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Agoraphobia in adults: Incidence and longitudinal relationship with panic

Published online by Cambridge University Press:  02 January 2018

O. Joseph Bienvenu*
Affiliation:
Department of Psychiatry and Behavioral Sciences, Johns Hopkins University School of Medicine, Baltimore, Maryland
Chiadi U. Onyike
Affiliation:
Department of Psychiatry and Behavioral Sciences, Johns Hopkins University School of Medicine, Baltimore, Maryland
Murray B. Stein
Affiliation:
Departments of Psychiatry and Family and Preventive Medicine, University of California, San Diego, California
Li-Shiun Chen
Affiliation:
Department of Psychiatry, Washington University School of Medicine, St Louis, Missouri
Jack Samuels
Affiliation:
Department of Psychiatry and Behavioral Sciences, Johns Hopkins University School of Medicine, Baltimore, Maryland
Gerald Nestadt
Affiliation:
Department of Psychiatry and Behavioral Sciences, Johns Hopkins University School of Medicine, Baltimore, Maryland
William W. Eaton
Affiliation:
Department of Mental Health, Johns Hopkins University Bloomberg School of Public Health, Baltimore, Maryland, USA
*
Dr O. J. Bienvenu, 600 North Wolfe Street, Meyer 101, Baltimore, MD 21287, USA. Tel: +1 410 614 9063; fax: +1 410 614 5913; e-mail: [email protected]
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Abstract

Background

Theories regarding how spontaneous panic and agoraphobia relate are based mostly on cross-sectional and/or clinic data.

Aims

To determine how spontaneous panic and agoraphobia relate longitudinally, and to estimate the incidence rate of and other possible risk factors for first-onset agoraphobia, using a general population cohort.

Method

A sample of 1920 adults in east Baltimore were assessed in 1981 -1982 and the mid-1990s with the Diagnostic Interview Schedule (DIS). Psychiatristdiagnoses were made in a subset of the sample at follow-up (n=816).

Results

Forty-one new cases of DIS/DSM–III–R agoraphobia were identified (about 2 per 1000 person-years at risk). As expected, baseline DIS/DSM-III panic disorder predicted first incidence of agoraphobia (OR=12, 95% CI 3.2-45), as did younger age, female gender and other phobias. Importantly, baseline agoraphobia without spontaneous panic attacks also predicted first incidence of panic disorder (OR=3.9, 95% CI 1.8-8.4). Longitudinal relationships between panic disorder and psychiatrist-confirmed agoraphobia were strong (panic before agoraphobia OR=20, 95% CI 2.3–180; agoraphobia before panic OR=16, 95% CI 3.2–78).

Conclusions

The implied one-way causal relationship between spontaneous panic attacks and agoraphobia in DSM–IV appears incorrect.

Type
Papers
Copyright
Copyright © Royal College of Psychiatrists, 2006 

The DSM–IV implies that agoraphobia is almost always a consequence of spontaneous panic attacks (American Psychiatric Association, 1994, 2000). Recent editions of the DSM have been influenced by the work of Klein (Reference Klein1980) and others, whose patients usually reported that their agoraphobic symptoms followed unexpected spells of panic. Although epidemiological studies found many people with agoraphobia but no history of panic, typical epidemiological methods, employing fully structured non-clinician interviews, were suspect (Reference Horwath, Lish and JohnsonHorwath et al, 1993). Also, although retrospective investigations found that agoraphobic symptoms preceded panic in some patients with both conditions (reviewed in Reference Fava and MangelliFava & Mangelli, 1999), the authors of DSM–IV were concerned about possible recall bias (Reference Craske, Widiger, Frances and PincusCraske, 1996) given the absence of prospective longitudinal studies such as the one reported here. We sought to determine first, how spontaneous panic and agoraphobia relate longitudinally, and second, the incidence rate of and other possible risk factors for first-onset agoraphobia, using a longitudinally assessed general population cohort, with clinical reappraisal at follow-up to assess effects of possible diagnostic misclassification.

METHOD

Sample

The Epidemiologic Catchment Area (ECA) programme was completed in five centres in the USA from 1981 to 1982 (Reference Regier, Myers and KramerRegier et al, 1984). Trained non-clinician interviewers administered the National Institute of Mental Health Diagnostic Interview Schedule (DIS; Reference Robins, Helzer and CroughanRobins et al, 1981) to a probabilistic sample of the adult population in each centre at two points in time, separated by a 1-year interval. In Baltimore, the original sample included 3481 participants (Fig. 1).

Fig. 1 Overview of the Baltimore Epidemiologic Catchment Area (ECA) Study. DIS, Diagnostic Interview Schedule; SCAN, Schedules for Clinical Assessment in Neuropsychiatry.

Between 1993 and 1996, in the Baltimore ECA Follow-up Study, 88% of the original Baltimore cohort were traced, and 73% of those known to be alive were interviewed again using the DIS (n=1920). The survey method is described in detail elsewhere (Reference Eaton, Anthony and GalloEaton et al, 1997). Briefly, the same survey procedures were used as in 1981. The interview was augmented with a life chart, in order to assist recall over the follow-up period. Mortality in the intervening 13 years was substantial as a result of the high proportion of elderly respondents originally sampled at this site. Neither baseline phobias nor panic disorder were significant predictors of loss to follow-up or refusal to participate in the follow-up study, although phobias were weakly predictive of mortality between interview waves (Reference Badawi, Eaton and MyllyluomaBadawi et al, 1999).

A subset of the 1920 participants in the Baltimore ECA Follow-up Study was additionally interviewed by psychiatrists (n=816). Individuals were selected for this interview mainly if they showed evidence of Axis I psychopathology (especially with the DIS) in 1981 and/or in the Follow-up Study, although about a quarter were selected at random from the remaining members of the sample (Reference Samuels, Eaton and BienvenuSamuels et al, 2002). A total of 816 persons participated in the psychiatric evaluation, which included the use of a semi-structured diagnostic instrument, the Schedule for Clinical Assessment in Neuropsychiatry (SCAN; Reference Wing, Babor and BrughaWing et al, 1990). Participants provided informed consent for each interview, and the current study was approved by the Johns Hopkins Medicine Institutional Review Board 3.

Diagnostic interviews

The version of the DIS used in the first two interview waves (1981 and 1982) included a general description of a phobia (‘such a strong fear of something or some situation that [you] try to avoid it, even though [you] know there is no real danger’), followed by screening questions about fears of ‘tunnels or bridges’, ‘public transportation (airplanes, buses, elevators)’, ‘crowds’, ‘going out of the house alone’ and ‘being alone’. If respondents acknowledged having any of these unreasonable fears that resulted in avoidance and ‘interfered with (their lives) or activities a lot’, they were given DIS/DSM–III diagnoses of agoraphobia (Reference Boyd, Robins, Holzer, Eaton and KesslerBoyd et al, 1985). As noted by Weissman et al (Reference Weissman, Leaf and Blazer1986), the DIS did not address the DSM–III concept of agoraphobia as ‘fear of being in a place from which escape might be impossible or difficult in case of incapacitation’ (American Psychiatric Association, 1980).

The version of the DIS used from 1993 to 1996 was modified to reflect the changes in diagnostic criteria in DSM–III–R (American Psychiatric Association, 1987). Screening questions for agoraphobia read:

  1. (a) ‘Some people have such an unreasonable fear of being in a crowd, travelling in buses, cars or trains, or crossing a bridge that they always get very upset in such a situation or avoid it altogether. Did you ever go through a period when being in such a situation always frightened you badly?’

  2. (b) ‘Did you ever have such an unreasonably strong fear of being alone away from home that you always got very upset in this situation, or you avoided it altogether?’

  3. (c) ‘Have you ever had an unreasonable fear of being alone in your own home?’

If positive, these screening questions were followed with questions pertaining to onset, recency, associated anxiety symptoms and level of interference (including limits on being able to travel or leave home). In order to meet DIS/DSM–III–R criteria for agoraphobia, respondents had to endorse at least one of the screening questions, as well as at least one associated anxiety symptom (specifically dizziness, palpitations, nausea/vomiting, feeling of loss of control of bodily functions, or derealisation) and interference. Again, the nature of the fear was not directly assessed, only the typical situations in which such fear was likely to occur.

Psychiatrists made agoraphobia diagnoses according to DSM–III–R criteria, using the SCAN. Agoraphobic fears were grouped together, with the following six probes: ‘being in a public place when alone, open spaces, empty streets’, ‘crowds, shops, theatres – places with no easy exit’, ‘travelling alone – buses, trains, planes’, ‘going out alone – being alone away from home’, ‘collapsing while alone or with no help near’ and ‘being alone indoors’. The SCAN glossary describes agoraphobia as anxiety related to being in such situations, lessened in the presence of a trusted companion. The anxiety is related to difficulty escaping quickly (feeling trapped) or leaving without embarrassment, or fear of being incapacitated, with no help near. Thus, psychiatrists administering the SCAN assessed the nature of the fears, not just the situations in which they occurred.

Defining incident DIS/DSM–III–R agoraphobia

In the follow-up sample, 221 cases of lifetime DIS/DSM–III agoraphobia were identified at wave 1 (1981); in these cases the individuals were considered not at risk for incidence of the disorder. Of the remaining participants, 1557 were considered at risk for development of the disorder during the 13 years of follow-up, and 140 had missing data. Incident cases for this study were those who were at risk and met criteria for lifetime DSM–III–R agoraphobia at wave 3 (1993–1996). Participants with incident DIS/DSM–III agoraphobia at wave 2 (1982, n=3) were considered new cases only if they met DSM–III–R criteria at wave 3 as well (n=1). Given the multiwave nature of the study, there was a potential for discrepancies in timing of onsets (Reference Rubio-Stipec, Freeman and RobinsRubio-Stipec et al, 1992). Seventeen respondents with incident DSM–III–R agoraphobia reported no disorder-level symptoms in the first wave but, at followup, reported the onset of their earliest related fears as before 1981. It should be noted that the DIS–III–R did not assess age at onset of associated symptoms or interference, so these respondents could have had agoraphobia-related fears without meeting full criteria for agoraphobia until the follow-up period. Consistent with this, we found that more than half of these individuals (9 out of 17) reported ‘subthreshold’ DIS/agoraphobia-related fears in 1981. An additional three people reported that both the onset and offset of their fears occurred before 1981. All 20 were considered incident cases (in effect, giving priority to the time of assessment data and assuming errors in recall for the three respondents mentioned above). We conducted additional analyses in which these three cases were excluded, and there was no substantive difference in results. There were also slight differences in the screening questions for DIS/DSM–III–R agoraphobia; that is, it was conceivable that participants with phobias of riding in cars or trains were missed with the DIS/DSM–III interview and incorrectly classified as incident DIS/DSM–III–R cases. However, we found that incident cases of DIS/DSM–III–R agoraphobia respondents who endorsed items containing these fears were, if anything, less likely to report onset before 1981, compared with those who endorsed items containing the same situations in both interviews (further information available from the author on request).

Statistical analysis

A weighted cumulative incidence proportion was calculated with an elaboration of the Woodbury down-weighting procedure (Reference Kessler, Folsom, Royall, Eaton and KesslerKessler et al, 1985). This procedure was developed for the ECA programme to ensure that parameter estimates were accurate. Weighting, in this case, corrects the parameter estimate by the probability of selection into the sample; also, it adjusts for non-response to replicate the target population of survivors, according to age, ethnicity and gender categories. Putative baseline risk factors, including demographic factors and lifetime psychiatric diagnoses (as recorded in 1981), were examined in relation to subsequent development of agoraphobia. Baseline agoraphobia (with and without a history of spontaneous panic attacks) and other Axis I conditions were also examined in relation to subsequent development of panic disorder. Univariate and adjusted odds ratios were generated in logistic regression analyses.

RESULTS

Incidence of agoraphobia

There were 41 new cases of DIS/DSM–III–R agoraphobia identified among the 1557 participants at risk. Of these, 14 (34%) reported fears of being in a crowd or standing in line; 10 (24%) reported fears of riding on trains or buses, planes or in a car; 14 (34%) reported fears of crossing a bridge; 11 (27%) reported fears of being alone away from home and 11 (27%) reported fears of being alone at home. The unweighted 13-year cumulative incidence proportion of DIS/DSM–III–R agoraphobia is estimated at 2.6 per 100 persons at risk. The weighted 13-year cumulative incidence proportion is estimated at 2.4 per 100 persons at risk. These estimates correspond to an annual incidence rate of approximately 2 per 1000. The mean age at onset of agoraphobia-related fears for these incident cases was 21.2 years (s.d.=16.8).

Baseline demographic characteristics and incident agoraphobia

The 41 respondents with incident DIS/DSM–III–R agoraphobia were compared with the 1516 respondents who were at risk but did not develop agoraphobia. Younger age, female gender, African American ethnicity and having never married (at baseline, 1981) were statistically significant predictors of incident agoraphobia in univariate models (Table 1). The odds ratio for incident agoraphobia was more than twice as high in young adults (18–29 years old at baseline) compared with middle-aged adults (45–64 years old; there was no new case among those over 65 years old), and more than three times as high in women. When age group and gender were taken into account, ethnicity and marital status were not significantly related to incidence (e.g. as might be expected, younger participants were less likely to be married).

Table 1 Odds of first-onset agoraphobia over a 13-year period, given baseline (1981) demographic characteristics

New-onset agoraphobia1 Univariate Adjusted2
Present n Absent n OR (95% CI) OR (95% CI)
Age, years
    18-29 21 508 1.0 1.0
    30-44 14 455 0.7 (0.4-1.5) 0.7 (0.4-1.4)
    45-64 6 385 0.4 (0.2-0.9)* 0.3 (0.1-0.8)*
    65-86 0 168
Gender
    Female 34 900 3.3 (1.5-7.5)* 3.6 (1.6-8.2)*
    Male 7 616 1.0 1.0
Ethnicity
    White 20 966 1.0 1.0
    African American 21 497 2.0 (1.1-3.8)* 1.6 (0.8-2.9)
    Other 0 53
Education3
    Up to grade 8 2 126 0.7 (0.2-3.6) 1.5 (0.3-7.8)
    Grades 9-11 14 378 1.7 (0.7-4.2) 1.9 (0.8-4.7)
    Grade 12 16 504 1.5 (0.6-3.5) 1.4 (0.6-3.3)
    More than grade 12 8 377 1.0 1.0
Marital status3
    Married 13 701 1.0 1.0
    Widowed 1 143 0.4 (0.0-2.9) 0.6 (0.1-5.0)
    Separated 6 128 2.5 (0.9-6.8) 2.0 (0.7-5.3)
    Divorced 3 143 1.1 (0.3-4.0) 1.0 (0.3-3.5)
    Never married 18 400 2.4 (1.2-5.0)* 1.9 (0.9-4.3)
Annual household income3
    Up to $4999 8 191 4.6 (0.6-38) 3.8 (0.4-31)
    $5000-9999 5 223 2.5 (0.3-22) 2.4 (0.3-21)
$10 000-14 999 7 252 3.1 (0.4-25) 2.6 (0.3-22)
    $15 000-19 999 4 199 2.2 (0.2-20) 2.1 (0.2-20)
    $20 000-34 999 9 417 2.4 (0.3-19) 2.3 (0.3-18)
    > $35 000 1 111 1.0 1.0

Baseline Axis I disorders and incident agoraphobia

In univariate analyses, participants with lifetime DIS/DSM–III major depression, spontaneous panic attacks (not cued by phobic stimuli), panic disorder and other phobias at baseline (i.e. in 1981) were significantly more likely to develop agoraphobia over the follow-up period, compared with those without these conditions at baseline (Table 2). By far the strongest predictor of incident agoraphobia was baseline panic disorder (unadjusted OR=12, as opposed to odds ratios of about 3–4 for the other significant Axis I predictors). The relationships between baseline major depression or spontaneous panic attacks and incident agoraphobia were no longer statistically significant when age group and gender were taken into account. Although baseline alcohol use disorders did significantly predict onset of agoraphobia when these demographic factors (particularly gender) were taken into account (women were less likely to have baseline alcohol use disorders), this relationship was not significant when baseline comorbid conditions were also taken into account (i.e. panic disorder and other phobias).

Table 2 Odds of first-onset agoraphobia over a 13-year period, given baseline (1981) lifetime Axis I disorders

Lifetime Axis 1 disorder at baseline1 First-onset agoraphobia2 Univariate Adjusted3 Adjusted4
Present n Absent n OR (95% C1) OR (95% C1) OR (95% C1)
Alcohol use disorder
    Present 7 172 1.6 (0.7-3.6) 3.1 (1.2-7.8)* 2.4 (0.9-6.2)
    Absent 34 1316
Drug use disorder
    Present 2 81 0.9 (0.2-3.8) 0.8 (0.2-3.3) 0.6 (0.1-2.7)
    Absent 38 1401
Major depression
    Present 4 50 3.1 (1.1-9.1)* 2.4 (0.8-7.2) 1.5 (0.4-5.3)
    Absent 37 1439
Dysthymia
    Present 2 29 2.6 (0.6-11.2) 1.9 (0.4-8.5) 0.3 (0.0-3.6)
    Absent 39 1460
Panic disorder
    Present 3 10 12 (3.2-45)* 11 (2.8-46)* 8.3 (1.9-35)*
    Absent 37 1478
Spontaneous panic attack
    Present 3 30 3.9 (1.2-13)* 2.9 (0.8-10) 2.1 (0.6-7.8)5
    Absent 37 1457
Other phobia
    Present 13 227 2.6 (1.3-5.1)* 2.3 (1.2-4.5)* 2.2 (1.1-4.4)*
    Absent 28 1262

Baseline agoraphobia and other Axis I disorders, and incident panic disorder

As reported previously by Eaton et al (Reference Eaton, Anthony and Romanoski1998), there were 35 new cases of panic disorder during the follow-up period out of 1731 at risk; demographic risk factors included female gender, younger age and White ethnicity. Significant baseline (1981) Axis I predictors of incident panic disorder included lifetime DIS/DSM–III drug use disorder, major depression, dysthymia, agoraphobia, and agoraphobia without a history of spontaneous panic attacks (last OR=3.9 95% CI 1.8–8.4) (Table 3). However, there was a substantial degree of comorbidity among baseline disorders. When baseline comorbidity was taken into account, agoraphobia was the only significant predictor of incident panic disorder.

Table 3 Odds of first-onset panic disorder over a 13-year period, given baseline (1981) lifetime Axis I disorders

Lifetime Axis I disorder at baseline1 First-onset panic disorder2 Univariate Adjusted3 Adjusted4
Present n Absent n OR (95% CI) OR (95% CI) OR (95% CI)
Alcohol use disorder
    Present 5 195 1.2 (0.5-3.3) 2.5 (0.9-7.1) 1.7 (0.6-5.1)
    Absent 30 1471
Drug use disorder
    Present 7 96 4.1 (1.7-9.6)* 3.9 (1.6-10)* 2.6 (1.0-7.0)
    Absent 28 1564
Major depression
    Present 7 66 6.1 (2.6-14)* 3.7 (1.5-9.2)* 2.2 (0.8-5.9)
    Absent 28 1602
Dysthymia
    Present 4 33 6.4 (2.1-19)* 3.8 (1.2-12)* 2.4 (0.7-8.6)
    Absent 31 1635
Agoraphobia
    Present 11 169 4.1 (2.0-8.5)* 3.7 (1.7-7.9)* 2.9 (1.3-6.5)*
    Absent 24 1516
Agoraphobia without panic5
    Present 10 161 3.9 (1.8-8.4)* 3.5 (1.6-7.8)* 2.7 (1.2-6.1)*,6
    Absent 24 1516
Other phobia
    Present 4 231 2.5 (1.3-5.0) 0.7 (0.2-2.2) 1.1 (0.4-3.4)
    Absent 31 1436

Limiting to psychiatrist-confirmed agoraphobia

Twenty-seven of the participants with incident DIS/DSM–III–R agoraphobia were seen by psychiatrists. Masked to DIS diagnoses, psychiatrists rated 15 of these individuals as having substantial, unambiguous lifetime agoraphobic phenomena, although the psychiatrists thought 6 of these 15 cases were below the rigorous SCAN diagnostic threshold (in all 6 of these cases the individual had at least two agoraphobia-type fears). Of the remaining 12 cases, it appeared that 6 had been misclassified with the DIS (i.e. using the psychiatric interview as the standard); that is, their avoidances were understandable in terms of other kinds of fears. In the latter cases one person had a fear of flying, one had a fear of heights, and four had social and other fears (one was practically house-bound with fear of people; the rest had additional fears of enclosed spaces, being attacked or heights/bridges). In the final 6 cases, two people were assessed as unreliable informants, one young woman said that her physician had recommended she avoid stressful situations following possible transient ischaemic attacks, and three appeared to give discrepant answers to similar questions in the two interviews (i.e. the non-clinician-administered DIS and the psychiatrist-administered SCAN).

In addition, 26 participants at risk of DIS/DSM–III–R agoraphobia but without the DIS diagnosis were diagnosed as having agoraphobia by psychiatrists. Twelve of these participants endorsed DIS agoraphobia-related fears but did not endorse sufficient additional criteria for the diagnosis, and 10 appeared to provide discrepant answers to similar questions in the two interviews. In the remaining 4 cases it was possible that psychiatrists administering the SCAN had elicited symptoms not specifically addressed with the DIS: fear of shops and theatres, and fear of collapsing with no help nearby.

For the following analyses, we defined psychiatrist-confirmed incident agoraphobia as present if the participant met criteria for incident DIS/DSM–III–R agoraphobia and was diagnosed by a psychiatrist as having lifetime agoraphobia at follow-up (n=9). We excluded discrepant cases (with unconfirmed incident DIS/DSM–III–R agoraphobia, n=18; or psychiatrist-diagnosed agoraphobia without the incident DIS diagnosis, n=26), so the comparison group was also slightly smaller than in the previous sections (n=1490). The pattern of predictors for psychiatrist-confirmed incident agoraphobia was similar to that reported above; however, given the restricted number of cases, statistical significance was not usually present. Nevertheless, the expected relationship between baseline DIS/DSM–III panic disorder and psychiatrist-confirmed incident agoraphobia was highly significant (OR=20, 95% CI 2.3–180). Given the relatively small number of cases here, we did not think it wise to include covariates in the logistic regression models. We also conducted additional analyses of predictors of ‘incident’ psychiatrist-diagnosed DSM–III–R agoraphobia; cases were classified as incident if they met lifetime criteria at follow-up but did not meet criteria for DIS/DSM–III agoraphobia in 1981 (n=35/667; unconfirmed DIS cases were excluded). As with incident DIS/DSM–III–R agoraphobia, significant predictors included baseline young adult age, female gender, spontaneous panic attacks and panic disorder (further information available from the author on request).

The good concordance between DIS/DSM–III–R and psychiatrist-diagnosed (SCAN) incident panic disorder has been reported elsewhere (Reference Eaton, Anthony and RomanoskiEaton et al, 1998). For the purposes of the current analyses, we defined psychiatrist-confirmed baseline agoraphobia as present if DIS/DSM–III agoraphobia was present in 1981 and a psychiatrist made the diagnosis of lifetime agoraphobia at follow-up (n=15, of whom 11 had no history of DIS/DSM–III spontaneous panic attacks at baseline). We excluded participants with unconfirmed baseline agoraphobia (n=97). Psychiatrist-confirmed baseline agoraphobia, with and without a history of spontaneous panic attacks, was a strong predictor of incident DIS/DSM–III–R panic disorder (OR=16, 95% CI 3.2–78 and OR=15, CI 3.1–75 respectively); again, given relatively small numbers, we did not include covariates in these models.

DISCUSSION

Panic and agoraphobia

A primary goal of this study was to determine how spontaneous panic attacks/panic disorder and agoraphobia relate longitudinally. Consistent with Klein's cogent argument regarding the unconditioned stimulus property of spontaneous panic attacks causing a conditioned avoidance response (Reference KleinKlein, 1980), several previous retrospective clinical studies (reviewed by Reference Craske, Widiger, Frances and PincusCraske, 1996; Reference Fava and MangelliFava & Mangelli, 1999) and the one previous community study of incident agoraphobia we know of (Reference Eaton and KeylEaton & Keyl, 1990), baseline spontaneous panic attacks (especially frequent ones, i.e. DSM–III panic disorder) strongly predicted new-onset agoraphobia. This finding was not surprising. However, the finding that baseline agoraphobia without spontaneous panic attacks also predicted first-onset panic disorder is clearly inconsistent with Klein's theory. In fact, in the present study, baseline agoraphobia without panic was the only baseline Axis I disorder studied that significantly predicted incident panic disorder when baseline comorbidity was taken into account.

Our results are consistent with previous retrospective reports in which patients with both agoraphobia and panic sometimes reported agoraphobia preceding panic (e.g. Reference Fava, Kellner and ZieleznyFava et al, 1988; Reference Argyle and RothArgyle & Roth, 1989; Reference Lelliott, Marks and McNameeLelliott et al, 1989). Given that the causal relationship between spontaneous panic attacks and agoraphobia does not appear as straightforward as Klein's theory suggests, we suggest that DSM–V should de-emphasise the implied one-way causal relationship from spontaneous panic to agoraphobia and make agoraphobia itself a stand-alone diagnosis again, as in ICD–10 (World Health Organization, 1993). That is, although panic does appear to be a potent risk factor for agoraphobia, agoraphobia also appears to be a risk factor for panic disorder.

Other recent epidemiological research is relevant to Marks's argument that agoraphobia should be a stand-alone diagnosis, like other phobias, often but not always associated with panic (Reference MarksMarks, 1987a ). Three cross-sectional community studies that employed rigorous clinical methods found that agoraphobia was sometimes present in people with no history of panic: Wittchen et al (Reference Wittchen, Reed and Kessler1998) found that many adolescents and young adults had clinician-confirmed agoraphobia but no history of panic; Hayward et al (Reference Hayward, Killen and Taylor2003) found that rigorously defined agoraphobic fear and avoidance, although relatively rare in a sample of high-school students, was usually not associated with a history of panic attacks; and Faravelli et al (Reference Faravelli, Abrardi and Bartolozzi2004), who – like many in the USA – were sceptical that agoraphobia without a history of panic existed, found several such cases in their mostly adult sample. Epidemiologists have long noted that one reason clinicians rarely encounter patients with agoraphobia but without panic is that panic itself influences treatment-seeking. Two epidemiological studies have provided empirical evidence that individuals experiencing agoraphobia without panic are less likely to seek psychiatric care (Reference Wittchen, Reed and KesslerWittchen et al, 1998; Reference Andrews and SladeAndrews & Slade, 2002); however, these studies did not find that such individuals never seek care, so it is important that clinicians recognise agoraphobia in the absence of panic. In the USA at least, many younger clinicians tend to consider the diagnosis of agoraphobia only when their patients report panic attacks – this is understandable as a result of changes in recent versions of DSM. Diagnostic criteria clearly influence the conceptualisation of psychiatric conditions, and this is not limited to the clinical setting: if researchers conceptualise agoraphobia only as avoidance of certain situations because of fear of panic, the suffering of many people with agoraphobia is ignored.

One reason Marks contended that agoraphobia is a syndrome is that agoraphobic fears have repeatedly been found to cluster together within individuals, separate from other types of fears (Reference MarksMarks, 1987b ; Reference Arrindell, Eisemann and RichterArrindell et al, 2003). Further support for allowing agoraphobia to stand apart from panic comes from a recent study of data from the National Comorbidity Survey (Reference Kessler, McGonagle and ZhaoKessler et al, 1994), in which Cox et al (Reference Cox, McWilliams and Clara2003) found that agoraphobic fears clustered together within individuals whether or not they had a history of panic attacks.

Hettema et al (Reference Hettema, Prescott and Myers2005) have recently provided evidence that genetic factors in common may predispose to both agoraphobiaphobia agora and panic disorder, in a cross-sectional multivariate twin study of common anxiety disorders. A genetically informative bivariate longitudinal study of panic and agoraphobia could potentially provide additional information about aetiological mechanisms, in that there may be direct causal paths from the experience of panic to agoraphobia (Reference KleinKlein, 1980) and/or vice versa (Reference Fava and MangelliFava & Mangelli, 1999). Regardless of specific aetiological mechanisms, though, clinicians should keep in mind that agoraphobia without panic appears to be at least a marker of risk for later-onset panic disorder.

Agoraphobia incidence and other predictors

Eaton & Keyl (Reference Eaton and Keyl1990) estimated the annual first incidence of DIS/DSM–III agoraphobia at 22 per 1000 population. We believe our estimate of DSM–III–R agoraphobia incidence (approximately 2 per 1000 per year) is likely to be a conservative one for two reasons. First, the 13-year period of risk probably affected recall for some agoraphobic symptoms at follow-up. Second, many of the sample who might have been at risk and developed agoraphobia over the follow-up period were not diagnosed with DIS/DSM–III–R agoraphobia (the number of people apparently misclassified as having agoraphobia with the DIS was smaller than the number of people apparently misclassified as not agoraphobic). Our findings regarding demographic predictors of agoraphobia (i.e. younger age and female gender) were in agreement with those of Eaton & Keyl (Reference Eaton and Keyl1990).

We found that other baseline phobias also predicted onset of agoraphobia, although these were a much weaker predictor than baseline panic disorder. The difference in strength of this relationship, and the fact that baseline depressive disorders were not significantly related to onset of agoraphobia (at least when demographic correlates were taken into account), suggest a somewhat specific longitudinal relationship between panic disorder and agoraphobia in adults, beyond membership in a larger group of ‘internalising’ or ‘neurotic’ disorders (Reference KruegerKrueger, 1999; Reference TyrerTyrer, 1985).

Strengths and limitations of the study

This study's strengths include the use of a longitudinally assessed population-based cohort, with psychiatrist interviews to determine the possible effects of misclassification. To our knowledge, this is the first comprehensive report of longitudinal associations between panic and agoraphobia using a prospective design.

We note the following caveats. First, since the psychiatric interviews were conducted at follow-up, it is possible that some individuals classified here as having baseline (1981) DIS/DSM–III agoraphobia without panic and subsequent first-onset DIS/DSM–III–R panic disorder would have been found to have a history of baseline panic with a thorough clinical assessment of lifetime symptoms at baseline. However, given results of a previous clinical reappraisal of DIS/DSM–III agoraphobia without panic, the most likely form of misclassification by far involved diagnosing simple (specific) phobias as DIS/DSM–III agoraphobia (Reference Horwath, Lish and JohnsonHorwath et al, 1993). Also, participants who had mild agoraphobia at baseline and developed first-onset panic disorder during the follow-up period could have had worsening of agoraphobia symptoms after the onset of panic, thus making them more likely to be diagnosed with lifetime agoraphobia by psychiatrists at follow-up. This is consistent with our and others’ clinical experience; for example, some patients report always being afraid of situations such as driving on express-ways or through tunnels, but their agoraphobia symptoms become worse and generalise further after the onset of panic in those situations: see Fava & Mangelli (Reference Fava and Mangelli1999) for a review. Second, we focused on time-of-interview data, ignoring the specific timing of onset of syndromes between interview waves (e.g. there were seven participants with first onset of both panic disorder and agoraphobia during the follow-up period). We chose to do this because longitudinally collected time-of-interview data are less susceptible to recall bias, and they are a particular strength of this dataset. Third, since the psychiatric interviews were conducted at follow-up, and only on a selected subset of our sample, it was not possible to adjust incidence rates accurately using this method. Fourth, the relatively small number of cases with psychiatrist-confirmed incident DIS/DSM–III–R agoraphobia precluded statistical confirmation of baseline predictors other than panic disorder. Nevertheless, for most cases in which the diagnosis of incident DIS/DSM–III–R agoraphobia was not confirmed by psychiatrists, the issue was not chiefly frank misclassification (e.g. the symptoms were better conceptualised as another phobia), but rather a combination of stricter thresholds in the psychiatric interviews or inconsistent responses by the participant concerned to similar questions in the two interviews (thus, DIS/DSM–III–R agoraphobia appears to resemble more closely what clinicians call ‘agoraphobia’ than did DIS/DSM–III agoraphobia). We gain further confidence in our reported risk factors since we found similar results in predictors of psychiatrist-diagnosed ‘incident’ agoraphobia.

Clinical Implications and Limitations

CLINICAL IMPLICATIONS

  1. Agoraphobia without panic appears to be a risk factor, or at least a marker of risk, for the onset of panic.

  2. Clinicians should be aware that agoraphobia can exist without a history of panic, despite what is implied in DSM–IV.

  3. Young women are at greatest risk for the onset of agoraphobia.

LIMITATIONS

  1. Non-clinician-administered, fully structured interviews such as the Diagnostic Interview Schedule sometimes misclassify people with other phobias as having agoraphobia.

  2. Psychiatrists only performed (lifetime) diagnostic interviews at follow-up.

  3. It was not possible to adjust incidence rates using data obtained from psychiatrists.

Acknowledgements

The National Institute of Mental Health (grants R01-MH47447, R01-MH50616 and K23-MH6454) supported this study.We thank the many individuals who have taken part over the years as administrators, trainers, interviewers and participants in the Baltimore Epidemiologic Catchment Area Study.

Footnotes

Declaration of interest

None.

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Figure 0

Fig. 1 Overview of the Baltimore Epidemiologic Catchment Area (ECA) Study. DIS, Diagnostic Interview Schedule; SCAN, Schedules for Clinical Assessment in Neuropsychiatry.

Figure 1

Table 1 Odds of first-onset agoraphobia over a 13-year period, given baseline (1981) demographic characteristics

Figure 2

Table 2 Odds of first-onset agoraphobia over a 13-year period, given baseline (1981) lifetime Axis I disorders

Figure 3

Table 3 Odds of first-onset panic disorder over a 13-year period, given baseline (1981) lifetime Axis I disorders

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