Peter T. Loosen scite author profile

The possibility that hypersecretion of corticotropin-releasing factor (CRF) contributes to the hyperactivity of the hypothalamo-pituitary-adrenal axis observed in patients with major depression was investigated by measuring the concentration of this peptide in cerebrospinal fluid of normal healthy volunteers and in drug-free patients with DSM-III diagnoses of major depression, schizophrenia, or dementia. When compared to the controls and the other diagnostic groups, the patients with major depression showed significantly increased cerebrospinal fluid concentrations of CRF-like immunoreactivity; in 11 of the 23 depressed patients this immunoreactivity was greater than the highest value in the normal controls. These findings are concordant with the hypothesis that CRF hypersecretion is, at least in part, responsible for the hyperactivity of the hypothalamo-pituitary-adrenal axis characteristic of major depression.

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Cognitive therapy and pharmacotherapy for depression.

Hollon¹,

Shelton²,

Loosen³

1991

Journal of Consulting and Clinical Psychology

325

349

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Cognitive therapy (CT) for depression has generated considerable interest in recent years. Comparisons with tricyclic pharmacotherapy in nonbipolar outpatients have suggested that (a) CT may be roughly comparable in the treatment of the acute episode: (b) combined CT-pharmacotherapy does not appear to be clearly superior to either modality (although indications of potential enhancement do exist to justify additional studies with larger samples), and (c) treatment with CT during the acute episode (either alone or with medications) may reduce the risk of subsequent relapse following termination. Nonetheless, for a variety of reasons (e.g., limitations in study design and execution, inadequate design power, and possible differential retention), these conclusions can be considered only suggestive at this time. More than a decade after the publication of the first controlled study involving CT, the approach remains a promising, but not adequately tested, alternative to pharmacotherapy in the treatment of depression.

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Hypothermia and intolerance to cold induced by intracisternal administration of the hypothalamic peptide neurotensin

Bissette

Nemeroff

Loosen

et al. 1976

Nature

297

161

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Individual differences in repressive-defensiveness predict basal salivary cortisol levels.

Brown¹,

Tomarken²,

Orth³

et al. 1996

Journal of Personality and Social Psychology

113

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Prior studies assessing the relation between negative affective traits and cortisol have yielded inconsistent results. Two studies assessed the relation between individual differences in repressive-defensiveness and basal salivary cortisol levels. Experiment 1 assessed midafternoon salivary cortisol levels in men classified as repressors, high-anxious, or low-anxious. In Experiment 2, more rigorous controls were applied as salivary cortisol levels in women and men were assessed at 3 times of day on 3 separate days. In both studies, as hypothesized, repressors and high-anxious participants demonstrated higher basal cortisol levels than low-anxious participants. These findings suggest that both heightened distress and the inhibition of distress may be independently linked to relative elevations in cortisol. Also discussed is the possible mediational role of individual differences in responsivity to, or mobilization for, uncertainty or change.Laurel L. Brown and Andrew J. Tomarken contributed equally to the research conducted in this article. Experiment 2 was conducted by Laurel L. Brown as part of her second-year project at Vanderbilt University under the supervision of Andrew J. Tomarken.

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The TRH-induced TSH response in psychiatric patients: a possible neuroendocrine marker

Loosen

1985

Psychoneuroendocrinology

149

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Low cerebrospinal fluid corticotropin-releasing hormone concentrations in eucortisolemic depression

Geracioti

Loosen

Orth

1997

Biological Psychiatry

101

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Neurotensin: Central nervous system effects of a hypothalamic peptide

Nemeroff

Bissette²,

Prange³

et al. 1977

Brain Research

252

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Serial cerebrospinal fluid corticotropin-releasing hormone concentrations in healthy and depressed humans.

Geracioti

Orth

Ekhator

et al. 1992

The Journal of Clinical Endocrinology & Metabolism

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CRH, a hypothalamic peptide that is the most potent ACTH secretagogue known, also appears to be produced in the cerebral cortex and spinal cord. Depressed patients have blunted responses to exogenous CRH and normal to high concentrations of CRH immunoreactivity in single morning samples of lumbar cerebrospinal fluid (CSF). Although these data suggest that depression may be associated with hypersecretion of CRH, it has also been postulated that central nervous system insufficiency of CRH might have a pathophysiological role in certain depressive syndromes. We continuously sampled lumbar CSF via indwelling subarachnoid catheters from 1100-1700 h and measured CRH at 10-min intervals in depressed patients and normal subjects. A standardized mixed liquid meal was administered at 1300 h. CSF CRH was strikingly reduced in depressed patients compared to normal subjects [4.2 +/- 1.1 pmol/L vs. 13 +/- 2.1 pmol/L (mean +/- SEM), respectively, P less than 0.01 by Wilcoxon test]. CSF CRH concentrations rose progressively during the experiment in both groups, suggesting a diurnal rhythm and, possibly, response to a test meal. CRH had a very brief half-life in CSF (less than 10 min), suggesting that the spinal cord is the origin of CRH in lumbar CSF. The rapid transients in CSF CRH concentration demonstrate that single samples provide very limited information. There were no intraindividual correlations between CSF CRH concentrations and those of either plasma ACTH or cortisol, both of which rose in response to eating. The present data show that impaired central nervous system secretion of CRH can exist during states of severe depression.

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Peter T. Loosen

Elevated Concentrations of CSF Corticotropin-Releasing Factor-Like Immunoreactivity in Depressed Patients

Cognitive therapy and pharmacotherapy for depression.

Hypothermia and intolerance to cold induced by intracisternal administration of the hypothalamic peptide neurotensin

Individual differences in repressive-defensiveness predict basal salivary cortisol levels.

The TRH-induced TSH response in psychiatric patients: a possible neuroendocrine marker

Low cerebrospinal fluid corticotropin-releasing hormone concentrations in eucortisolemic depression

Neurotensin: Central nervous system effects of a hypothalamic peptide

Serial cerebrospinal fluid corticotropin-releasing hormone concentrations in healthy and depressed humans.

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