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Early Intervention in Psychosis > Lecture 3: Prodrome, Early Detection of UHR and Risks > Flashcards

Lecture 3: Prodrome, Early Detection of UHR and Risks Flashcards

1
Q

Name 3 widely uses intruments

A

SPI-A
Schixophrenia Proness Instrument - Adult Version

CAARMS
Community Assessment of At Risk Mental State

SIPS/SOPS
Schizophrenia Interview for Prodromal Symptoms
Schizophrenia Scale of Prodromal Symptoms

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2
Q

What was the SPI-A designed to primarily support?

A

The prediction of first episode psychosis

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3
Q

What are the rating areas of the SPI-A (7)

A

Affectve-dynamic distrubances (Impaired tolerance for certain stressors)
Cognitive attentional impediments
Cogtnitive Disturbances
Disturbances in experiencing self and surroundings
Body perception disturbances
Percetion Disturbances
Optional Additional Items

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4
Q

When is a symptom a symptom according to SPI-A?

A

must ONLY be subjectively experienced
scored ehrn symptoms experienced as a disturbance deficiency or a complaint IRRESPECTIVE of its appearace in behaviour

induvidual reports but not observed by itnerviewer = RECORD
interviewer observes but induivudal not reported IS NOT recorded by interviewer

Symptoms must reporesent achance from what the person used to be like when they were well

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5
Q

How is “at-risk” defined with SPI-A?

what two symptoms measured by SPI-A have shown to predict sympotms of psychosis?
and who’s studies showed them?

Kl_________r et al (2001)

S——-L——- et al (2007)

A

COPER and COGDIS

COPER 
Cognitive-perceptive basic symptoms: 
-- Thought Inferences 
--Thought Blockages 
-- Disturbance of recetpive speech 
--Decreased abiity to discriminate ideas/fantasies from reality

Klosterkoetter et al (2001) - very high transition rates for COPER
20% in 12 months
50% after 3 years

COGDIS
Cognitive Disturbances
Schultze-Lutter et al (2007)
24% in 12 months and 61% after 3 years

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6
Q

what are problems with COPER/COGDIS prediction?

A

Problems
Regarded difficult to assess
Pathway to care unclear
can this be used in a clinical setting

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7
Q

How does the other measures (CAARMS and SIPS) differ?

A

THey focused on latter stages more at-risk focus, Ultra High Risk

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8
Q

What are CAARMS and SIPS used to detect

what popualtion are CAARMS and SIPS used on?

What are the implications of that?

A

CAARMS and SIPS are used to detect attenuated/subthreshold symptoms

Person MUST be help-seeking
- not used in GP so dont know PPV and NPV in GP

Person may require a functional impairment
- persisitent low functioning or 30% delcine in last 12 months

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9
Q

How do attenuated/subthreshold symptoms differ from frank symptoms

A
    • these symptoms differ from frank symptoms in intensity, frequency and/or duration
  • —- persecutory beleif about someone who is behind you on train you don’t
  • —— Hold it fully (intensity)
  • —— Hold it for long (duration)
  • —— it only happened once (Hz)
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10
Q

What are the CAARMS criteria?

A

Group 1 Attenuated Psychosis
– SUbthreshold Intenisty or Frequency
Group 2 BLIPS Breif Limited Intermittened Psychotic Symptoms
– Full threshold symptoms that last less than a week
Group 3 Vulnerabilty
– 1st degree relative with psychosis OR personal history of schizophrenia, plus a functional decline

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11
Q

What are the aims of CAARMS? (3)

A

UHR
Determine if the induviudal meets UHR criteria

Onset
Rule out or confirm criteria for onset of psychosis (transitioners)

Map
To map over time a range of symptoms found in psychotic prodromes

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12
Q

What are the psychometric properties of CAARMS

A

Inter rate = 0.85
Concurrent = Great 2.08 vs 0.29 (C) scores on CAARMS
Discriminant =
12 month tranistion rate CAARMS = .42 CI 95% 0.26- 0.55
12 month tranistion rate BPRS =.41 CI 95% 0.25-0.53

Sen = .83
Spe=.74
PPV = 0.12
NPV = 0.99

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13
Q

7 domains of psychopathology covered by CAARMS

A
  1. Postive symptoms
  2. Negative symptoms
  3. Cognitive changes (attention/concentration)
  4. Behavioural changes
  5. General Psychopathology
  6. Emotional changes
  7. Motor/physical changes
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14
Q

Yung et al (2005)

Psychometric properties

A

Collected data from ORYGEN Youth Health which has UHR clinic (PACE clinic)

CAARMS scores predicted onset of psychosis (-ve symptoms not popstive) - not presence of hallunications or dleusions but negative symptoms

Those mething UHR criteria on the CAARMS had a higher rate of tranistion to psychosis at 6 month follow up

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