally related to obsessive-compulsive disorder is unclear. Hypochondriasis involving a preoccupation with health related fears can be similar to the disorder. Body dysmorphic disorder, which involves obsessional thoughts relating to imagined or slight defects in appearance and frequent checking in the mirror, can also be difficult to distinguish from obsessive-compulsive disorder.
Isobel Haymen
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I thought I loved you, but it was just how you looked in the light.
Last edited by !-nessica-!; 01-29-2008 at 09:39 AM.
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