A survey of psychosis risk symptoms in Kenya

Mamah, Daniel; Mbwayo, Anne; Mutiso, Victoria; Deanna, M; Constantino, John N.; Nsofor, Thelma; Khasakhala, Lincoln; Ndetei, David M.

doi:10.1016/j.comppsych.2011.08.003

Cited by 26 publications

(34 citation statements)

References 38 publications

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“…Written and signed consent was obtained from the study participants and the study was approved by the institutional review board of Washington University Medical School, the Kenyan Medical Research Institute, and the Ministry of Education, Science, and Technology, Kenya. A total of 2758 individuals between the ages of 14 and 29 were recruited for our prior survey using mPRIME, as detailed in Mamah et al [25]. …”

Section: Methodsmentioning

confidence: 99%

“…Our group previously examined psychosis risk in young Kenyan populations using a slightly modified version of the PRIME screen to account for cultural differences in screen item interpretation (mPRIME), and found that 45.5% of participants aged 14 to 29 reported having had a psychosis risk symptom (i.e., a score of ‘6’) on the screen [25]. The main goal for the current study was to evaluate the validity of the mPRIME as a screening tool for general youth populations, using the SIPS as the reference standard.…”

Section: Introductionmentioning

confidence: 99%

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Validation of a modified version of the PRIME screen for psychosis-risk symptoms in a non-clinical Kenyan youth sample

Owoso

Ndetei

Mbwayo

et al. 2014

Comprehensive Psychiatry

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Background The PRIME screen is a self-administered questionnaire designed to quickly assess individuals at risk for developing a psychotic disorder. It is shorter in both length and administration time compared to the Structured Interview for Psychosis-Risk Syndromes (SIPS)—a standard instrument for psychosis prodromal risk assessment. Validation of the PRIME against the SIPS has not been reported in large non-clinical populations. Methods A culturally modified version of the PRIME screen (mPRIME) was administered to Kenyan youth between the ages of 14 and 29. 182 completed both the SIPS and mPRIME. Validation measures (sensitivity, specificity, positive predictive value, negative predictive value) were calculated and the study sample was then broken down into true positives, false positives, and false negatives for comparison on different quantitative measures. Results Using previously suggested thresholds for a positive screen, the mPRIME had a sensitivity of 40% and a specificity of 64.8% for our entire sample. Positive predictive value (PPV) and negative predictive value (NPV) were 12.3% and 89.7%, respectively. Breaking the sample down by questionnaire outcome showed that true-positive individuals scored higher on average rate and intensity of endorsement of mPRIME items compared to false-positive and false-negatives, while false-negatives on average registered disagreement on all mPRIME questionnaire items. Conclusions The mPRIME does not appear to be an effective screener of at-risk individuals for psychosis in our non-clinical sample. Further validation efforts in other general populations are warranted.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Validation of a modified version of the PRIME screen for psychosis-risk symptoms in a non-clinical Kenyan youth sample

Owoso

Ndetei

Mbwayo

et al. 2014

Comprehensive Psychiatry

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“…72 A community study of youth aged 14 to 29 years from Kenya reported that 45% of the sample endorsed at least 1 psychotic risk symptom. 73 These experiences do not necessarily predict the onset of a psychotic disorder; rather, they are apt to be indicators of risk for a variety of mental disorders (including depression, bipolar disorder, and sometimes schizophrenia). Even when psychotic symptoms do represent a prodrome for psychotic disorders (usually schizophrenia spectrum disorders), approximately 18% to 36% of people defined as high risk go on to transition to a mental disorder, with the risk of transition increasing over time.…”

Section: Research Priority Setting For Global Mental Healthmentioning

confidence: 99%

“…Identifying who is at risk to transition to a psychotic disorder, and intervening early, remains a critical area for investigation. Efforts to harmonize data across research sites in HICs enrich these research activities, but questions remain about the validity of commonly used measures to assess those who may be at high risk for psychosis in low-income country settings 73 (see Table 1). …”

Section: Research Priority Setting For Global Mental Healthmentioning

confidence: 99%

Advancing Research to Action in Global Child Mental Health

Ordóñez

Collins

2015

Child and Adolescent Psychiatric Clinics of North America

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“…Differences in health care systems and patterns of referral for specialized care affect the ways in which high risk individuals can be identified for research purposes and the implementation of intervention research. Base rates of self-reported psychosis prodrome symptoms appear to differ among countries [ 21 , 22 ], thus impacting estimates of prevalence and conversion rates. Translation and validation of the measures used to detect the psychosis risk state facilitates data sharing and integration across countries and cultures.…”

Section: Reviewmentioning

confidence: 99%

Informed consent in the psychosis prodrome: ethical, procedural and cultural considerations

Morris

Heinssen

2014

Philos Ethics Humanit Med

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Research focused on the prodromal period prior to the onset of psychosis is essential for the further development of strategies for early detection, early intervention, and disease pre-emption. Such efforts necessarily require the enrollment of individuals who are at risk of psychosis but have not yet developed a psychotic illness into research and treatment protocols. This work is becoming increasingly internationalized, which warrants special consideration of cultural differences in conceptualization of mental illness and international differences in health care practices and rights regarding research participation. The process of identifying and requesting informed consent from individuals at elevated risk for psychosis requires thoughtful communication about illness risk and often involves the participation of family members. Empirical studies of risk reasoning and decisional capacity in young people and individuals with psychosis suggest that most individuals who are at-risk for psychosis can adequately provide informed consent; however ongoing improvements to tools and procedures are important to ensure that this work proceeds with maximal consideration of relevant ethical issues. This review provides a discussion of these issues in the context of international research efforts.

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A survey of psychosis risk symptoms in Kenya

Cited by 26 publications

References 38 publications

Validation of a modified version of the PRIME screen for psychosis-risk symptoms in a non-clinical Kenyan youth sample

Validation of a modified version of the PRIME screen for psychosis-risk symptoms in a non-clinical Kenyan youth sample

Advancing Research to Action in Global Child Mental Health

Informed consent in the psychosis prodrome: ethical, procedural and cultural considerations

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