Asthma is the most common cause of hospitalization in children in the U.S. other than infections, and cities such as Detroit have troublingly high asthma mortality rates. So-called """"""""risky"""""""" families-characterized by conflict, neglect, and lacking in emotional warmth and support-place children in jeopardy for asthma, and lay the groundwork for various chronic illnesses throughout life. However, little is known about the pathways through which risky family environments """"""""get under the skin"""""""" to exert their deleterious effects on health. Formulating a clear picture of everyday risky family behaviors and their effects on childhood asthma morbidity and biological mediators (e.g., epigenetic changes and gene expression) is essential for developing effective interventions targeted at improving health outcomes of children from risky families. The proposed research will take a multi-method biopsychosocial approach to the study of childhood asthma by investigating the links between everyday family behaviors and asthma morbidity in a sample of 180 youth aged 10-15 in Detroit, MI, in three waves of data collection over a 2-year period. The study will incorporate a novel naturalistic observation technology called the Electronically Activated Recorder (EAR), as well as well-validated parent- and child-reports of family functioning, clinical interviews, biological measures and clinical asthma evaluations. This project will test whether risky family behaviors assessed by the EAR (measuring conflict, neglect, lack of emotional warmth and support)-above and beyond traditional measures of family functioning-are longitudinally associated with greater asthma morbidity (e.g., symptom severity, ER visits, and pulmonary function) and with an increase in asthma morbidity (e.g., progression to more severe asthma diagnosis) over the three-wave, 2-year follow-up period. We will test biological mediators of these effects, including greater cortisol output in daily life, glucocorticoid receptor (GCR) gene expression, and methylation of GCR CpG promoter sites. Finally, we will test whether the links between risky family behaviors in daily life and asthma morbidity are mediated by avoidant coping behaviors and by poor asthma management behaviors (e.g., poorer asthma control medication adherence and poorer asthma trigger avoidance). Isolating specific biological and psychological processes in families that potentially contribute to, or buffer, asthma morbidity will foster future """"""""bench to bedside"""""""" translation of key findings from this project into novel and developmentally sensitive interventions to reduce asthma morbidity, and will also inform and improve family interventions that are currently being tested by our team with NHLBI funding. Finally, the findings from this study will be used to inform how to more accurately assess family interactions and stress with new technology and biomarkers to better capture potential mechanisms of behavior change in family intervention research.

Public Health Relevance

Asthma is the most common cause of hospitalization in children in the U.S. other than infections. So- called risky families-characterized by conflict, neglect, and lacking in emotional warmth and support- place children in jeopardy for asthma and other health problems. This project uses an innovative technology called the Electronically Activated Recorder (EAR) to investigate the links between everyday risky family behaviors, asthma morbidity and behavioral and biological mediators (including diurnal cortisol, gene expression, and epigenetic markers) in a sample of 180 youth aged 10-15 in Detroit, MI, whom we will follow for three waves of data collection over a two-year period.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL114097-04
Application #
8731270
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Freemer, Michelle M
Project Start
2011-09-30
Project End
2016-06-30
Budget Start
2014-07-01
Budget End
2015-06-30
Support Year
4
Fiscal Year
2014
Total Cost
Indirect Cost
Name
Wayne State University
Department
Psychology
Type
Schools of Arts and Sciences
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202
Farrell, Allison K; Slatcher, Richard B; Tobin, Erin T et al. (2018) Socioeconomic status, family negative emotional climate, and anti-inflammatory gene expression among youth with asthma. Psychoneuroendocrinology 91:62-67
Stanton, Sarah C E; Zilioli, Samuele; Briskin, Julia L et al. (2017) Mothers' Attachment is Linked to their Children's Anti-Inflammatory Gene Expression via Maternal Warmth. Soc Psychol Personal Sci 8:796-805
Imami, Ledina; Zilioli, Samuele; Tobin, Erin T et al. (2017) Youth secrets are associated with poorer sleep and asthma symptoms via negative affect. J Psychosom Res 96:15-20
Slatcher, Richard B; Schoebi, Dominik (2017) Protective Processes Underlying the Links between Marital Quality and Physical Health. Curr Opin Psychol 13:148-152
Slatcher, Richard B; Selcuk, Emre (2017) A Social Psychological Perspective on the Links between Close Relationships and Health. Curr Dir Psychol Sci 26:16-21
Tobin, Erin T; Zilioli, Samuele; Imami, Ledina et al. (2016) Neighborhood Stress, Depressive Symptoms, and Asthma Morbidity in Youth. J Pediatr Psychol 41:952-60
Abbas, Tazeen; Zilioli, Samuele; Tobin, Erin T et al. (2016) Youth reports of parents' romantic relationship quality: Links to physical health. Health Psychol 35:927-34
Tobin, Erin T; Kane, Heidi S; Saleh, Daniel J et al. (2015) Naturalistically observed conflict and youth asthma symptoms. Health Psychol 34:622-31
Imami, Ledina; Tobin, Erin T; Kane, Heidi S et al. (2015) Effects of socioeconomic status on maternal and child positive behaviors in daily life among youth with asthma. J Pediatr Psychol 40:55-65
Tobin, Erin T; Kane, Heidi S; Saleh, Daniel J et al. (2015) Asthma-Related Immune Responses in Youth With Asthma: Associations With Maternal Responsiveness and Expressions of Positive and Negative Affect in Daily Life. Psychosom Med 77:892-902

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