This document provides an overview of Acute and Transient Psychotic Disorder (ATPD). It discusses the history and evolution of ATPD from early descriptions in the late 19th century to its inclusion as a diagnostic category in ICD-10 in 1992. The document outlines the ICD-10 diagnostic criteria for ATPD and reviews several landmark studies that helped establish ATPD as a separate diagnostic category from schizophrenia and affective disorders. It also discusses cultural variants of brief psychotic episodes and debates around classifying certain culture-bound syndromes as ATPD.
2. LAYOUT
1. Introduction
2. History and evolution of ATPD
3. ICD-10 diagnostic criteria
4. Epidemiology of ATPD
5. Course and outcome
6. Treatment of ATPD
7. Issues with nosology
8. Future of ATPD as a diagnostic criteria
9. Conclusion
3. INTRODUCTION
Acute and transient Psychotic Disorder (ATPD) as a descriptive entity
was recognized in ICD-10 in 1992
Included under psychotic disorder (F23) as a three-digit code
“Nomenclature of these acute disorders is as uncertain as their nosological
status”
“Psychotic disorder” is used as a term of convenience”
The fact remains that systematic clinical information that would guide the
classification of acute psychotic states is not yet available”
4. HISTORY AND EVOLUTION OF ATPD
1876 German Psychiatist Karl westphal described paranoia acuta
1890 Meynert repeated the clinical description but named the condition
“amentia”
Sigmund Freud chose this type of acute delusion with hallucinations for
his psychoanalytic conception of psychosis
100 Years
5. The existence of acute psychoses has been described by almost
all important authors of the Pre-Kraepelinian period
Meynert in 1889 first described transient amentia (amnesia with
a sad spirit)
Psychotic confusional state
Good prognosis
Emil Kraepelin’s dichotomy of dementia praecox and manic-
depressive insanity
Kraepelin based this dichotomy mainly on symptomatology,
course and longitudinal outcome
(Kraepelin, 1893, 1896, 1899)
HISTORY OF
ACUTE PSYCHOSIS
6. KRAEPELIN’S DICHOTOMY
Kraepelin knew of Brief and Acute Psychoses
Could not be allocate it either to schizophrenia or to affective
disorder
Such disorders could cause severe doubts regarding the
reliability of his dichotomy (Kraepelin, 1920)
Kraepelin allocated them either to manic-depressive insanity or to
dementia praecox
Majority of Brief and Acute Psychoses were allocated by
Kraepelin to the manic-depressive insanity group
7. JUGGLE OF ACUTE PSYCHOSIS
GROUP TO SCHIZOPHRENIA
Kraepelin’s dichotomic system was
reformed by Eugen Bleuler (1911)
Created the group of schizophrenias
Problem of the brief, acute, transient and
good prognosis psychoses persisted
Acute psychosis category was moved
from Kraepelin’s manic-depressive
insanity to Bleuler’s schizophrenia
A tradition which is still going on
8. Psychotic Symptoms, Mood Symptoms, Cognitive symptoms,
Aggression, Poor insight, excitement, Decreased self care,
Socio-occupational dysfunction
Acute vs Insidious Onset
Continuous Vs Episodic vs Remitting Course
Good Vs Bad Prognosis
KRAEPELIN’S
DICHOTOMY
Dementia
praecox
Manic-
Depressive
Psychosis
Not schizophrenia
Not an affective disorder
Not a schizoaffective
disorder
Good Prognosis
Eugen
Bleuler
Schizophrenia
9. OPPOSITION TO KRAPELINIAN DICHOTOMY
France:
Bouffee Delirante
Germany:
Motility Psychosis
Cycloid Psychosis
Scandinavia:
Psychogenic psychosis
Reactive Psychosis
America:
Schizophreniform
Psychosis
Remitting
Schizophrenia
Japan :
Atypical Psychosis
Africa :
Acute Primitive
Psychosis
Acute Paranoid
Psychosis
Transient Psychosis
West Indies :
Acute Psychotic
Reaction
India :
Acute Psychoses of
Uncertain Origin
Hysterical Psychosis
Acute Psychosis
without Antecedent
Stress
Acute Schizophrenic
Episode
10. THE CYCLOID PSYCHOSES- GERMANY
It was created and developed by three Karls’:
1. Carl Wernicke
2. Karl Kleist
3. Karl Leonhard
Focused mainly on clinical and on genetic findings
Demanded a separation from Kraepelin’s manic-depressive insanity
Fish (1964) introduced the concept of cycloid psychosis to English
speaking countries
(Acute and transient psychosis by Andreas Marneros and Frank pillmann,2004)
11. BOUFFEE DELIRANTE- FRANCE
1. It can be regarded as the French root of ATPD and Brief Psychoses
2. Valentin Magnan (1835–1916)
3. The modern concept of bouffee delirante is based on operational criteria
like:
1. Sudden onset
2. Specific symptomatology
3. Evolution of the disorder
4. Retained the category bouffee delirante as an independent mental
disorder
12. ACUTE PSYCHOSIS - INDIA
Wig and Singh extracted psychiatric categories from the APA DSM II
relevant for use in India
They argued for the category of acute psychosis for brief episodes
precipitated by stress which does not fit into the Kraepelinian
dichotomy
They sub-classified acute psychosis into:
1. Confusional
2. Paranoid hallucinatory
3. Schizoaffective
4. Hysterical psychosis (K. S. Jacob, 2016)
13. REACTIVE/PSYCHOGENIC PSYCHOSES
Basic concept was developed by Karl Jaspers
Very strong tradition mainly in Scandinavia
The first monograph was written by August Wimmer
The concept developed by Wimmer is based on Jaspers General
Psychopathology
(Acute and transient psychosis by Andreas Marneros and Frank pillmann,2004)
14. TOWARDS A PERMANENT PLACE IN
INTERNATIONAL CLASSIFICATION
What happened to individual national concepts of acute
psychosis?
How did they find a permanent place in international
classification?
Which landmark studies identified them as a separate
category?
15. INTERNATIONAL PILOT STUDY OF
SCHIZOPHRENIA (IPSS) (1968-70)
This was a nine-country study on schizophrenia led and
funded by WHO, with the main aims:
1. Whether schizophrenia existed in different parts of the
world?
2. What were the common/differing clinical presentations?
3. What was the course and outcome among different
cultures?
16. INTERNATIONAL PILOT STUDY OF
SCHIZOPHRENIA (IPSS) (1968-70)
Agra was the center from India
The main findings:
1. Course and outcome in developing world was better than
developed countries
2. 25% of people diagnosed to have schizophrenia had only one
episode and good outcome
IPSS raised questions like whether these subjects with good outcome
had a:
Separate psychosis?
Were they part of the schizophrenia group?
17. Determinants Of Outcome Of Severe Mental Health
Disorders (DOSMED) (1978-80)
Designed to study:
1. First onset psychosis
2. Incidence of schizophrenia
3. Findings related to acute psychosis
Chandigarh was the Indian center
The incidence of “broadly defined schizophrenia” was 10 times higher in
the developing world than in the developed countries as compared to
“narrowly defined schizophrenia”
These patients also exhibited a benign course at two-year follow-up
Possibility of psychotic states that were not yet clearly identified
18. THE CROSS-CULTURAL STUDY OF ACUTE
PSYCHOSIS (CAP) (1980-82)
The study aimed to:
1. Differentiate ATPD from schizophrenia and manic depressive
psychosis
2. Understand its relationship with psychological and physical stress
Main findings included:
1. 41.2% of patients had symptoms of schizophrenia
2. 20% had Affective symptoms
3. 35.3% had “other psychoses”
4. 41.7% reported stress at onset
5. Two-thirds of the subjects remained without relapse at one year
follow-up
19. INDIAN COUNCIL OF MEDICAL RESEARCH’S
MULTICENTRE STUDY OF ACUTE PSYCHOSIS
Bikaner, Goa, Patiala and Vellore
It was found that:
1. 35% of were Schizophrenia
2. 25% were MDP
3. 40% as non-organic psychosis as per ICD-9
4. 52% of cases of acute psychosis could not be categorized into any of
the categorical diagnosis
20. RECOGNITION OF ACUTE PSYCHOSIS
AS A SEPARATE CATEGORY
These studies provided evidence of a non-affective, non
schizophrenia psychosis with remission and good outcome
Inclusion of acute and transient Psychosis as a separate
category in ICD-10 in 1992
21. CLINICAL DESCRIPTION: PSYCHOPATHOLOGY
The heterogeneous group of acute and transient psychotic disorders
Characterized by three typical features in the descending order of
priority:
1. An acute onset (within 2 weeks) as the defining feature of the whole
group
2. Presence of typical syndromes
3. Presence of associated acute stress
22. ACUTE ONSET
Acute onset is defined as a change from a state without psychotic
features to a clearly abnormal psychotic state, within a period of 2
weeks or less
There is some evidence that acute onset is associated with a good
outcome
More abrupt the onset better the outcome
It is therefore recommended that whenever appropriate, abrupt onset
(within 48 hours or less) be specified
23. THE TYPICAL SYNDROMES
1. Rapidly changing and variable state called "polymorphic“
2. Typical schizophrenic symptoms
3. Differentiated on the basis of first rank Symptoms of schizophrenia
24. ASSOCIATED ACUTE STRESS
Traditional linkage of stress with acute psychosis
Substantial proportion of acute psychotic disorders arise without
associated stress
First psychotic symptoms should occur within about 2 weeks of one or
more events that would be regarded as stressful to most people
Typical events would be bereavement, unexpected loss of partner or
job, marriage or the psychological trauma of combat, terrorism, and
torture
Long-standing difficulties or problems should not be included
25. F23.0 Acute polymorphic psychotic disorder
without symptoms of schizophrenia
The delusional themes are varied and include grandeur, persecution,
influence, possession, body transformation (depersonalization),
derealization or world alteration
These themes change with time and may combine
Consciousness fluctuates with the delirious convictions and changes of
emotion
Karl Jaspers - ‘first delirious experience‘ which is a “dreamlike state”
The criteria for manic episode, depressive episode or schizophrenia are not
fulfilled
26. F23.0 Acute polymorphic psychotic disorder
without symptoms of schizophrenia
Duration of less than a month
In most cases recovery occurs within a few weeks or months
If resolution of the symptoms has not occurred after 3 months, the
diagnosis should be changed to persistent delusional disorder (F22) or
non-organic psychotic disorder (F28)
27. F23.1 Acute polymorphic disorder with symptoms
of schizophrenia
This diagnostic category combines the symptoms of acute polymorphic
psychotic disorder with some typical symptoms of schizophrenia (F20)
present for most of the time
It can be a provisional diagnosis, which is changed to schizophrenia if
the criteria of schizophrenia persist more than a month
28. F23.2 Acute schizophrenia-like psychotic disorder
This acute psychotic disorder lasts for less than a month and is mostly
schizophrenic
The polymorphic psychotic symptoms are stable
The duration criterion is the most important
This category is a provisional diagnosis
In ICD-10 if the first episode lasts for more than a month, it has to be
considered as an acute onset of schizophrenia
29. F23.3 Other acute predominantly delusional
psychotic disorders
The main clinical features of this category are delusions and
hallucinations
Do not meet the criteria for schizophrenia
The duration of this psychotic episode must be less than 3 months
If the persecutory delusions persist for more than 3 months, the
diagnosis changes to persistent delusional disorders (F22)
Auditory hallucinations persist for more than 3 months, the diagnosis is
changed to other non-organic psychotic disorders (F28)
30. F23.8 Other acute and transient psychotic disorders
1. Any other acute psychotic disorders that are unclassifiable under
any other category in F23
2. States of undifferentiated excitement should also be coded here if
more detailed information about the patient's mental state is not
available
F23.9 Acute and transient psychotic disorder
unspecified
(brief) reactive psychosis NOS
32. Year Term
Given By
Historic Term Current Terminology
1876 Westphal Akute primare Verruckheit
paranoia acuta
Other acute predominantly
delusional psychotic disorder
1890 Meynert Amentia
1895 Magnan
and
Legrain
Bouffee Delirante Acute polymorphic psychotic
disorder without symptoms of
schizophrenia
1899 Kraepelin Dementia praecox Schizophrenia
1909-
1913
Kraepelin Paranoia Persistent delusional disorder
1911 Bleuler Acute onset schizophrenia Acute Polymorphic psychotic
disorder with symptoms of
schizophrenia
Acute schizophrenia like psychotic
disorder
33. Year Term Given
By
Historic Term Current Terminology
1916 Wimmer Psychogenic
psychosis
Other acute predominantly psychotic
disorder
1924 Mayer-
Gross
Oneroide
erlebnisform
Acute Schizophrenia like psychotic
disorder
1933 Kasanin Acute schizoaffective
psychoses
Schizoaffective disorder
1939 Langfeldt Schizophreniform
states
Acute schizophrenia like psychotic
disorder
1954 EY Bouffees Delirante
et psychoses
hallucinatoires aigues
Acute polymorphic psychotic disorder
without symptoms of schizophrenia
1961 Leonhard Cycloid psychoses Acute polymorphic psychotic disorder
without symptoms of schizophrenia
34. CULTURAL VARIANTS
Other forms of acute psychoses have been observed with high
prevalence in Asia, Africa, and Latin America
These brief psychotic episodes are culture-bound syndromes
Immediate precipitating stress or life events
There is disorganized behaviour, delusions, thought disorders,
confusion, and mood disorders
Full recovery and no relapse in a 1-year follow-up
ICD-10 does not suggest category of ATPD
35. CULTURE BOUND SYNDROME VS
PSYCHOTIC DISORDER
Culture-bound syndromes should be classified as acute and transient
psychotic disorders (Mezzisch and Lin)
This is justified only for a very few such as:
1. amok (dissociative episode with persecutory ideas and aggressive
behaviour from Malaysia)
2. shin-byung (Korean dissociation and possession)
3. spell (trance state in southern United States)
36. CULTURE BOUND SYNDROME AS NEUROSIS
ICD-10 includes the two Malaysian syndromes koro and latah as well as
Dhat (India) in (F48.8) Other specified neurotic disorders
Short-lived psychotic episodes are expressions of overcharged
mechanisms of defence or of individual psychological fragility
The brief psychosis is an understandable development of the psychic life
of the subject and has a cathartic effect
37. BRIEF PSYCHOTIC DISORDER OF DSM-5 AND
ATPD OF ICD-10
Brief Psychotic
Disorder
ATPD
Duration from
onset to full
remission of
psychotic episode
1 day to 1
Month
up to 3 months
exceptions
‘With Symptoms of Schizophrenia’ and
‘Acute Schizophrenia-like Psychotic
Disorder’
In these cases less than 1 month
Full development
Of the Syndrome
Not Specified Within 2 weeks
Defining
Symptomatology
Positive
Psychotic
Symptoms
Psychotic symptoms + Polymorphic
Symptoms
38. EPIDEMIOLOGY OF ATPD
1. The Halle Study on Brief and Acute Psychoses (HASBAP) by
Andreas Marneros and Frank Pillmann
2. The Cairo study by Okasha and co-workers (1993)
3. The cohort study of Pondicherry, India by Sajith and co-workers
(2002) at JIPMER, Pondicherry, India
4. The cohort study of Chandigarh at PGI
5. The Danish Cohort Study
39. THE FREQUENCY OF ATPD
The frequency of Brief and Acute Psychoses is considerably higher in
developing countries
Frequency of subtypes of ATPD according to ICD-10:
1. Acute Polymorphic Psychoses- 67%
2. Acute Schizophrenia-like Psychoses - 26%
3. Other Acute Predominantly Delusional Psychoses - 2%
4. Other Acute and Transient Psychoses (F23.8) - 5%
Frequency of Subtypes of Acute Polymorphic:
1. Without Symptoms of Schizophrenia-50%
2. With Symptoms of Schizophrenia-50%
40. GENDER DISTRIBUTION
More frequent in women than in men
This constitutes an important difference to schizophrenia and to
schizoaffective disorders
AGE AT ONSET
Acute and Transient Psychotic Disorders may occur at any age
Peak in the mid thirties
Age at onset is higher than in schizophrenia
41. MENTAL DISORDERS IN THE FAMILY
In a major case control study found family history of ATP was three
times greater in first degree relatives(FDRS) of ATP
History of schizophrenia was seen in FDRs of those ATP patients who
had schizophrenic symptoms
These findings gave evidence that ATP is genetically distinct from
MDP
There is genetic overlap between ATP and schizophrenia and
schizophrenic symptoms
42. PREMORBID PERSONALITY
Assessment by ‘Big Five’ personality dimensions
No significant difference between ATPD patients and healthy controls
Bipolar Schizoaffective Disorder patients differ from mentally healthy
controls on two of five subscales-neuroticism and extraversion
Schizophrenia patients show pronounced differences from the mentally
healthy controls on three of five subscales: neuroticism, extraversion
and conscientiousness
43. ONSET AND DURATION OF EPISODE
Neither abrupt nor acute onset are specific for ATPD
Schizophrenia can have an acute onset and rarely an abrupt onset
The duration of the psychotic period as well as the duration of inpatient
treatment is significantly shorter in ATPD
Insidious onset tends to have a longer duration of the psychotic period
Tendency for patients with a precipitating life event to show a more
acute onset
44. PSYCHOPATHOLOGICAL ASPECTS OF
ATPD
The most crucial differences in phenomenology of ATPD:
1. Rapidly changing delusional topics
2. Rapidly changing mood
3. Anxiety
Significantly more frequently represented in ATPD
45. LONGITUDINAL COURSE OF ATPD
Relapse rates in ATPD are similar to those in controls with
Schizophrenia and BPAD
After 2.3 years one-half of the ATPD patients will experience a relapse
Patients with ATPD who experience a relapse usually have ATPD
episodes again
Affective and schizoaffective episodes during follow-up are also
common
(HALLE STUDY)
46. COURSE AND DIAGNOSTIC STABILITY
OF ATPD
Recurrence of psychotic episodes is common
Not as common as in schizophrenia or bipolar disorder
Over 15 years of follow-up:
1. 30% of ATPD patients experienced a single episode
2. 50% had an episodic-remitting course
3. 20% had a chronic course
Four studies in India have evaluated the diagnostic stability of ATPD
for a follow up period from 12-36 months
63-100% of patients retained their diagnosis of ATPD at follow-up
47. DIAGNOSTIC STABILITY IN INDIAN STUDIES
Thangadurai et al. while analyzing the medical records of all patients with
psychotic disorders found:
13.9% were diagnosed with acute psychosis
Mean duration of follow-up was 13.2 months
The diagnosis was revised to:
1. Affective disorder in 9.2%
2. Schizophrenia in 26.4%
3. 11.5% presented with recurrent episodes of acute psychosis
48. DIAGNOSTIC STABILITY OF ATPD
A Danish study covering 15 years of register data found a 39% stability
rate of ATPD
Majority of patients transitioning to diagnoses of schizophrenia or
affective disorders
60% of the total ATPD sample developing another psychiatric disorder by
their third admission
49. DIAGNOSTIC STABILITY OF ATPD
Diagnostic stability differs widely by diagnosis and length of
follow-up
A small study of first-episode psychotic patients in Iran found that
100% of those diagnosed with ICD-10 ATPD maintained the same
diagnosis over 12 months of follow-up
In a 15-year follow-up the diagnoses of ATPD, Schizophreniform and
brief psychotic disorder were unstable over time
50. DIAGNOSTIC STABILITY
DEVELOPING VS DEVELOPED NATIONS
In industrialized nations like Europe more than 50% of cases with ATPD
tend to change diagnosis into another category
In a review of 13 follow-up studies of ATPD:
Castagnini and Berrios noted that studies in developing settings
tend to show higher diagnostic stability and lower rates of relapse
than studies in western settings
51. PREDICTORS OF DIAGNOSTIC STABILITY
AND FAVOURABLE OUTCOME IN ATPD
1. Sudden onset
2. Female sex
3. Duration less than one month
4. Good premorbid functioning
5. Acute insomnia
52. DIAGNOSTIC STABILITY OF ATPD
Syndrome stability of ATPD is found to be located in the middle
between the high stability of schizophrenia and the low stability of
schizoaffective disorder
After exclusion of the Acute Schizophrenia-like Psychotic Disorders
from the group of ATPD 50% of the ATPD patients have a
‘monosyndromal’ course during the prospective follow-up of five years
53. OUTCOME
After 10 years of illness patients with ATPD in comparison to controls
with schizophrenia show:
1. Better global functioning
2. Less social disability
3. Fewer persisting alterations
4. Fewer negative and positive symptoms
5. Higher rates of heterosexual relationships
54. MANAGEMENT OF ATPD
Early hospitalization in order to make:
1. Careful clinical evaluation
2. To separate the patient from environment
3. To provide a reassuring setting
4. To prevent any suicidal or aggressive tendencies
Antipsychotic drugs are indicated
The choice of antipsychotic drug depends on the clinician's experience
and the clinical features
Benzodiazepines may be given to potentiate the action of the
neuroleptics
55. CONTINUATION OF TREATMENT
AND PREVENTION OF RECURRENCE
The effectiveness of psychopharmacotherapy is usually manifested in the
first 6 weeks
If mood disorders or cyclic episodes occur treatment with antidepressants
or mood stabilizers is warranted
Low-dosage pharmacotherapy must be maintained for 1 or 2 years after
recovery
During this long-term follow-up, periodic assessment and effective
clinical care with social and psychological therapy are essential
56. ISSUES OF NOSOLOGY
THE BOUNDARIES OF HOMOGENEITY:
Various sub-classifications of ATPD leads to an inhomogeneous group of
psychotic disorders
ICD-10 differentiates Acute Polymorphic Psychoses ‘with’ and ‘without”
symptoms of schizophrenia based on first-rank symptoms
WHO defines ‘Acute Schizophrenia-like Psychotic Disorder” based on:
1. Presence of first-rank symptoms
2. Absence of polymorphic symptomatology
No significant differences between the Polymorphic Psychotic Disorders
with or without schizophrenic symptoms was found
57. THE BOUNDARIES OF HOMOGENEITY
First-rank symptoms cannot distinguish the Acute Polymorphic
Disorders into subgroups
The polymorphism of the symptomatology has a much more
discriminating power than the presence of first-rank symptoms
The WHO distinction of ‘Acute Polymorphic Disorder’ into the two
categories ‘with’ and ‘without’ schizophrenic symptoms is unwarranted
and unnecessary
ICD-10 subtype F23.0 (‘with’ schizophrenic symptoms) and F23.1
(‘without’ schizophrenic symptoms) can be put together
58. Is the ‘Acute Schizophrenia-like Psychosis’ simply
schizophrenia
Main difference between Acute Schizophrenia-like Disorders and
schizophrenia concerns is duration (1 month)
Is this criterion valid enough to combine with ATPD ??
Patients with Acute Schizophrenia-like Psychoses are more similar to
patients with schizophrenia
The category ‘ATPD’ can be much more homogeneous if the ‘Acute
Polymorphic Psychotic Disorders’ are not combined with the ‘Acute
Schizophrenia-like Psychotic Disorders
59. FUTURE OF ATPD IN ICD-11
Working Group on the Classification of Psychotic Disorders (WGPD)
Diagnostic focus should be “Polymorphic” clinical presentation:
“”High variability/fluctuation of psychotic and affective symptoms”
WGPD recommends that:
1. Subcategory F23.0 (Acute polymorphic psychotic disorder without
symptoms of schizophrenia) be retained as the clinical guideline for
ATPD
2. Delusional subtype (F23.3) be incorporated into the revised category
Delusional disorder
60. EXPECTED CHANGES IN ICD-11
3. Present ICD-10 categories:
F23.1 (Acute polymorphic psychotic disorder with symptoms of
schizophrenia)
F23.2 (Acute schizophrenia-like psychotic disorder) be combined into:
“Unspecified primary psychotic disorders” if duration of disorder is
less than 4 weeks
If duration is more than 4 weeks schizophrenia should be diagnosed
61. CONCLUSION
Psychiatrists often subscribe to the Kraepelinian dichotomy
Attempt to label all functional psychosis as schizophrenia or affective
disorders
Clinical presentations of acute psychosis challenge such categorisation
More work is necessary to tighten up the definition
Few concepts need to be defined:
1. What is an adequate precipitant
2. Its temporal relation to the psychosis
There is a need for greater precision in delineating vulnerability, course
and outcome in acute psychosis
62. NEED FOR ETIOLOGICAL/ DIMENSIONAL
CLASSIFICATION SYSTEM
Any classification that is only phenomenological/descriptive in nature
without a validating biological criteria is far from ideal
The concept of ATPD has opened new vistas for further research and
theorization even about schizophrenias and affective disorders
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