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Accepted for/Published in: JMIR Formative Research

Date Submitted: Feb 3, 2019
Open Peer Review Period: Feb 4, 2019 - Feb 11, 2019
Date Accepted: Aug 31, 2019
(closed for review but you can still tweet)

The final, peer-reviewed published version of this preprint can be found here:

Use of Patient-Reported Data to Match Depression Screening Intervals With Depression Risk Profiles in Primary Care Patients With Diabetes: Development and Validation of Prediction Models for Major Depression

Jin H, Wu S

Use of Patient-Reported Data to Match Depression Screening Intervals With Depression Risk Profiles in Primary Care Patients With Diabetes: Development and Validation of Prediction Models for Major Depression

JMIR Form Res 2019;3(4):e13610

DOI: 10.2196/13610

PMID: 31573900

PMCID: 6774232

Leveraging Patient-Reported Data and Predictive Modeling to Match Depression Screening Interval with Depression Risk Profile in Primary Care Patients with Diabetes

  • Haomiao Jin; 
  • Shinyi Wu

ABSTRACT

Background:

Clinical guideline recommends screening for depression in the general adult population but recognizes that optimum interval for screening is unknown. Ideal screening intervals should match with patient risk profiles.

Objective:

This study describes an approach that mined patient-reported data from a large clinical trial with predictive modeling to improve case identification for primary care patients at high risk for depression to match depression screening interval with patient risk profile.

Methods:

This paper analyzed data from a large safety-net primary care study for diabetes and depression. A regression-based data mining technique was used to examine 53 demographics, clinical, and patient-reported variables to develop three prediction models for major depression at 6, 12, and 18 months from baseline. Predictors among the strongest predictive power that also require low information collection efforts were selected to develop the prediction models. Predictive accuracy was measured by the area under the receiver operating curve (AUROC) and was evaluated by 10-fold cross-validation. The effectiveness of the prediction algorithms in supporting clinical decision making for five “typical” types of patients was demonstrated.

Results:

The analysis included 923 patients. Five patient-reported variables were selected in the prediction models: 1) Patient Health Questionnaire 2-item score; 2) the Sheehan Disability Scale; 3) previous problems with depression; 4) the diabetes symptoms scale; and 5) diabetes emotional burden. All three depression prediction models have AUROC>0.80, comparable with published depression prediction studies. Among the 5 “typical” types of patients, the algorithms suggest patients who reported impaired daily functioning by health status are at an elevated risk for depression in all three periods.

Conclusions:

This study demonstrated leveraging patient-reported data and prediction models can help improve case identification and clinical decision about depression screening interval for diabetes patients. Implementation of this approach can be coupled with application of modern technologies such as tele- and mobile-health assessment for collecting patient-reported data to improve privacy, reduce stigma and costs, and promote a personalized depression screening that matches screening interval with patient risk profiles.


 Citation

Please cite as:

Jin H, Wu S

Use of Patient-Reported Data to Match Depression Screening Intervals With Depression Risk Profiles in Primary Care Patients With Diabetes: Development and Validation of Prediction Models for Major Depression

JMIR Form Res 2019;3(4):e13610

DOI: 10.2196/13610

PMID: 31573900

PMCID: 6774232

Per the author's request the PDF is not available.

© The authors. All rights reserved. This is a privileged document currently under peer-review/community review (or an accepted/rejected manuscript). Authors have provided JMIR Publications with an exclusive license to publish this preprint on it's website for review and ahead-of-print citation purposes only. While the final peer-reviewed paper may be licensed under a cc-by license on publication, at this stage authors and publisher expressively prohibit redistribution of this draft paper other than for review purposes.