Co-Occurring Disorders and Treatment Complexity Within Personality Disorders
Abstract
Excessive comorbidity within personality disorders and other psychiatric disorders is a perennial problem in psychiatric diagnosis and treatment. Questions of etiology, disorder hierarchies, and treatment decisions are problems clinicians face on a daily basis. From a pragmatic view, the presence of multiple psychiatric disorders co-occurring within the context of a personality disorder can be viewed as proxy for psychiatric severity particularly as it relates to impairments in interpersonal relating, affective instability, and impulsivity. By extension, impairments in the above facets of functioning can alert clinicians to a range of potential treatment challenges including forming and maintaining a treatment alliance, sustaining treatment adherence, and targeting symptoms for medication treatment. Evidence from high-quality efficacy studies demonstrate significant, and in some cases lasting, symptom and behavioral change, especially for patients diagnosed with borderline personality disorder.
The phenomena of co-occurring personality disorders (PDs) has been a persistent problem because most patients diagnosed with a personality disorder meet criteria for more than one (1–4). Clinicians tend to rely on implicit prototypes (5, 6) for determining diagnoses and are unlikely to include hierarchical rankings of PDs in the diagnostic process. Empirical efforts to ascertain hierarchies have failed (7), thus making it difficult for clinicians to determine which personality disorder to diagnose and treat. Although there are a number of explanations for the high rate of PD co-occurrence, it appears that this is an artifact of a criterion count system that does not reflect daily clinical practice, which is closer to a prototype matching system (8, 9).
While comorbidity among personality disorders may eventually decline if a dimensional or prototype matching approach is adopted (6, 10), there should be no changes in patterns of comorbidity (in this country at least) in the immediate future, since the content of the PD section of DSM−5 will be unchanged from that of DSM-IV-TR. Even if the alternative model for PDs, presented in Section III of DSM−5, were to be utilized, it is unlikely that the substantial prevalence of co-occurring disorders such as mood, anxiety, and substance dependence (4, 11) would be eliminated. This perspective raises perplexing questions regarding development, order of onset, etiology, and sequence of treatment priorities.
In the absence of definite answers to resolving the issues involving potentially inflated co-occurring disorders, a pragmatic approach is to regard the degree of co-occurrence as a marker of psychiatric severity. From this vantage point, co-occurring disorders that include a personality disorder may serve as one of several markers for treatment complexity (12).
As evidence for this approach, consider the following: Co-occurring disorders substantially increase the risk of poor outcome, even when patients and clinicians are adherent to evidence-based treatments. Indirect evidence from meta-analyses of depression outcomes implicates co-occurrence of PDs with poor outcome and, by extension, more complex treatment. For example, the presence of a personality disorder in the context of major depression doubles the risk of poor outcome when compared with depressed subjects without a personality disorder (13). In a reanalysis of the Sequenced Treatment Alternatives to Relieve Depression (STAR*D) results (14), researchers found that patients without any co-occurring disorders tolerated medication better, had higher rates of treatment response (51.6% versus 39.1%), and showed better rates of remission from depressive symptoms (34.4% versus 24.7%) than patients with comorbidity.
While co-occurring disorders may serve as a proxy for treatment complexity, there is mounting evidence that severity of symptoms and degree of impairment in social and occupational functioning also have an impact on response to treatment (15–17). Secondary analyses of the NIMH Treatment of Depression Collaborative Research Program (18) found that numerous markers of psychiatric severity predicted negative outcome across all treatments (pretreatment depression severity, social dysfunction, cognitive dysfunction, low expectation of improvement, combined major depressive disorder and dysthymia, and duration of current episode). In a 2-year follow-up of subjects with borderline personality disorder (BPD), the Collaborative Longitudinal Personality Disorders Study (CLPS) found that severity of BPD (as manifested by higher number of borderline personality disorder criteria, greater functional impairment, and greater interpersonal relationship instability) predicted poorer outcome (19). Evidence is also mounting to suggest that severity of psychiatric disturbance has far greater implications for treatment outcome than any single diagnosis. A reanalysis of the CLPS data found that general severity of psychiatric disturbance was most predictive of current and prospective dysfunction, and the personality trait level criteria that loaded most highly on the severity dimension were preoccupation with social rejection, fear of social ineptness, feelings of inadequacy, anger, identity disturbance, and paranoid ideation (20). The cross-cutting nature of these personality traits is suggestive of central disturbances of PDs of all types (21).
The complexity of treating individuals with greater severity of psychiatric disturbance is compounded by underlying features of interpersonal hypersensitivity among patients with PDs. Heightened rejection sensitivity, poor affect regulation, and intense interpersonal conflicts negatively impact consistent delivery of treatment (somatic and psychosocial). This is especially prominent among patients with BPD and has been proposed as a phenotype for the disorder (22). Not surprisingly then, interpersonal hypersensitivity is a contributor to frequent ruptures and is a likely underlying factor influencing high rates of premature termination among individuals with PDs. It is widely understood that individuals with personality disorders have higher rates of global service utilization (23). However, individuals with Cluster B personality disorders tend to have poorer treatment adherence and higher dropout than patients with other psychiatric disorders such as depression (24). A recent meta-analysis (25) of 669 studies including 83,834 patients found that dropout from treatment was greatest for patients with a personality disorder (25.6%). Higher rates of personality disorder criteria are also associated with higher dropout (26).
A literature review by members of the DSM−5 workgroup for personality and personality disorders revealed an overarching pattern of distorted and maladaptive thinking about oneself, and impaired interpersonal relationships as central, defining features of the personality disorders (21, 27). Numerous studies indicate that maladaptive patterns of mental representations form a common substrate of core impairments across personality disorders (28). Thus, internal working models that inform the individual’s attachment style constitute an overarching domain of personality function that impacts the quality of relationships, including those with health care professionals (29).
Clinicians are familiar with the challenges of engaging patients with personality disorders due to their preset biases and assumptions about relationships. Psychiatrists and psychologists involved in a practice research network described five distinct enduring relational patterns in the psychotherapies of 181 patients with personality disorders engaged in long-term psychotherapy (30). Four of the five transference patterns described (angry/entitled, anxious/preoccupied, avoidant/counterdependent, and sexualized) are particularly problematic in maintaining a viable therapeutic alliance.
Examination of specific personality disorders reveals unique features that create challenges in providing medical and psychological care. For example, individuals with avoidant PD are burdened with a sense of self as defective and shame ridden, with expectations of being abandoned by others because of personal shortcomings and are thus more prone to limit contact, while those with obsessive–compulsive PD are burdened by a schema of self-imposed, unrelenting standards that tends to subvert the importance of the other (31). Patients with paranoid PD typically view the self as weak and inadequate in the face of hostile and dangerous others (32). Patients with narcissistic PD have a predominant bias pervaded by distrust toward others and feeling excluded or harmed (33) and are prone to externalize and blame others for interpersonal conflict (34). By contrast, individuals with BPD have repeatedly been found to express and experience overelaborated and complex views of others with a particular bias toward hostile attributions of others’ actions and intentions (35–37). This pattern has been observed in laboratory paradigms assessing neurological structure of social cognition and distrust (38). Recent findings from a study of adolescents with BPD traits demonstrate that overactive, inaccurate attributions represent a common pathway to BPD (39). As a result of these distorted representations of self and others, BPD patients have great difficulty creating a helpful mental image of treatment providers and the treatment relationship (40). This mistrust, combined with hypersensitivity to rejection and insecure attachment styles, creates significant challenges for establishing and maintaining a viable treatment alliance and reasonable adherence to a treatment model.
In addition to the complexities of forming and maintaining an alliance, deciding which of the many psychiatric disorders to approach first has proven to be a major conundrum for clinicians. APA practice guidelines emphasize single disorders and give preference to initial treatment of clinical syndromes such as anxiety and mood disorders. The American Psychiatric Association’s Practice Guideline Watch for major depressive disorder (41) suggests strategies for treating patients with co-occurring conditions who are unresponsive to first-line agents, yet definitive evidence for “best practices” for co-occurring conditions is still unavailable. Thus there is limited guidance on which disorders to target first in the case of significant comorbidity. This is in part due to competing models of the etiology and relationship among the psychic disorders including the notion of hierarchies. One model poses that personality disorders such as BPD constitute an underlying dominant form of psychopathology that accounts for co-occurring depression, while a second model would suggest that BPD is better understood as an atypical presentation of severe biologically based depressive disorder. A third model emphasizes true independence of the two disorders and a fourth assumes overlapping etiological factors that predispose individuals with either disorder to develop the second.
A longitudinal study of symptom interactions found that between 60 to 70% of patients with depression and BPD demonstrated improvement when BPD symptomatology was the primary focus of treatment, followed by decreases in depression. Conversely, targeting mood and depression as the primary focus of treatment did not significantly impact BPD features subsequently (42). Of great importance was the fact that BPD criteria associated with affect instability, anger, emptiness, self-injurious behaviors, and psychotic experiences were most predictive of remission of depressive symptoms. Similar findings were reported in another longitudinal analysis of patients with dysthymia and BPD: improvement in BPD features was followed by reduction of dysthymic features but not vice versa (43). These studies indicate that BPD may represent an underlying dominant form of psychopathology that drives or is responsible for the expression of other disorders such as depression. The clinical implications are relatively clear in that treating borderline features early in treatment (especially features associated with affect instability) may bring about improvements in depression.
Psychotherapies that focus interventions on personality impairments reinforce the above findings more generally across PDs. A series of meta-analyses on the effectiveness of psychotherapy for treatment of personality disorders demonstrated that psychodynamic and cognitive behavioral psychotherapies of mid- to long duration were effective in reducing depression and the burden of global psychiatric symptoms, even when co-occurring disorders were present (44–46). There is far less evidence on the effectiveness of psychotherapies and medications in the treatment of specific PDs other than BPD; nonetheless, some evidence has emerged in the past decade (47). Effectiveness of dynamic and cognitive psychotherapy for avoidant personality disorder (AVPD) has been demonstrated. In this study, CBT proved to be superior to brief dynamic therapy in improving avoidance, social phobia, and obsessive symptoms (48). A long-term (52-week) form of CBT showed reductions in depression and personality symptoms at the end of treatment of patients with AVPD, and of patients with obsessive-compulsive personality disorder (OCPD) (49). Other studies have demonstrated a poorer response for individuals with AVPD compared with other Cluster C diagnoses (50) and greater relapse following treatment termination (51). Some evidence suggests that psychosocial treatment such as contingency management can be of limited benefit for patients with antisocial personality disorder (ASPD) and comorbid cocaine dependence (52), while a randomized controlled trial carried out in the United Kingdom found that a combination of multisystemic therapy (MST) and youth offender teams was effective in reducing nonviolent criminal behavior at treatment termination and at 18-month follow-up in a cohort of adolescents (average age of 15) with emerging ASPD (53). What is abundantly clear is the fact that more systematic efficacy and effectiveness studies must be conducted involving patients with PDs, especially those PDs with relatively high prevalence rates such as AVPD, OCPD, and ASPD.
Psychotropic medications are prescribed for patients with PDs with substantial frequency, and some evidence supports symptom-targeted use of antidepressants, antipsychotics, and mood stabilizers to reduce impulsivity and aggression, and to a lesser extent to reduce psychotic-like symptoms and to improve cognitive deficits characteristic of schizotypy (54). Double-blind placebo-controlled trials have demonstrated some benefit of divalproex sodium for patients with Cluster B personality disorders who demonstrate impulsive aggression (55).
The vast majority of effectiveness and efficacy studies target BPD symptomatology, therefore more is known about effective treatment for this disorder. The American Psychiatric Associations guideline for treatment of BPD (56) and the subsequent guideline watch (57) confirm that psychotherapy represents the primary treatment for this disorder with adjunctive, symptom-targeted pharmacotherapy to mitigate severity of core symptoms. A persuasive review of data from approximately 24 randomized controlled trials of BPD (58) demonstrates clear and compelling evidence that several forms of psychotherapy help borderline patients decrease the frequency of self-destructive behaviors (59–65) as well as common secondary symptoms of depression, anxiety, and substance abuse (66–68). Recent evidence indicates that durable gains can be achieved with decreased suicide attempts and service use, improved global psychiatric functioning, and reduced ratings of borderline functioning at 5-years posttreatment with long-term mentalization-based treatment (59).
While no specific “brand” of treatment has clearly demonstrated superiority to date, several common factors have been identified in individual psychotherapies for BPD. Treatments that include a clear treatment framework, attention to affect and the treatment relationship, an active therapist, and exploratory and change-oriented interventions appear to be core features of effective treatments (69).
A number of studies indicate the adjunctive benefit of pharmacotherapy for patients with BPD. Several meta-analyses of pharmacotherapy of BPD indicate that drug treatment, especially with mood stabilizers and antipsychotics, may be effective for treating affective dysregulation and impulsive-behavioral dyscontrol (70, 71). A meta-analysis of randomized controlled trials suggests that drug treatment, especially with mood stabilizers and second-generation antipsychotics, may be effective for treating a number of core symptoms and associated psychopathology, but the evidence does not currently support effectiveness for overall severity of borderline personality disorder (71). A recent meta-analysis indicated that mood stabilizers significantly reduced anger, while antidepressants had a moderate effect on anger reduction but a small effect on depression. Antipsychotics had a moderate effect on anger (70). Antipsychotics have also been shown to be effective in reducing cognitive-perceptual symptoms (72). The clinical implications are relatively clear: pharmacotherapy should target specific symptoms such as affect dysregulation, but clinicians should not expect dramatic improvement in overall BPD symptomatology. While the majority of patients with BPD are prescribed psychotropic medications for sustained periods, caution is warranted because those with BPD are at greater risk of abusing prescription medications in psychiatric and general medical practices (73).
Further research is needed to validate the approach taken by the 2001 guideline to select one of three different medication algorithms on the basis of the predominance of cognitive-perceptual symptoms, affective dysregulation symptoms, or impulse dyscontrol symptoms. One retrospective report from the NIMH Collaborative Longitudinal Personality Disorders Study produced mixed results on this question (74).
Conclusions
Despite considerable confusion regarding the comorbidity puzzle inherent in the diagnosis and treatment of individuals with personality disorders, the last decade of research has yielded high-quality efficacy studies of psychotherapeutic and psychopharmacological approaches that demonstrate reduction in debilitating symptoms common to specific personality disorders as well as cross-cutting symptoms of suicide-related behaviors, hospitalization, and relapse. This evidence from high-quality randomized control trials is particular promising given the fact that most of the studies included patients with comorbid mood, anxiety, and substance use disorders. Unlike many efficacy studies conducted on a single disorder (75), treatment studies of personality disorders include patients with co-occurring disorders and are more realistic and therefore more generalizable to general populations.
Footnote
J. Christopher Fowler, Ph.D., The Menninger Clinic, Houston, TX and Baylor College of Medicine, Houston, TX
John M. Oldham, MD, The Menninger Clinic, Houston, TX and Baylor College of Medicine, Houston, TX
The authors report no competing interests.
References
1.
Pilkonis PA, Heape CL, Proietti JM, Clark SW, McDavid JD, Pitts TE: The reliability and validity of two structured diagnostic interviews for personality disorders. Arch Gen Psychiatry 1995; 52:1025–1033
2.
Oldham JM, Skodol AE, Kellman HD, Hyler SE, Rosnick L, Davies M: Diagnosis of DSM-III-R personality disorders by two structured interviews: patterns of comorbidity. Am J Psychiatry 1992; 149:213–220
3.
Grilo CM, Sanislow CA, McGlashan TH: Co-occurrence of DSM-IV personality disorders with borderline personality disorder. J Nerv Ment Dis 2002; 190:552–554
4.
McGlashan TH, Grilo CM, Skodol AE, Gunderson JG, Shea MT, Morey LC, Zanarini MC, Stout RL: The Collaborative Longitudinal Personality Disorders Study: baseline Axis I/II and II/II diagnostic co-occurrence. Acta Psychiatr Scand 2000; 102:256–264
5.
Reed GM, Mendonça Correia J, Esparza P, Saxena S, Maj M: The WPA-WHO Global Survey of Psychiatrists’ Attitudes Towards Mental Disorders Classification. World Psychiatry 2011; 10:118–131
6.
Westen D: Prototype diagnosis of psychiatric syndromes. World Psychiatry 2012; 11:16–21
7.
Hopwood CJ, Morey LC, Gunderson JG, Skodol AE, Tracie Shea M, Grilo CM, McGlashan TH: Hierarchical relationships between borderline, schizotypal, avoidant and obsessive-compulsive personality disorders. Acta Psychiatr Scand 2006; 113:430–439
8.
First MB, Westen D: Classification for clinical practice: how to make ICD and DSM better able to serve clinicians. Int Rev Psychiatry 2007; 19:473–481
9.
Westen D, Shedler J, Bradley B, DeFife JA: An empirically derived taxonomy for personality diagnosis: bridging science and practice in conceptualizing personality. Am J Psychiatry 2012; 169:273–284
10.
Skodol AE: Personality disorders in DSM-5. Annu Rev Clin Psychol 2012; 8:317–344
11.
Zanarini MC, Frankenburg FR, Dubo ED, Sickel AE, Trikha A, Levin A, Reynolds V: Axis II comorbidity of borderline personality disorder. Compr Psychiatry 1998; 39:296–302
12.
Fowler J, Plakun E, Shapiro E: Treatment resistance and patient authority, in The Austen Riggs Reader. New York, WW Norton & Co, 2011, pp 6–23
13.
Newton-Howes G, Tyrer P, Johnson T: Personality disorder and the outcome of depression: meta-analysis of published studies. Br J Psychiatry 2006; 188:13–20
14.
Wisniewski SR, Rush AJ, Nierenberg AA, Gaynes BN, Warden D, Luther JF, McGrath PJ, Lavori PW, Thase ME, Fava M, Trivedi MH: Can phase III trial results of antidepressant medications be generalized to clinical practice? A STAR*D report. Am J Psychiatry 2009; 166:599–607
15.
Fawcett J: The role of comorbidity in severity and outcome. Psychiatr Ann 2008; 38:702
16.
Lehman A, Alexopoulos G, Goldman H, Jeste D, Üstün B: Mental disorders and disability: Time to reevaluate the relationship? in A Research Agenda for DSM-V. Edited by, Kupfer DJ, First MB, Regier DA. Washington, DC, American Psychiatric Association, 2002, pp 201–218
17.
Skodol AE, Bender DS: The future of personality disorders in DSM-V? Am J Psychiatry 2009; 166:388–391
18.
Sotsky SM, Glass DR, Shea MT, Pilkonis PA, Collins JF, Elkin I, Watkins JT, Imber SD, Leber WR, Moyer J, et al.: Patient predictors of response to psychotherapy and pharmacotherapy: findings in the NIMH Treatment of Depression Collaborative Research Program. Am J Psychiatry 1991; 148:997–1008
19.
Gunderson JG, Daversa MT, Grilo CM, McGlashan TH, Zanarini MC, Shea MT, Skodol AE, Yen S, Sanislow CA, Bender DS, Dyck IR, Morey LC, Stout RL: Predictors of 2-year outcome for patients with borderline personality disorder. Am J Psychiatry 2006; 163:822–826
20.
Hopwood CJ, Malone JC, Ansell EB, Sanislow CA, Grilo CM, McGlashan TH, Pinto A, Markowitz JC, Shea MT, Skodol AE, Gunderson JG, Zanarini MC, Morey LC: Personality assessment in DSM-5: empirical support for rating severity, style, and traits. J Pers Disord 2011; 25:305–320
21.
Bender DS, Morey LC, Skodol AE: Toward a model for assessing level of personality functioning in DSM-5, part I: a review of theory and methods. J Pers Assess 2011; 93:332–346
22.
Gunderson JG, Lyons-Ruth K: BPD’s interpersonal hypersensitivity phenotype: a gene-environment-developmental model. J Pers Disord 2008; 22:22–41
23.
Bender DS, Dolan RT, Skodol AE, Sanislow CA, Dyck IR, McGlashan TH, Shea MT, Zanarini MC, Oldham JM, Gunderson JG: Treatment utilization by patients with personality disorders. Am J Psychiatry 2001; 158:295–302
24.
Holma IA, Holma KM, Melartin TK, Isometsä ET: Treatment attitudes and adherence of psychiatric patients with major depressive disorder: a five-year prospective study. J Affect Disord 2010; 127:102–112
25.
Swift JK, Greenberg RP: Premature discontinuation in adult psychotherapy: a meta-analysis. J Consult Clin Psychol 2012; 80:547–559
26.
Crawford MJ, Price K, Gordon F, Josson M, Taylor B, Bateman A, Fonagy P, Tyrer P, Moran P: Engagement and retention in specialist services for people with personality disorder. Acta Psychiatr Scand 2009; 119:304–311
27.
Morey LC, Berghuis H, Bender DS, Verheul R, Krueger RF, Skodol AE: Toward a model for assessing level of personality functioning in DSM-5, part II: empirical articulation of a core dimension of personality pathology. J Pers Assess 2011; 93:347–353
28.
Bender DS, Skodol AE: Borderline personality as a self-other representational disturbance. J Pers Disord 2007; 21:500–517
29.
Agrawal HR, Gunderson J, Holmes BM, Lyons-Ruth K: Attachment studies with borderline patients: a review. Harv Rev Psychiatry 2004; 12:94–104
30.
Bradley R, Heim AK, Westen D: Transference patterns in the psychotherapy of personality disorders: empirical investigation. Br J Psychiatry 2005; 186:342–349
31.
Jovev M, Jackson HJ: Early maladaptive schemas in personality disordered individuals. J Pers Disord 2004; 18:467–478
32.
Salvatore G, Nicolò G, Dimaggio G: Impoverished dialogical relationship patterns in paranoid personality disorder. Am J Psychother 2005; 59:247–265
33.
Dimaggio G, Nicolo G, Fiore D, Centenero E, Semerari A, Carcione A, Pedone R: States of minds in narcissistic personality disorder: three psychotherapies analyzed using the grid of problematic states. Psychother Res 2008; 18:466–480
34.
Ronningstam E: Narcissistic personality disorder: facing DSM–V. Psychiatr Ann 2009; 39:111–121
35.
Baity MR, Blais MA, Hilsenroth MJ, Fowler JC, Padawer JR: Self-mutilation, severity of borderline psychopathology, and the Rorschach. Bull Menninger Clin 2009; 73:203–225
36.
Fowler JC, Hilsenroth MJ, Nolan E: Exploring the inner world of self-mutilating borderline patients: a Rorschach investigation. Bull Menninger Clin 2000; 64:365–385
37.
Westen D, Lohr N, Silk K, Gold L, Kerber K: Object relations and social cognition in borderlines, major depressives, and normals: a Thematic Apperception Test analysis. Psychol Assess 1990; 2:355–364
38.
King-Casas B, Sharp C, Lomax-Bream L, Lohrenz T, Fonagy P, Montague PR: The rupture and repair of cooperation in borderline personality disorder. Science 2008; 321:806–810
39.
Sharp C, Pane H, Ha C, Venta A, Patel AB, Sturek J, Fonagy P: Theory of mind and emotion regulation difficulties in adolescents with borderline traits. J Am Acad Child Adolesc Psychiatry 2011; 50:563–573, e1
40.
Bender DS, Farber BA, Sanislow CA, Dyck IR, Geller JD, Skodol AE: Representations of therapists by patients with personality disorders. Am J Psychother 2003; 57:219–236
41.
Fochtmann LJ, Gelenberg AJ: Guideline Watch: Practice Guideline for the Treatment of Patients With Major Depressive Disorder, second ed. Focus 2005, 3:34–42
42.
Gunderson JG, Morey LC, Stout RL, Skodol AE, Shea MT, McGlashan TH, Zanarini MC, Grilo CM, Sanislow CA, Yen S, Daversa MT, Bender DS: Major depressive disorder and borderline personality disorder revisited: longitudinal interactions. J Clin Psychiatry 2004; 65:1049–1056
43.
Klein DN, Schwartz JE: The relation between depressive symptoms and borderline personality disorder features over time in dysthymic disorder. J Pers Disord 2002; 16:523–535
44.
Leichsenring F, Leibing E: The effectiveness of psychodynamic therapy and cognitive behavior therapy in the treatment of personality disorders: a meta-analysis. Am J Psychiatry 2003; 160:1223–1232
45.
Leichsenring F, Rabung S, Leibing E: The efficacy of short-term psychodynamic psychotherapy in specific psychiatric disorders: a meta-analysis. Arch Gen Psychiatry 2004; 61:1208–1216
46.
Leichsenring F, Rabung S: Effectiveness of long-term psychodynamic psychotherapy: a meta-analysis. JAMA 2008; 300:1551–1565
47.
McMain S, Pos AE: Advances in psychotherapy of personality disorders: a research update. Curr Psychiatry Rep 2007; 9:46–52
48.
Emmelkamp PM, Benner A, Kuipers A, Feiertag GA, Koster HC, van Apeldoorn FJ: Comparison of brief dynamic and cognitive-behavioural therapies in avoidant personality disorder. Br J Psychiatry 2006; 189:60–64
49.
Strauss JL, Hayes AM, Johnson SL, Newman CF, Brown GK, Barber JP, Laurenceau JP, Beck AT: Early alliance, alliance ruptures, and symptom change in a nonrandomized trial of cognitive therapy for avoidant and obsessive-compulsive personality disorders. J Consult Clin Psychol 2006; 74:337–345
50.
Beretta V, de Roten Y, Drapeau M, Kramer U, Favre N, Despland JN: Clinical significance and patients’ perceived change in four sessions of brief psychodynamic intervention: characteristics of early responders. Psychol Psychother 2005; 78:347–362
51.
Karterud S, Pedersen G, Bjordal E, Brabrand J, Friis S, Haaseth O, Haavaldsen G, Irion T, Leirvåg H, Tørum E, Urnes O: Day treatment of patients with personality disorders: experiences from a Norwegian treatment research network. J Pers Disord 2003; 17:243–262
52.
Messina N, Farabee D, Rawson R: Treatment responsivity of cocaine-dependent patients with antisocial personality disorder to cognitive-behavioral and contingency management interventions. J Consult Clin Psychol 2003; 71:320–329
53.
Butler S, Baruch G, Hickey N, Fonagy P: A randomized controlled trial of multisystemic therapy and a statutory therapeutic intervention for young offenders. J Am Acad Child Adolesc Psychiatry 2011; 50:1220–1235, e2
54.
Ripoll LH, Triebwasser J, Siever LJ: Evidence-based pharmacotherapy for personality disorders. Int J Neuropsychopharmacol 2011; 14:1257–1288
55.
Hollander E, Tracy KA, Swann AC, Coccaro EF, McElroy SL, Wozniak P, Sommerville KW, Nemeroff CB: Divalproex in the treatment of impulsive aggression: efficacy in cluster B personality disorders. Neuropsychopharmacology 2003; 28:1186–1197
56.
American Psychiatric Association Practice Guidelines: Practice guideline for the treatment of patients with borderline personality disorder. Am J Psychiatry 2001; 158(Suppl):1–52
57.
Oldham JM, Beretta V, de Roten Y, Drapeau M, Kramer U, Favre N, Despland JN: Guideline Watch: Practice Guideline for the Treatment of Patients With Borderline Personality Disorder. Focus 2005; 3:396–400
58.
Leichsenring F, Leibing E, Kruse J, New AS, Leweke F: Borderline personality disorder. Lancet 2011; 377:74–84
59.
Bateman A, Fonagy P: 8-year follow-up of patients treated for borderline personality disorder: mentalization-based treatment versus treatment as usual. Am J Psychiatry 2008; 165:631–638
60.
Clarkin JF, Levy KN, Lenzenweger MF, Kernberg OF: Evaluating three treatments for borderline personality disorder: a multiwave study. Am J Psychiatry 2007; 164:922–928
61.
Doering S, Hörz S, Rentrop M, Fischer-Kern M, Schuster P, Benecke C, Buchheim A, Martius P, Buchheim P: Transference-focused psychotherapy v. treatment by community psychotherapists for borderline personality disorder: randomised controlled trial. Br J Psychiatry 2010; 196:389–395
62.
Levy KN, Meehan KB, Kelly KM, Reynoso JS, Weber M, Clarkin JF, Kernberg OF: Change in attachment patterns and reflective function in a randomized control trial of transference-focused psychotherapy for borderline personality disorder. J Consult Clin Psychol 2006; 74:1027–1040
63.
Linehan MM, Comtois KA, Murray AM, Brown MZ, Gallop RJ, Heard HL, Korslund KE, Tutek DA, Reynolds SK, Lindenboim N: Two-year randomized controlled trial and follow-up of dialectical behavior therapy vs therapy by experts for suicidal behaviors and borderline personality disorder. Arch Gen Psychiatry 2006; 63:757–766
64.
McMain SF, Links PS, Gnam WH, Guimond T, Cardish RJ, Korman L, Streiner DL: A randomized trial of dialectical behavior therapy versus general psychiatric management for borderline personality disorder. Am J Psychiatry 2009; 166:1365–1374
65.
Verheul R, Van Den Bosch LM, Koeter MW, De Ridder MA, Stijnen T, Van Den Brink W: Dialectical behaviour therapy for women with borderline personality disorder: 12-month, randomised clinical trial in The Netherlands. Br J Psychiatry 2003; 182:135–140
66.
Bateman A, Fonagy P: Randomized controlled trial of outpatient mentalization-based treatment versus structured clinical management for borderline personality disorder. Am J Psychiatry 2009; 166:1355–1364
67.
Bohus M, Haaf B, Simms T, Limberger MF, Schmahl C, Unckel C, Lieb K, Linehan MM: Effectiveness of inpatient dialectical behavioral therapy for borderline personality disorder: a controlled trial. Behav Res Ther 2004; 42:487–499
68.
Soler J, Pascual JC, Tiana T, Cebrià A, Barrachina J, Campins MJ, Gich I, Alvarez E, Pérez V: Dialectical behaviour therapy skills training compared to standard group therapy in borderline personality disorder: a 3-month randomised controlled clinical trial. Behav Res Ther 2009; 47:353–358
69.
Weinberg I, Ronningstam E, Goldblatt MJ, Schechter M, Maltsberger JT: Common factors in empirically supported treatments of borderline personality disorder. Curr Psychiatry Rep 2011; 13:60–68
70.
Mercer D, Douglass AB, Links PS: Meta-analyses of mood stabilizers, antidepressants and antipsychotics in the treatment of borderline personality disorder: effectiveness for depression and anger symptoms. J Pers Disord 2009; 23:156–174
71.
Lieb K, Völlm B, Rücker G, Timmer A, Stoffers JM: Pharmacotherapy for borderline personality disorder: Cochrane systematic review of randomised trials. Br J Psychiatry 2010; 196:4–12
72.
Vita A, De Peri L, Sacchetti E: Antipsychotics, antidepressants, anticonvulsants, and placebo on the symptom dimensions of borderline personality disorder: a meta-analysis of randomized controlled and open-label trials. J Clin Psychopharmacol 2011; 31:613–624
73.
Sansone RA, Wiederman MW: The abuse of prescription medications: borderline personality patients in psychiatric versus non-psychiatric settings. Int J Psychiatry Med 2009; 39:147–154
74.
Oldham JM, Bender DS, Skodol AE, Dyck IR, Sanislow CA, Yen S, Grilo CM, Shea MT, Zanarini MC, Gunderson EJ, McGlashan TH: Testing an APA practice guideline: symptom-targeted medication utilization for patients with borderline personality disorder. J Psychiatr Pract 2004; 10:156–161
75.
Westen D, Novotny CM, Thompson-Brenner H: The empirical status of empirically supported psychotherapies: assumptions, findings, and reporting in controlled clinical trials. Psychol Bull 2004; 130:631–663
Information & Authors
Information
Published In
History
Published online: 1 April 2013
Published in print: Spring 2013
Authors
Funding Information
Author Information and CME Disclosure
Metrics & Citations
Metrics
Citations
Export Citations
If you have the appropriate software installed, you can download article citation data to the citation manager of your choice. Simply select your manager software from the list below and click Download.
For more information or tips please see 'Downloading to a citation manager' in the Help menu.
View Options
View options
PDF/EPUB
View PDF/EPUBGet Access
Login options
Already a subscriber? Access your subscription through your login credentials or your institution for full access to this article.
Personal login Institutional Login Open Athens loginNot a subscriber?
PsychiatryOnline subscription options offer access to the DSM-5-TR® library, books, journals, CME, and patient resources. This all-in-one virtual library provides psychiatrists and mental health professionals with key resources for diagnosis, treatment, research, and professional development.
Need more help? PsychiatryOnline Customer Service may be reached by emailing [email protected] or by calling 800-368-5777 (in the U.S.) or 703-907-7322 (outside the U.S.).