The diagnosis of major depression represents a clinical syndrome with a number of biological, behavioral, affective, and cognitive components. Recent evidence suggests that depression places people at increased risk for physical morbidity and mortality. Increased risk among depressed persons is thought to be attributable to intense affect triggering biological changes that make people more susceptible to physical diseases. Because the immune system is known to respond to changes in affect, research has focused on immune alteration as a plausible pathway through which depression could influence physical health. There is substantial evidence that clinically depressed persons are immunologically different than nondepressed persons, although why these differences occur is not known. The primary focus of this investigation is to address the important question of why immune differences exist in clinical depression. To do this, four specific questions are asked: (1) Are the immune changes associated with clinical depression related to the start of depression or are they characteristic of those who have ever been clinically depressed? (2) Are associations between depression and immunity attributable to the affective component of the depressive state? (3) Do cortisol and/or the catecholamines mediate the immune alterations in subjects with clinical depression? and (4) Do health practices such as sleep, diet, caffeine and alcohol intake, cigarette use, and exercise account for the associations of depression with immunity? The scope of immune outcomes of interest in this study is broad and includes both enumerative measures (i.e., the numbers of circulating eosinophils, basophils, monocytes, neutrophils, and lymphocytes, as well as specific lymphocyte subsets including N-K, B, T, helper T, suppressor T, and cytotoxic T cells) and functional measures (i.e., IL-1 production by monocytes, IL-2 production by lymphocytes, lymphocyte proliferative response to PHA, Con A, and PWM, and NK cell cytotoxic activity). The design to be used will increase the reliability of data collected. Because immune system functions and enumerations are influenced by a variety of factors, obtaining a reliable characterization of an individual's immune status requires more than one assessment. Therefore, the reliability of measurement of the neuroendocrine and immune parameters will be improved by assessing subjects twice separated by 24 hours. Subjects for the study will be physically healthy, age- and race-matched women, between 25 and 50 years of age. No depressed patients will be hospitalized and all subjects will be free of medication.

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH050430-02
Application #
2249764
Study Section
Psychobiological, Biological, and Neurosciences Subcommittee (MHAI)
Project Start
1993-02-01
Project End
1997-01-31
Budget Start
1994-02-01
Budget End
1995-01-31
Support Year
2
Fiscal Year
1994
Total Cost
Indirect Cost
Name
Mellon Pitts Corporation (Mpc Corp)
Department
Type
DUNS #
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213
Cohen, Sheldon; Janicki-Deverts, Denise; Doyle, William J et al. (2012) Chronic stress, glucocorticoid receptor resistance, inflammation, and disease risk. Proc Natl Acad Sci U S A 109:5995-9
Pressman, Sarah D; Cohen, Sheldon; Miller, Gregory E et al. (2005) Loneliness, social network size, and immune response to influenza vaccination in college freshmen. Health Psychol 24:297-306
Miller, Gregory E; Cohen, Sheldon; Pressman, Sarah et al. (2004) Psychological stress and antibody response to influenza vaccination: when is the critical period for stress, and how does it get inside the body? Psychosom Med 66:215-23
Cohen, S; Hamrick, N (2003) Stable individual differences in physiological response to stressors: implications for stress-elicited changes in immune related health. Brain Behav Immun 17:407-14
Hamrick, Natalie; Cohen, Sheldon; Rodriguez, Mario S (2002) Being popular can be healthy or unhealthy: stress, social network diversity, and incidence of upper respiratory infection. Health Psychol 21:294-8
Cohen, Sheldon; Hamrick, Natalie; Rodriguez, Mario S et al. (2002) Reactivity and vulnerability to stress-associated risk for upper respiratory illness. Psychosom Med 64:302-10
Miller, Gregory E; Cohen, Sheldon; Ritchey, A Kim (2002) Chronic psychological stress and the regulation of pro-inflammatory cytokines: a glucocorticoid-resistance model. Health Psychol 21:531-41
Cohen, S; Hamrick, N; Rodriguez, M S et al. (2000) The stability of and intercorrelations among cardiovascular, immune, endocrine, and psychological reactivity. Ann Behav Med 22:171-9
Miller, G E; Cohen, S; Herbert, T B (1999) Pathways linking major depression and immunity in ambulatory female patients. Psychosom Med 61:850-60
Cohen, S; Herbert, T B (1996) Health psychology: psychological factors and physical disease from the perspective of human psychoneuroimmunology. Annu Rev Psychol 47:113-42

Showing the most recent 10 out of 13 publications