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Premature ejaculation and pharmaceutical company-based medicine: the dapoxetine case.
J Sex Med. 2008 Apr; 5(4):966-997.JS

Abstract

INTRODUCTION

The manufacturer of dapoxetine funded randomized clinical trials to study its effect in premature ejaculation (PE). Financial support by pharmaceutical companies, however, may jeopardize the neutrality of clinical research.

AIM

To investigate the scientific process that has been followed in dapoxetine treatment trials and reviews as compared to daily drug treatment trials and reviews with selective serotonin reuptake inhibitors (SSRIs) in men with PE.

METHODS

A search of Medline and Embase was conducted using the search terms "dapoxetine" or "SSRI." References of retrieved articles were searched. Only studies describing the use of these drugs in men with PE were included. Main Outcome Measures. Compared fold-increase intravaginal ejaculation latency time (IELT), geometric mean IELT, and adverse effect profiles between dapoxetine and SSRIs in PE.

RESULTS

Preclinical studies on dapoxetine, including a multicenter study (category A) and reviews (category B), were compared with clinical studies with daily conventional SSRIs in PE (category C). Categories A/B focused on patient-reported outcomes with less attention for the IELT. The ejaculation-delaying effect of dapoxetine was expressed as natural mean IELT rather than as geometrical mean IELT. Dapoxetine side effects were monthly scored. In contrast, a significant part of category C articles focused on IELT data, used geometric mean IELT outcomes, and one study reported the side effects measured 24-48 hours after drug intake using a validated questionnaire. Without the Food and Drug Administration approval, dapoxetine, as well as other SSRIs in PE, is an off-label drug for PE. However, the off-label use of dapoxetine has never been criticized by clinical investigators in contrast to commentaries against the off-label use of daily SSRI treatment in PE.

CONCLUSIONS

Manufacturer-funded drug treatment research (categories A and B) is advantageously treated by some authors as compared with nonfunded trials with daily conventional SSRIs (category C). PE drug treatment research is a young and dynamic field, and its development deserves transparency to its development.

Links

Publisher Full Text (DOI)

Authors+Show Affiliations

Waldinger MD
Department of Psychiatry and Neurosexology, HagaHospital Leyenburg, The Hague, the Netherlands;; Department of Psychopharmacology, Utrecht Institute for Pharmaceutical Sciences and Rudolf Magnus Institute for Neurosciences, Utrecht University, Utrecht, the Netherlands;. Electronic address: md@waldinger.demon.nl.
Schweitzer DH
Department of Internal Medicine and Endocrinology, Reinier de Graaf Groep Hospital, Delft-Voorburg, the Netherlands.

MeSH

AnimalsBenzylaminesControlled Clinical Trials as TopicDrug Evaluation, PreclinicalDrug IndustryEjaculationEvidence-Based MedicineHumansMaleMeta-Analysis as TopicNaphthalenesSelective Serotonin Reuptake InhibitorsSexual Dysfunction, Physiological

Pub Type(s)

Journal Article
Review

Language

eng

PubMed ID

18371047

Citation

Waldinger, Marcel D., and Dave H. Schweitzer. "Premature Ejaculation and Pharmaceutical Company-based Medicine: the Dapoxetine Case." The Journal of Sexual Medicine, vol. 5, no. 4, 2008, pp. 966-997.
Waldinger MD, Schweitzer DH. Premature ejaculation and pharmaceutical company-based medicine: the dapoxetine case. J Sex Med. 2008;5(4):966-997.
Waldinger, M. D., & Schweitzer, D. H. (2008). Premature ejaculation and pharmaceutical company-based medicine: the dapoxetine case. The Journal of Sexual Medicine, 5(4), 966-997. https://doi.org/10.1111/j.1743-6109.2008.00633.x
Waldinger MD, Schweitzer DH. Premature Ejaculation and Pharmaceutical Company-based Medicine: the Dapoxetine Case. J Sex Med. 2008;5(4):966-997. PubMed PMID: 18371047.
* Article titles in AMA citation format should be in sentence-case
TY - JOUR T1 - Premature ejaculation and pharmaceutical company-based medicine: the dapoxetine case. AU - Waldinger,Marcel D, AU - Schweitzer,Dave H, PY - 2008/3/29/pubmed PY - 2008/4/23/medline PY - 2008/3/29/entrez SP - 966 EP - 997 JF - The journal of sexual medicine JO - J Sex Med VL - 5 IS - 4 N2 - INTRODUCTION: The manufacturer of dapoxetine funded randomized clinical trials to study its effect in premature ejaculation (PE). Financial support by pharmaceutical companies, however, may jeopardize the neutrality of clinical research. AIM: To investigate the scientific process that has been followed in dapoxetine treatment trials and reviews as compared to daily drug treatment trials and reviews with selective serotonin reuptake inhibitors (SSRIs) in men with PE. METHODS: A search of Medline and Embase was conducted using the search terms "dapoxetine" or "SSRI." References of retrieved articles were searched. Only studies describing the use of these drugs in men with PE were included. Main Outcome Measures. Compared fold-increase intravaginal ejaculation latency time (IELT), geometric mean IELT, and adverse effect profiles between dapoxetine and SSRIs in PE. RESULTS: Preclinical studies on dapoxetine, including a multicenter study (category A) and reviews (category B), were compared with clinical studies with daily conventional SSRIs in PE (category C). Categories A/B focused on patient-reported outcomes with less attention for the IELT. The ejaculation-delaying effect of dapoxetine was expressed as natural mean IELT rather than as geometrical mean IELT. Dapoxetine side effects were monthly scored. In contrast, a significant part of category C articles focused on IELT data, used geometric mean IELT outcomes, and one study reported the side effects measured 24-48 hours after drug intake using a validated questionnaire. Without the Food and Drug Administration approval, dapoxetine, as well as other SSRIs in PE, is an off-label drug for PE. However, the off-label use of dapoxetine has never been criticized by clinical investigators in contrast to commentaries against the off-label use of daily SSRI treatment in PE. CONCLUSIONS: Manufacturer-funded drug treatment research (categories A and B) is advantageously treated by some authors as compared with nonfunded trials with daily conventional SSRIs (category C). PE drug treatment research is a young and dynamic field, and its development deserves transparency to its development. SN - 1743-6109 UR - https://www.unboundmedicine.com/medline/citation/18371047/Premature_ejaculation_and_pharmaceutical_company_based_medicine:_the_dapoxetine_case_ DB - PRIME DP - Unbound Medicine ER -