Personality Disorders

Background: A personality disorder, as defined in the Diagnostic and Statistical Manual of the American Psychiatric Association, Fourth Edition (DSM-IV), is an enduring pattern of inner experience and behavior that differs markedly from the expectations of the individual's culture, is pervasive and inflexible, has an onset in adolescence or early adulthood, is stable over time, and leads to distress or impairment. Personality disorders are a long-standing and maladaptive pattern of perceiving and responding to other people and to stressful circumstances. Ten personality disorders, grouped into 3 clusters (ie, A, B, C), are defined in the DSM-IV.

Pathophysiology: The origin of personality disorders is a matter of considerable controversy. Traditional thinking holds that these maladaptive patterns are the result of dysfunctional early environments that prevent the evolution of adaptive patterns of perception, response, and defense. A body of data points toward genetic and psychobiologic contributions to the symptomology of these disorders; however, the inconsistency of the data prevents authorities from drawing definite conclusions.

Frequency:

• In the US: Personality disorders affect 10-15% of the adult US population. Individuals may have more than one personality disorder. The following are prevalences for specific personality disorders in the general population:
  • Paranoid personality disorder - 0.5-2.5%

  • Schizotypal personality disorder - 3%

  • Antisocial personality disorder - 3% of men, 1% of women

  • Borderline personality disorder - 2%

  • Histrionic personality disorder - 2-3%

  • Narcissistic personality disorder - Less than 1%

  • Avoidant personality disorder - 0.5-1%

  • Obsessive-compulsive personality disorder - 1%

• Internationally: Because the DSM-IV criteria are so bound to North American cultural definitions, epidemiologic data about personality disorders in other countries are notoriously unreliable.

Mortality/Morbidity: Patients with personality disorders are at higher risk than the general population for many (Axis I) psychiatric disorders. Mood disorders are a particular risk across all personality diagnoses. Some comorbidities are more specific to particular personality disorders and clusters.

• Cluster A: Paranoid personality disorder may appear as a prodrome to delusional disorder or frank schizophrenia. These individuals are at risk for agoraphobia, major depression, obsessive-compulsive disorder, and substance abuse. Individuals with schizoid personality disorder may develop major depression. Patients with schizotypal personality disorder may develop brief psychotic disorder, schizophreniform disorder, or delusional disorder. At the time of diagnosis, 30-50% have concurrent major depression, and most have a history of at least one major depressive episode.

• Cluster B: Antisocial personality disorder is associated with a risk for anxiety disorders, substance abuse, somatization disorder, and pathological gambling. Borderline personality disorder is associated with a risk for substance abuse, eating disorders (particularly bulimia), and posttraumatic stress disorder. Suicide is a particular risk in borderline patients. Histrionic personality disorder is associated particularly with somatoform disorders. People with narcissistic personality disorder are at risk for anorexia nervosa and substance abuse.

• Cluster C: Avoidant personality disorder is associated with anxiety disorders (especially social phobia). Dependent personality disorder carries a risk for anxiety disorders and adjustment disorder. People with obsessive-compulsive personality disorder may be at risk for myocardial infarction because of their common type A lifestyles. They may also be at risk for anxiety disorders. Notably, they are probably not at increased risk for obsessive-compulsive disorder.

Race: No differences in prevalence across the races have been noted.

Sex:

• Cluster A: Schizoid personality disorder is slightly more common in males than in females.

• Cluster B: Antisocial personality disorder is 3 times more prevalent in men than in women. Borderline personality disorder is 3 times more common in women than in men. Of patients with narcissistic personality disorder, 50-75% are male.

• Cluster C: Obsessive-compulsive personality disorder is diagnosed twice as often in men than in women.

Age: Personality disorders generally should not be diagnosed in children and adolescents because personality development is not complete and symptomatic traits may not persist into adulthood. Because the criteria for diagnosis of personality disorders are closely related to behaviors of young and middle adulthood, DSM-IV diagnoses of personality disorders are notoriously unreliable in the elderly population.

CLINICAL

History: In general, patients with personality disorders have wide-ranging problems in social relationships and mood regulation. These problems have usually been present throughout adult life. These patients’ patterns of perception, thought, and response are fixed and inflexible, although their behavior is often unpredictable. These patterns markedly deviate from their specific culture's expectations. To meet the DSM-IV threshold for clinical diagnosis, the pattern must result in clinically significant distress or impairment in social, occupational, or other important areas of functioning.

• Cluster A (odd, eccentric)

• Paranoid personality disorder: Individuals with this disorder display pervasive distrust and suspiciousness. Common beliefs include the following:
  • Others are exploiting or deceiving the person.

  • Friends and associates are untrustworthy.

  • Information confided to others will be used maliciously.

  • There is hidden meaning in remarks or events others perceive as benign.

  • The spouse or partner is unfaithful.

• Schizoid personality disorder: This type of personality disorder is uncommon in clinical settings. A person with this disorder is markedly detached from others and has little desire for close relationships. This person’s life is marked by little pleasure in activities. People with this disorder appear indifferent to the praise or criticism of others and often seem cold or aloof.

• Schizotypal personality disorder: People with this disorder exhibit marked eccentricities of thought, perception, and behavior. Typical examples are as follows:
  • Ideas of reference (ie, believing that public messages are directed personally at them)

  • Odd beliefs or magical thinking

  • Vague, circumstantial, or stereotyped speech

  • Excessive social anxiety that does not diminish with familiarity

  • Idiosyncratic perceptual experiences or bodily illusions

• Cluster B (dramatic, emotional)

• Antisocial personality disorder: Individuals with antisocial personality disorder display a pervasive pattern of disregard for and violation of the rights of others and the rules of society. Onset must occur by age 15 years and includes the following features:
  • Repeated violations of the law

  • Pervasive lying and deception

  • Physical aggressiveness

  • Reckless disregard for safety of self or others

  • Consistent irresponsibility in work and family environments

  • Lack of remorse

• Borderline personality disorder: The central feature of borderline personality disorder is a pervasive pattern of unstable and intense interpersonal relationships, self-perception, and moods. Impulse control is markedly impaired. Transiently, such patients may appear psychotic because of the intensity of their distortions. Borderline personality disorder is one of the most commonly overused diagnoses in DSM-IV. Diagnostic criteria require at least 5 of the following features:
  • Frantic efforts to avoid expected abandonment

  • Unstable and intense interpersonal relationships

  • Markedly and persistently unstable self-image

  • Impulsivity in at least 2 areas that are potentially self-damaging (eg, sex, substance abuse, reckless driving)

  • Recurrent suicidal behaviors or threats or self-mutilation

  • Affective instability

  • Chronic feelings of emptiness

  • Inappropriate and intense anger

  • Transient paranoia or dissociation

• Histrionic personality disorder: Patients with histrionic personality disorder display excessive emotionality and attention-seeking behavior. They are quite dramatic and often sexually provocative or seductive. Their emotions are labile. In clinical settings, their tendency to vague and impressionistic speech is often highlighted.

• Narcissistic personality disorder: Narcissistic patients are grandiose and require admiration from others. Particular features of the disorder include the following:
  • Exaggeration of their own talents or accomplishments

  • Sense of entitlement

  • Exploitation of others

  • Lack of empathy

  • Envy of others

  • An arrogant, haughty attitude

• Cluster C (anxious, fearful)

• Avoidant personality disorder: Avoidant patients are generally very shy. They display a pattern of social inhibition, feelings of inadequacy, and hypersensitivity to rejection. Unlike patients with schizoid personality disorder, they actually desire relationships with others but are paralyzed by their fear and sensitivity into social isolation.

• Dependent personality disorder: While many people exhibit dependent behaviors and traits, people with dependent personality disorder have an excessive need to be taken care of that results in submissive and clinging behavior, regardless of consequences. Diagnosis requires at least 5 of the following features:
  • Difficulty making decisions without guidance and reassurance

  • Need for others to assume responsibility for most major areas of the person's life

  • Difficulty expressing disagreement with others

  • Difficulty initiating activities because of lack of confidence

  • Excessive measures to obtain nurturance and support

  • Discomfort or helplessness when alone

  • Urgent seeking for another relationship when one has ended

  • Unrealistic preoccupation with fears of being left to fend for themselves

• Obsessive-compulsive personality disorder: People with obsessive-compulsive personality disorder are markedly preoccupied with orderliness, perfectionism, and control. They lack flexibility or openness. Their preoccupations interfere with their efficiency despite their focus on tasks. They are often scrupulous and inflexible about matters of morality, ethics, and values to a point beyond cultural norms. They are often stingy as well as stubborn.

Physical: No specific physical findings are associated with any personality disorders. Physical examination may reveal findings related to the consequences and sequelae of various personality disorders.

• Patients (particularly those with cluster B disorders) may show signs of prior suicide attempts or stigmata of substance abuse.

• Substance abuse is a common comorbidity and may be reflected in the physical stigmata of alcoholism or drug abuse.

• Suicide attempts may leave scars from self-inflicted wounds.

• Mental status findings

• Patients with histrionic personality disorder may display la belle indifférence, a seemingly indifferent detachment while describing dramatic physical symptoms.

• A hostile attitude is typical of patients with antisocial personality disorder.

• Patients with cluster B personality disorders, particularly borderline personality disorder, frequently display affective lability.

• Patients with paranoid personality disorder voice persecutory ideation without the formal thought disorder observed in schizophrenia.

• Patients with schizotypal personality disorder speak with odd or idiosyncratic use of language.

Causes:

• Paranoid personality disorder: A genetic contribution to paranoid traits and a possible genetic link between this personality disorder and schizophrenia exist. Psychosocial theories implicate projection of negative internal feelings and parental modeling.

• Schizoid personality disorder: Support for the heritability of this disorder exists.

• Schizotypal personality disorder: This disorder is genetically linked with schizophrenia. Evidence for dysregulation of dopaminergic pathways in these patients exists.

• Antisocial personality disorder: A genetic contribution to antisocial behaviors is strongly supported. Low levels of behavioral inhibition may be mediated by serotonergic dysregulation in the septohippocampal system. There may also be developmental or acquired abnormalities in the prefrontal brain systems and reduced autonomic activity in antisocial personality disorder. This may underlie the low arousal, poor fear conditioning, and decision-making deficits described in antisocial personality disorder.

• Borderline personality disorder: Psychosocial formulations point to the high prevalence of early abuse (sexual, physical, and emotional) in these patients, and the borderline syndrome is often formulated as a variant of posttraumatic stress disorder. Mood disorders in first-degree relatives are strongly linked. Biological factors, such as abnormal monoaminergic functioning (especially in serotonergic function) and prefrontal neuropsychological dysfunction, have been implicated but have not been well established by research.

• Histrionic personality disorder: Little research has been conducted to determine the biologic sources of this disorder. Psychoanalytic theories incriminate seductive and authoritarian attitudes by fathers of these patients.

• Narcissistic personality disorder: No data on biological features of this disorder are available. In the classic model, narcissism functions as a defense against awareness of low self-esteem.

• Avoidant personality disorder: This personality disorder appears to be an expression of extreme traits of introversion and neuroticism. No data on biological causes are available, although a diagnostic overlap with social phobia probably exists.

• Dependent personality disorder: No studies of genetics or of biological traits of these patients have been conducted. Central to their psychodynamic constellation is an insecure form of attachment to others, which may be the result of clinging parental behavior.

• Obsessive-compulsive personality disorder: Modest evidence points toward the heritability of this disorder. Psychodynamically, these patients are viewed as needing control as a defense against shame or powerlessness.

Other Problems to be Considered:

The diagnosis of personality disorders in patients who have comorbid Axis I disorders, including mood, substance abuse, and medical disorders (eg, head injury, seizure disorders), can make the diagnosis of personality disorders more difficult because of overlapping features. Premorbid and developmental history, especially from collateral sources, is helpful in differential diagnosis.

WORKUP

Lab Studies:

• Toxicology screen: Substance abuse is common in many personality disorders, and intoxication can lead patients to present with some features of personality disorders.

• Screening for HIV and other sexually transmitted diseases: Patients with personality disorders often exhibit poor impulse control and many act without regard to risk.

Other Tests:

• Psychological testing may support or direct the clinical diagnosis.

• The Minnesota Multiphasic Personality Inventory (MMPI) is the best-known psychological test. The Eysenck Personality Inventory and the Personality Diagnostic Questionnaire are also used. None of these has been reliably validated against DSM-IV diagnoses.

• The Structured Clinical Interview for DSM-IV for Axis II Disorders (SCID-II) can also be used to aid in diagnosis.

TREATMENT

Medical Care: Psychotherapy is at the core of care for personality disorders. Because personality disorders produce symptoms as a result of poor or limited coping skills, psychotherapy aims to improve perceptions of and responses to social and environmental stressors.

• Psychodynamic psychotherapy examines the ways that patients perceive events, based on the assumption that perceptions are shaped by early life experiences. Psychotherapy aims to identify perceptual distortions and their historical sources and to facilitate the development of more adaptive modes of perception and response. Treatment is usually extended over a course of several years at a frequency from several times a week to once a month.

Consultations: The primary care physician should usually consider psychiatric consultation for patients with personality disorders because the ongoing psychiatric care that patients require is not readily provided in the primary care setting.

MEDICATION

Medications are in no way curative for any personality disorder. They should be viewed as an adjunct to psychotherapy so that the patient may productively engage in psychotherapy.

The focus is on treatment of symptom clusters such as cognitive-perceptual symptoms, affective dysregulation, and impulsive-behavioral dyscontrol. These symptoms may complicate almost all personality disorders to varying degrees, but all of them have been noted in borderline personality disorder.

The assumption is that neurotransmitter abnormalities underlie these symptom clusters that transcend the concepts of Axis I and Axis II disorders. The strongest evidence for pharmacologic treatment of personality disorders has been for borderline personality disorder, but even this is based on a fairly small database of studies.

Drug Category: Antidepressants -- Because of overdose risk, tricyclic antidepressants and monoamine oxidase inhibitors (MAOIs) are usually not prescribed for patients with personality disorders. The selective serotonin reuptake inhibitors (SSRIs) and newer antidepressants are safe and reasonably effective. However, because the depression of most patients with personality disorders stems from their limited range of coping capacities, antidepressants are usually less effective than in patients with uncomplicated major depression.
Antidepressants are most often prescribed for a limited time in patients with serious depressive episodes lasting longer than a few weeks.

Drug Name	Sertraline (Zoloft) -- Selectively inhibits presynaptic serotonin reuptake.
Adult Dose	50-150 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; MAOIs taken within prior 2 wk
Interactions	Serotonergic agents, such as other SSRIs, meperidine, and MAOIs, can produce serotonergic reactions with sertraline
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in preexisting seizure disorders and those that have experienced recent MI, have unstable heart disease, or hepatic or renal impairment

Drug Name	Paroxetine (Paxil) -- Potent selective inhibitor of neuronal serotonin reuptake. Also has weak effect on norepinephrine and dopamine neuronal reuptake.
Adult Dose	20-60 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; concurrent administration with MAOIs, or within 14 d of discontinuing
Interactions	Phenobarbital, phenytoin, and carbamazepine may decrease effects; cimetidine may increase toxicity; because of its effects on the cytochrome P-450 enzyme systems and protein binding, can increase blood levels of antipsychotics, anticonvulsants, other antidepressants, beta-blockers, type 1C antiarrhythmics, and coumadin; serotonin syndrome may occur when used with other serotonergic agents such as buspirone, meperidine, tramadol, dextromethorphan, triptans, mirtazapine, nefazodone, and other SSRIs, but especially with MAOIs
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in history of seizures, mania, renal disease, and cardiac disease; adverse effects include drowsiness, headache, weight gain, and sexual dysfunction

Drug Name	Fluoxetine (Prozac) -- Selectively inhibits presynaptic serotonin reuptake with minimal or no effect in the reuptake of norepinephrine or dopamine.
Adult Dose	20-80 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; concurrent administration of MAOIs or within the last 2 wk
Interactions	Phenobarbital, phenytoin, and carbamazepine may decrease effects; cimetidine may increase toxicity; because of its effects on the cytochrome P-450 enzyme systems and protein binding can increase blood levels of antipsychotics, anticonvulsants, other antidepressants, beta-blockers, type 1C antiarrhythmics, and coumadin; serotonin syndrome may occur when used with other serotonergic agents such as buspirone, meperidine, tramadol, dextromethorphan, triptans, mirtazapine, nefazodone, and other SSRIs, but especially with MAOIs
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in hepatic impairment and history of seizures; MAOIs should be discontinued at least 14 d before initiating fluoxetine therapy; adverse effects include insomnia, headache, weight gain, and sexual dysfunction

Drug Name	Citalopram (Celexa) -- Enhances serotonin activity because of selective reuptake inhibition at the neuronal membrane.
Adult Dose	40-80 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; concurrent MAOI therapy
Interactions	May be potentiated by cimetidine; serotonin syndrome may occur when used with other serotonergic agents such as buspirone, meperidine, tramadol, dextromethorphan, triptans, mirtazapine, nefazodone, and other SSRIs, but especially with MAOIs
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in cirrhosis, suicidal tendencies, SIADH, DM, and breastfeeding; common adverse effects include fatigue, headache, and sexual dysfunction

Drug Name	Nefazodone (Serzone) -- Antagonist at the 5-HT2 receptor and inhibits the reuptake of 5-HT. Also has negligible affinity for cholinergic and histaminergic receptors.
Adult Dose	300-600 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; MAOIs within 14 d of initiating treatment
Interactions	Increases effects of digoxin, carbamazepine, triazolam, alprazolam, and protease inhibitors through its effect of inhibiting CYP-450 3A4 enzyme. Serotonin syndrome may occur when used with other serotonergic agents such as buspirone, meperidine, tramadol, dextromethorphan, triptans, mirtazapine, and SSRIs, but especially with MAOIs
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in cardiac disease, cerebrovascular disease, or seizures; discontinue therapy and reevaluate if priapism occurs; adverse effects include drowsiness, headache, and weight gain

Drug Name	Mirtazapine (Remeron) -- Increases availability of serotonin and norepinephrine.
Adult Dose	15-60 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; MAOIs within 14 d of initiating treatment
Interactions	May potentiate effects of alcohol and benzodiazepines; serotonin syndrome may occur when used with other serotonergic agents such as buspirone, meperidine, tramadol, dextromethorphan, triptans, nefazodone, and SSRIs, but especially with MAOIs
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Common adverse effects include drowsiness, headache, and weight gain

Drug Category: Anticonvulsants -- Useful in stabilizing the affective extremes in patients with bipolar disorder but are less effective for that purpose in patients with personality disorders. They have some demonstrated efficacy in suppressing impulsive and particularly aggressive behavior in patients with personality disorder.

Drug Name	Valproic acid (Depakote) -- Most widely used agent in its class. Modestly effective and generally well tolerated.
Adult Dose	Initial: 750 mg/d in divided doses; may increase by 500 mg/d q2-3d to achieve trough serum levels of 50-125 mcg/mL
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity; hepatic disease/dysfunction
Interactions	Coadministration with cimetidine, salicylates, felbamate, and erythromycin may increase toxicity; rifampin may significantly reduce levels; in pediatric patients, protein binding and metabolism of valproate decrease when taken concomitantly with salicylates; coadministration with carbamazepine may result in variable changes of carbamazepine concentrations with possible loss of seizure control; valproate may increase diazepam and ethosuximide toxicity (monitor closely); may increase phenobarbital and phenytoin levels while either one may decrease valproate levels; may displace warfarin from protein-binding sites (monitor coagulation tests); may increase zidovudine levels in patients who are HIV seropositive
Pregnancy	D - Unsafe in pregnancy
Precautions	Thrombocytopenia and abnormal coagulation parameters have occurred; risk of thrombocytopenia increases significantly at total trough valproate plasma concentrations >110 mcg/mL in females and 135 mcg/mL in males; at periodic intervals and prior to surgery determine platelet counts and bleeding time before initiating therapy; reduce dose or discontinue therapy if hemorrhage, bruising, or a hemostasis/coagulation disorder occur; hyperammonemia may occur, resulting in hepatotoxicity; monitor patients closely for appearance of malaise, weakness, facial edema, anorexia, jaundice, and vomiting; may cause drowsiness; adverse effects include headache, drowsiness, nausea, tremor, dizziness, and alopecia

Drug Category: Antipsychotics -- Some personality disorders produce transient psychotic periods (especially borderline personality disorder), while others (eg, schizotypal personality disorder) feature chronic idiosyncratic ideation of nearly psychotic proportions.

Response to antipsychotics is less dramatic than in true psychotic Axis I disorders, but symptoms such as anxiety, hostility, and sensitivity to rejection may be reduced. Antipsychotics are typically used for a short time while the symptoms are active.

The atypical antipsychotics have almost completely replaced the traditional neuroleptics because of their safety margin, but neurologic risks (including tardive dyskinesia and neuroleptic malignant syndrome) are never absent. Risperidone and olanzapine are described here; however, quetiapine and ziprasidone may also be used. No evidence indicates that any of these has superior efficacy, and each one may have advantages and disadvantages from the standpoint of adverse effects.

Drug Name	Risperidone (Risperdal) -- Binds to dopamine D2 receptor with a 20-times lower affinity than for the 5-HT2 receptor. Improves negative symptoms of psychoses and reduces incidence of extrapyramidal adverse effects.
Adult Dose	0.5-4 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity
Interactions	Coadministration enhances the effects of alcohol and other CNS suppressants; may inhibit effects of levodopa; may increase clozapine levels
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	May cause extrapyramidal reactions, hypotension, tachycardia, and arrhythmias; adverse effects include pseudoparkinsonism (particularly at doses >6 mg/d), sedation, dizziness, and rhinitis

Drug Name	Olanzapine (Zyprexa) -- May inhibit serotonin, muscarinic, and dopamine effects.
Adult Dose	3.75-30 mg/d PO
Pediatric Dose	Not established
Contraindications	Documented hypersensitivity
Interactions	Fluvoxamine may increase effects; antihypertensives may increase risk of hypotension and orthostatic hypotension; levodopa, pergolide, bromocriptine, charcoal, carbamazepine, omeprazole, rifampin, and cigarette smoking may decrease effects
Pregnancy	C - Safety for use during pregnancy has not been established.
Precautions	Caution in narrow-angle glaucoma, cardiovascular disease, cerebrovascular disease, prostatic hypertrophy, seizure disorders, hypovolemia, and dehydration; adverse effects include sedation, constipation, weight gain, and postural hypotension; tardive dyskinesia has been reported

FOLLOW-UP

Further Inpatient Care:

• Criteria for hospitalization of patients with personality disorders are generally the same as for patients with Axis I psychiatric disorders: imminent danger to self or others, inability to care for basic needs, or psychosocial stressors overwhelming the patient's capacity to cope.

MISCELLANEOUS

Medical/Legal Pitfalls:

• The poor impulse control of these patients, particularly those with cluster B disorders, places some degree of legal responsibility on the physician. If a patient threatens someone else with injury, the physician may have a duty to warn the intended victim, either directly or through legal authorities, under the Tarasoff ruling.

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