Frontiers in Psychiatry (Dec 2017)

A Biomarker to Differentiate between Primary and Cocaine-Induced Major Depression in Cocaine Use Disorder: The Role of Platelet IRAS/Nischarin (I1-Imidazoline Receptor)

  • Benjamin Keller,
  • Benjamin Keller,
  • Joan-Ignasi Mestre-Pinto,
  • Joan-Ignasi Mestre-Pinto,
  • María Álvaro-Bartolomé,
  • María Álvaro-Bartolomé,
  • Diana Martinez-Sanvisens,
  • Diana Martinez-Sanvisens,
  • Magí Farre,
  • Magí Farre,
  • Magí Farre,
  • Magí Farre,
  • M. Julia García-Fuster,
  • M. Julia García-Fuster,
  • Jesús A. García-Sevilla,
  • Jesús A. García-Sevilla,
  • Marta Torrens,
  • Marta Torrens,
  • Marta Torrens,
  • The NEURODEP Group,
  • F. Fonseca,
  • J. Mateus,
  • E. Papaseit,
  • C. Pérez-Mañá,
  • R. Rodríguez-Minguela,
  • P. Rossi,
  • C. Tamarit,
  • G. Vallecillo

DOI
https://doi.org/10.3389/fpsyt.2017.00258
Journal volume & issue
Vol. 8

Abstract

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The association of cocaine use disorder (CUD) and comorbid major depressive disorder (MDD; CUD/MDD) is characterized by high prevalence and poor treatment outcomes. CUD/MDD may be primary (primary MDD) or cocaine-induced (CUD-induced MDD). Specific biomarkers are needed to improve diagnoses and therapeutic approaches in this dual pathology. Platelet biomarkers [5-HT2A receptor and imidazoline receptor antisera selected (IRAS)/nischarin] were assessed by Western blot in subjects with CUD and primary MDD (n = 16) or CUD-induced MDD (n = 9; antidepressant free, AD−; antidepressant treated, AD+) and controls (n = 10) at basal level and/or after acute tryptophan depletion (ATD). Basal platelet 5-HT2A receptor (monomer) was reduced in comorbid CUD/MDD subjects (all patients: 43%) compared to healthy controls, and this down-regulation was independent of AD medication (decreases in AD−: 47%, and in AD+: 40%). No basal differences were found for IRAS/nischarin contents in AD+ and AD− comorbid CUD/MDD subjects. The comparison of IRAS/nischarin in the different subject groups during/after ATD showed opposite modulations (i.e., increases and decreases) in response to low plasma tryptophan levels with significant differences discriminating between the subgroups of CUD with primary MDD and CUD-induced MDD. These specific alterations suggested that platelet IRAS/nischarin might be useful as a biomarker to discriminate between primary and CUD-induced MDD in this dual pathology.

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