![[dr. bob]](/dr-bob-sm.gif)
Dr. Bob is Robert Hsiung, MD,
bob@dr-bob.orgShown: posts 1 to 13 of 13. This is the beginning of the thread.
Posted by lostforwards on November 1, 2004, at 8:51:50
I really hate serotonin. Right now I need bromocriptine or something. My arms still don't swing and I'm still feeling pretty anhedonic, relative to what's normal for me anyway. Meanwhile I've been looking for information on antidepressants, in particular SRI-types, and their less often talked about adverse affects.
This has been one of my favourite topics ever since I read Brave New World.Very quickly I came across this. It's the second article called "Too High for Love?
Lost Your Drive? Antidepressants May Tinker with Mating Instincts..." on this page : http://flatrock.org.nz/topics/society_culture/sex_and_schopenhauer.htmto quote it "You can jeopardise your ability to choose a mate appropriately, you can jeopardise your ability to fall in love and you can jeopardise your ability to feel attachment."
comments?
Posted by linkadge on November 1, 2004, at 9:24:42
In reply to Unrequited love, sex, attachment, and serotonin., posted by lostforwards on November 1, 2004, at 8:51:50
You're right in some sences.
SSRI's can lession obsessions. Even so to the point of having no obsessions. This can extend to sexual and relationship behaviors.
However, there was a study done that showed that the people who were least depressed naturally (scored lowest on depression and anxiety scales), also had the least interest in sex!. One researcher concluded.. it is as if they naturally had prozac in their brains.This is true for me. When I am depressed, I seed consolation from others. When I am not depressed I am more independant, and want to stay that way.
I think a lot about this stuff too, really is a mind bender.
Linkadge
Posted by ed_uk on November 1, 2004, at 9:25:24
In reply to Unrequited love, sex, attachment, and serotonin., posted by lostforwards on November 1, 2004, at 8:51:50
A while ago, I fell in love on 60mg Paxil. It reduced my sex drive a bit but the sexual side effects were always mild. I still feel attachment and I still feel hurt if people reject me. Sadly, many people are not so lucky (in terms of the sexual dysfunction).
It sounds like you might be interested in the dopamine reuptake inhibitor amineptine (Survector).It's a 'pro-sexual' antidepressant which increases libido and intensifies orgasms. It's said to be particularly good for anhedonia. It's only available in south america these days since many countries have banned its use (because of reports of drug abuse and liver damage.) It was never on the market in the uk where I live. It might make you manic if you're bipolar though!!!
Ed
Posted by jrbecker on November 1, 2004, at 9:27:35
In reply to Unrequited love, sex, attachment, and serotonin., posted by lostforwards on November 1, 2004, at 8:51:50
> I really hate serotonin. Right now I need bromocriptine or something. My arms still don't swing and I'm still feeling pretty anhedonic, relative to what's normal for me anyway. Meanwhile I've been looking for information on antidepressants, in particular SRI-types, and their less often talked about adverse affects.
> This has been one of my favourite topics ever since I read Brave New World.
>
> Very quickly I came across this. It's the second article called "Too High for Love?
> Lost Your Drive? Antidepressants May Tinker with Mating Instincts..." on this page : http://flatrock.org.nz/topics/society_culture/sex_and_schopenhauer.htm
>
> to quote it "You can jeopardise your ability to choose a mate appropriately, you can jeopardise your ability to fall in love and you can jeopardise your ability to feel attachment."
>
> comments?
>I would totally agree. Of course, I will take a loss in amorousness over a full depressive relapse any day.
You might also find the following presentation by Dr. Helen Fisher interesting....
http://www.medscape.com/viewarticle/482059_1
We won't always have to take medications that dampen our sense of libido. Newer drug classes that are currently being researched will most likely not continue this vexing problem.
http://www.neurotransmitter.net/newdrugs.html
Posted by ed_uk on November 1, 2004, at 10:14:24
In reply to Re: Unrequited love, sex, attachment, and serotonin. » lostforwards, posted by jrbecker on November 1, 2004, at 9:27:35
Thank you jrbecker :)
Just read it, it was an excellent article.
ed
Posted by tinydancer on November 1, 2004, at 12:02:13
In reply to Unrequited love, sex, attachment, and serotonin., posted by lostforwards on November 1, 2004, at 8:51:50
Posted by Kari1 on November 1, 2004, at 12:18:38
In reply to Re: Unrequited love, sex, attachment, and serotonin., posted by ed_uk on November 1, 2004, at 10:14:24
I don't know if this is relevant to this particular topic, but I will give it a try. I've had, and have a lot of boughts of mania, and I don't know if seratonin has anything to do with my problem, but: I haven't wanted sex for the last 2 1/2 years...since my son was born, and during most of that time I was on Zoloft. Anyway, just recently, after being off all meds pretty much...and since being diagnosed bi-polar, i've gotten my sex-drive back. I'm not on any "anti-depressents" anymore, just mood-elevators basically (topamax/lamicatal) and my sex drive is still back. Do you think it's back to stay??? I was even on Symbyax there for awhile for around 3-4 months...and it still was gone. Like I said...just within the last month....going from just lamictal,(weaning myself off)to now topamax as well. Do you think these will have a negative side effect on my sex drive as my dose gets stronger? I'm on 50 topamax now, but will eventually be at 125. Thanks....
Posted by lostforwards on November 1, 2004, at 14:02:19
In reply to Re: Unrequited love, sex, attachment, and serotonin., posted by linkadge on November 1, 2004, at 9:24:42
> You're right in some sences.
>
> SSRI's can lession obsessions. Even so to the point of having no obsessions. This can extend to sexual and relationship behaviors.
>
>
> However, there was a study done that showed that the people who were least depressed naturally (scored lowest on depression and anxiety scales), also had the least interest in sex!. One researcher concluded.. it is as if they naturally had prozac in their brains.
>
> This is true for me. When I am depressed, I seed consolation from others. When I am not depressed I am more independant, and want to stay that way.
>
> I think a lot about this stuff too, really is a mind bender.
>
>
> Linkadge
>
I've read a page somewhere on sex-addiction, that mentioned a connection between depression and having a high sex drive too. Actually that's sort of the way I felt after all this akinesia. I felt 'post-orgasmic', and I wasn't depressed. I just didn't feel like doing anything. I didn't feel I needed anything. I was in this weird really satisfied state of mind until it started to gradually clear up. ( and it's still got a long way to go - my arms have yet to swing )
Posted by lostforwards on November 1, 2004, at 14:05:34
In reply to Re: Unrequited love, sex, attachment, and serotonin., posted by Kari1 on November 1, 2004, at 12:18:38
> I don't know if this is relevant to this particular topic, but I will give it a try. I've had, and have a lot of boughts of mania, and I don't know if seratonin has anything to do with my problem, but: I haven't wanted sex for the last 2 1/2 years...since my son was born, and during most of that time I was on Zoloft. Anyway, just recently, after being off all meds pretty much...and since being diagnosed bi-polar, i've gotten my sex-drive back. I'm not on any "anti-depressents" anymore, just mood-elevators basically (topamax/lamicatal) and my sex drive is still back. Do you think it's back to stay??? I was even on Symbyax there for awhile for around 3-4 months...and it still was gone. Like I said...just within the last month....going from just lamictal,(weaning myself off)to now topamax as well. Do you think these will have a negative side effect on my sex drive as my dose gets stronger? I'm on 50 topamax now, but will eventually be at 125. Thanks....
I've never been on Topamax. I have been on a low dose of Lamictal though and I found it increased my sex drive. One time, when I was off my lithium for a while, dramatically.
Posted by lostforwards on November 1, 2004, at 17:34:10
In reply to Let's just say that comment explains a WHOLE lot. (nm), posted by tinydancer on November 1, 2004, at 12:02:13
i'll try not to get too creative re that.
Posted by JohnDoenut on November 1, 2004, at 17:58:34
In reply to Re: Let's just say that comment explains a WHOLE lot. » tinydancer, posted by lostforwards on November 1, 2004, at 17:34:10
I found this part of the article quite interesting:
"Also, without frequent orgasms, men and women don’t have the flood of oxytocin and vasopressin that promote relationship bonding. Men might enjoy a woman’s company, but never fall head over heels for her. Semen may also be critical in retaining a woman’s interest, as recent studies indicate that men may alter women’s emotional states through chemicals transmitted through semen."
Crazy huh?!
:)
Posted by Dr. Bob on November 1, 2004, at 18:33:25
In reply to Unrequited love, sex, attachment, and serotonin., posted by lostforwards on November 1, 2004, at 8:51:50
> This has been one of my favourite topics ever since I read Brave New World...
I'd just like to plug the double double quotes feature at this site:
http://www.dr-bob.org/babble/faq.html#amazon
The first time anyone refers to a book, movie, or music without using this option, I post this to try to make sure he or she at least knows about it. It's just an option, though, and doesn't *have* to be used. If people *choose* not to use it, I'd be interested why not, but I'd like that redirected to Psycho-Babble Administration:
http://www.dr-bob.org/babble/admin/20020918/msgs/7717.html
Thanks!
Bob
Posted by jrbecker on November 3, 2004, at 12:45:51
In reply to Re: double double quotes » lostforwards, posted by Dr. Bob on November 1, 2004, at 18:33:25
http://www.currentpsychiatry.com/2004_11/1104_Nelson.asp
CURRENT PSYCHIATRY
Vol. 3, No. 11 / November 2004Sex and antidepressants: When to switch drugs or try an antidote
Help patients stay on depression treatment by reducing sexual side effects.
Erik Nelson, MD
Assistant professor
Department of psychiatry
University of Cincinnati College of Medicine, Cincinnati, OHAntidepressants’ sexual side effects can often be managed—while preserving the antidepressant effect—by altering dosages, switching to another drug class, or adding an “antidote.” Understanding the benefits and risks of each strategy can help you:
• base treatment choices on your patient’s history and side-effect experience
• improve long-term compliance with anti- depressant regimens.Effects vary by antidepressant class
Antidepressants may affect one or more phases of sexual functioning:• desire (libido)
• arousal (erection or vaginal lubrication)
• orgasm/ejaculation.Sexual symptoms linked to antidepressants range from diminished interest/arousal and delayed orgasm to heightened sexual functioning (Table 1). Resulting sexual dysfunction can impair quality of life and intimate relationships and discourage patients from taking antidepressants (Box).1,2
Although most reports have focused on SSRIs, all antidepressant classes have been associated with sexual dysfunction, with prevalence likely influenced by differences in neurotransmitter modulation (Table 2).1,3,4 The highest rates of sexual side effects have been reported with SSRIs, certain tricyclic antidepressants (TCAs), and monoamine oxidase inhibitors (MAOIs).
A recent study reported similarly high rates with mirtazapine, but its small sample size limits conclusions about side effect prevalence with this drug.1 Other studies have found significantly lower rates with bupropion and nefazodone.
TCAs’ sexual side-effect rates and types depend on how much each drug inhibits serotonin reuptake. Clomipramine appears to have the highest rates of sexual dysfunction—particularly anorgasmia—probably because it inhibits the serotonin transporter more than do other TCAs.5 In TCAs with lesser effects on serotonergic neurotransmission, alpha-adrenergic and cholinergic receptor blockade may cause sexual side effects—particularly erectile dysfunction (ED).
Cholinergic agonists such as bethanechol, 10 to 50 mg/d, may reverse sexual dysfunction caused by anticholinergic effects.6 Cyproheptadine—a nonselective serotonin receptor antagonist—has also shown benefit at 4 to 12 mg/d in treating TCA-related sexual side effects.7
MAOIs. Sexual side effects appear to be more prevalent with MAOIs than with TCAs,4 perhaps similar to the rate seen with SSRIs. MAOIs directly increase serotonergic neurotransmission, and their substantial alpha-adrenergic antagonist effects may also produce sexual side effects.
Waiting for symptoms to subside may be appropriate, as anorgasmia caused by MAOIs may remit spontaneously. Sildenafil8 and cyproheptadine9 may reverse MAOI sexual side effects, although serious toxicity has been reported in a patient taking cyproheptadine and an MAOI.10
SSRIs. Increased serotonergic neurotransmission is widely believed to cause SSRI sexual side effects. Resulting secondary effects—such as inhibited central dopamine release, increased prolactin secretion, and inhibited nitric oxide synthesis—may also play important roles.
In general, SSRIs appear to alter sexual functioning in 40% to 60% of patients—both men and women. Anorgasmia is the most commonly reported sexual symptom.
Although all SSRIs are associated with sexual dysfunction, some studies have found higher rates with paroxetine. One study associated paroxetine with significantly higher rates of ED compared with other SSRIs. The authors attributed this finding to paroxetine’s greater anticholinergic effects or to its directly decreasing nitric oxide synthesis.3
SSRI management strategies
Waiting. The simplest, safest way to manage SSRI-related sexual dysfunction is to wait and see if side effects resolve spontaneously. Sexual side effects improve without treatment in approximately 20% of cases,3 although improvement is often incomplete. Moreover, several months may pass before symptoms diminish adequately, making this strategy impractical for patients with substantial sexual dysfunction.Dosing changes. Because SSRIs’ sexual side effects appear to be dose-related,11 carefully reducing the dosage may reduce sexual dysfunction without compromising antidepressant efficacy. This strategy is most likely to sustain remission when you avoid dosages that have proven ineffective. For example, consider a patient who achieves remission of depressive symptoms when fluoxetine is increased from 20 to 40 mg/d. If sexual side effects emerge at 40 mg/d, relapse may be less likely at 30 mg/d than at 20 mg/d.
Other strategies that lessen sexual side effects for some patients include:
• dividing the dosage
• delaying dosing until after sexual activity
• allowing 2- to 3-day “drug holidays” over weekends, when sexual activity is more likely to occur.12Drug holidays probably would not help patients taking fluoxetine, as plasma concentrations would not drop sufficiently in 2 to 3 days to alleviate sexual side effects. Also, drug holidays are presumably safest for patients who are in maintenance treatment, are asymptomatic, and have no history of rapid symptom recurrence or withdrawal effects when discontinuing SSRIs.12
Switching medications. When sexual side effects do not resolve spontaneously or with dose reduction, consider switching to an antidepressant with a lower incidence of sexual dysfunction.
Bupropion has been shown to improve sexual functioning in patients treated for depression. One study reported improved sexual functioning in patients with SSRI-induced sexual side effects who were switched to bupropion.13 Similar studies have shown benefits with substituting nefazodone or mirtazapine for an SSRI.
These uncontrolled studies suggest that switching some patients to a non-SSRI antidepressant may diminish sexual side effects while continuing antidepressant efficacy. Bupropion or nefazodone may be more effective for this purpose, as mirtazapine showed a high rate of sexual side effects in a large observational study.1
Use caution when switching from an SSRI to nefazodone, as cytochrome P-450 2D6 isoenzyme inhibition may increase levels of mCPP—a nefazodone metabolite with anxiogenic properties. To avoid this interaction, taper the SSRI before starting nefazodone.
Switching medications may not be ideal for patients with an unacceptable depression relapse risk, characterized by severe dysfunction, suicidal ideation, or past treatment resistance.
Using an antidote
Adding a second medication to antidepressant therapy is another strategy to consider. An antidote seems most practical when:• a patient clearly benefits from an antidepressant regimen
• the risk of losing efficacy with a new medication is high
• reducing the dosage or waiting for sexual dysfunction to resolve spontaneously are impractical or have failed.Most reports of sexual side effect antidotes have been open-label trials of drugs thought to:
• improve some aspect of sexual functioning as with dopamine or noradrenergic agonists)
• or block antidepressant mechanisms suspected of contributing to sexual side effects (as with serotonin receptor antagonists or cholinergic agonists).Unfortunately, controlled trials with many of these strategies have been less than promising (Table 3).5,14-28 Several trials reported high placebo-response rates—which may complicate assessment of any sexual side effect treatment—and most produced negative results. Two notable exceptions have been sildenafil and bupropion.
Sildenafil, a phosphodiesterase-5 inhibitor, showed greater benefit than placebo in a prospective trial of 90 depressed men (mean age 45) diagnosed with sexual dysfunction caused by an SSRI.28 The men took sildenafil, 50 to 100 mg, 1 hour before sexual activity.
After 6 weeks, 55% of sildenafil-treated patients were rated as much/very much improved on the Clinical Global Impression Scale adapted for Sexual Function, compared with 4% of those taking placebo, a statistically significant difference. Measures used to assess sexual function showed that arousal, erectile function, and orgasm improved significantly, with a lesser effect on desire. This suggests that adjunctive sildenafil reduces SSRIs’ sexual side effects, and this benefit may extend beyond improving ED.
Sildenafil improves peripheral vasodilatation due to smooth muscle relaxation caused by enhanced nitric oxide release. Other sexual side effects—such as delayed orgasm/ejaculation—may improve because of indirect effects of increased penile and clitoral blood flow caused by vasodilatation.29
Sildenafil treatment was well-tolerated; the most common side effects were headache (40.5%), flushing (16.7%), dyspepsia (7.1%), nasal congestion (11.9%), and transient visual disturbances (11.9%).
Bupropion has also shown therapeutic efficacy for SSRI-related sexual dysfunction in a 4-week, placebo-controlled trial of 55 patients (mean age 39) diagnosed with SSRI-induced sexual dysfunction.15 Compared with the placebo group, those receiving add-on bupropion SR, 150 mg bid, improved significantly more in sexual desire and frequency of sexual activity, as measured by the Changes in Sexual Functioning Questionnaire.
Measures of arousal, orgasm, and global sexual functioning did not differ significantly between the two groups. Bupropion added to SSRI treatment was well-tolerated; most-commonly reported side effects were irritability (12%), dry mouth (12%), and headache (15%).
Other ED treatments. Two additional phosphodiesterase-5 inhibitors have become available in the past year. Like sildenafil, tadalafil and vardenafil are indicated for treating ED. They may be useful as alternatives for patients who do not respond to or tolerate sildenafil, although no published studies have examined their use in antidepressant-induced sexual dysfunction.
Recommendation. Based on the evidence, it seems reasonable to start with bupropion or sildenafil when considering an antidote for sexual side effects caused by SSRIs or other medications with strong serotonergic effects. Determining which agent would be “first-line” depends on patient factors, as summarized in Table 4.30,31 For example:
• Bupropion has been reported to augment SSRIs’ antidepressant effects32 and thus may provide added benefit in patients with residual depressive symptoms.
• Bupropion is more effective than sildenafil for improving sexual desire and thus would be preferred for patients in whom this sexual dysfunction symptom is prominent.
• Sildenafil appears to be more effective than bupropion for improving overall sexual satisfaction for men experiencing substantial erectile dysfunction.
References
1. Clayton AH, Pradko JF, Croft HA, et al. Prevalence of sexual
dysfunction among newer antidepressants. J Clin Psychiatry 2002;63(4):357-66.
2. Worthington JJ 3rd, Peters PM. Treatment of antidepressant-induced sexual dysfunction. Drugs Today (Barc) 2003;39(11):887-96.
3. Montejo AL, Llorca G, Izquierdo JA, Rico-Villademoros F. Incidence of sexual dysfunction associated with antidepressant agents: a prospective multicenter study of 1022 outpatients. Spanish Working Group for the Study of Psychotropic-Related Sexual Dysfunction. J Clin Psychiatry 2001;62(suppl 3):10-21.
4. Harrison WM, Rabkin JG, Ehrhardt AA, et al. Effects of antidepressant medication on sexual function: a controlled study. J Clin Psychopharmacol 1986;6(3):144-9.
5. Monteiro WO, Noshirvani HF, Marks IM, Lelliott PT. Anorgasmia from clomipramine in obsessive-compulsive disorder. A controlled trial. Br J Psychiatry 1987;151:107-12.
6. Gross MD. Reversal by bethanechol of sexual dysfunction caused by anticholinergic antidepressants. Am J Psychiatry 1982;139(9):1193-4.
7. Sovner R. Treatment of tricyclic antidepressant-induced orgasmic inhibition with cyproheptadine. J Clin Psychopharmacol 1984; 4(3):169.
8. Gupta S, Masand P, Ashton AK, Berry SL. Phenelzine-induced sexual dysfunction treated with sildenafil. J Sex Marital Ther 1999; 25(2):131-5.
9. Decastro RM. Reversal of MAOI-induced anorgasmia with cyproheptadine. Am J Psychiatry 1985;142(6):783.
10. Kahn DA. Possible toxic interaction between cyproheptadine and phenelzine. Am J Psychiatry 1987;144(9):1242-3.
11. Montejo-Gonzalez AL, Llorca G, Izquierdo JA, et al. SSRI-induced sexual dysfunction: fluoxetine, paroxetine, sertraline, and fluvoxamine in a prospective, multicenter, and descriptive clinical study of 344 patients. J Sex Marital Ther 1997;23:176-94.
12. Rothschild AJ. Selective serotonin reuptake inhibitor-induced sexual dysfunction: efficacy of a drug holiday. Am J Psychiatry 1995;152(10):1514-16.
13. Clayton AH, McGarvey EL, Abouesh AI, Pinkerton RC. Substitution of an SSRI with bupropion sustained release following SSRI-induced sexual dysfunction. J Clin Psychiatry 2001;62(3):185-90.
14. Shrivastava RK. Amantadine in the treatment of sexual dysfunction associated with selective serotonin reuptake inhibitors. J Clin Psychopharmacol 1995;15:83-84.
15. Clayton AH, Warnock JK, Kornstein SG, et al. A placebo-controlled trial of bupropion SR as an antidote for selective serotonin reuptake inhibitor-induced sexual dysfunction. J Clin Psychiatry 2004;65(1):62-7.
16. Meston CM. A randomized, placebo-controlled, crossover study of ephedrine for SSRI-induced female sexual dysfunction. J Sex Marital Ther 2004;30(2):57-68.
17. Roeloffs C, Bartlik B, Kaplan PM, Kocsis JH. Methylphenidate and SSRI-induced sexual side effects. J Clin Psychiatry 1996;57(11):548.
18. DeBattista C, Solvason HB, Breen JA, Schatzberg AF. Pramipexole augmentation of a selective serotonin reuptake inhibitor in the treatment of depression. J Clin Psychopharmacol 2000;20(2):274-5.
19. Worthington JJ 3rd, Simon NM, Korbly NB, et al. Ropinirole for antidepressant-induced sexual dysfunction. Int Clin Psychopharmacol 2002;17(6):307-10.
20. Aizenberg D, Zemishlany Z, Weizman A. Cyproheptadine treatment of sexual dysfunction induced by serotonin reuptake inhibitors. Clin Neuropharmacol 1995;18:320-4.
21. Nelson EB, Keck PE Jr., McElroy SL. Resolution of fluoxetine-induced sexual dysfunction with the 5-HT3 antagonist granisetron (letter). J Clin Psychiatry 1997;58:496-7.
22. Aizenberg D, Naor S, Zemishlany Z, Weizman A. The serotonin antagonist mianserin for treatment of serotonin reuptake inhibitor-induced sexual dysfunction in women: an open-label add-on study. Clin Neuropharmacol 1999;22:347-50.
23. Farah A. Relief of SSRI-induced sexual dysfunction with mirtazapine treatment. J Clin Psychiatry 1999;60:260-1.
24. Reynolds RD. Sertraline-induced anorgasmia treated with intermittent nefazodone. J Clin Psychiatry 1997;58:89.
25. Jacobsen F. Fluoxetine-induced sexual dysfunction and an open trial of yohimbine. J Clin Psychiatry 1992;53:119-22.
26. Michelson D, Bancroft J, Targum S, et al. Female sexual dysfunction associated with antidepressant administration: a randomized, placebo-controlled study of pharmacologic intervention. Am J Psychiatry 2000;157(2):239-43.
27. Kang BJ, Lee SJ, Kim MD, Cho MJ. A placebo-controlled, double-blind trial of Ginkgo biloba for antidepressant-induced sexual dysfunction. Hum Psychopharmacol 2002;17(6):279-84.
28. Nurnberg HG, Hensley PL. Sildenafil citrate for the management of antidepressant-associated erectile dysfunction. J Clin Psychiatry 2003;64(suppl 10):20-5.
29. Zajecka J. Strategies for the treatment of antidepressant-related sexual dysfunction. J Clin Psychiatry 2001;62(suppl 3):35-43.
30. DeBattista C, Solvason HB, Poirier J, et al. A prospective trial of bupropion SR augmentation of partial and non-responders to serotonergic antidepressants. J Clin Psychopharmacol 2003;23:27-30.
31. Ashton AK, Rosen RC. Bupropion as an antidote for serotonin reuptake inhibitor-induced sexual dysfunction. J Clin Psychiatry 1998;59:112-15.
32. Nurnberg HG, Gelenberg A, Hargreave TB, et al. Efficacy of sildenafil citrate for the treatment of erectile dysfunction in men taking serotonin reuptake inhibitors. Am J Psychiatry 2001;158:1926-8.Related resources
Worthington JJ 3rd, Peters PM. Treatment of antidepressant-induced sexual dysfunction. Drugs Today (Barc) 2003;39(11):887-96.
Montgomery SA, Baldwin DS, Riley A. Antidepressant medications: a review of the evidence for drug-induced sexual dysfunction. J Affect Disord 2002;69(1-3):119-40.
Drug brand names
Amantadine • Symmetrel
Bethanechol • Duvoid, Urecholine, Urabeth
Bupropion SR • Wellbutrin SR
Buspirone • Buspar
Citalopram • Celexa
Clomipramine • Anafranil
Cyproheptadine • Periactin
Fluoxetine • Prozac
Granisetron • Kytril
Methyphenidate • Ritalin
Mianserin • Bolvidon, Norval
Mirtazapine • Remeron
Nefazodone • Serzone
Paroxetine • Paxil
Pramipexole • Mirapex
Ropinirole • Requip
Sertraline • Zoloft
Sildenafil • Viagra
Tadalafil • Cialis
Vardenafil • Levitra
Venlafaxine • Effexor
This is the end of the thread.
Psycho-Babble Medication | Extras | FAQ
Dr. Bob is Robert Hsiung, MD,
bob@dr-bob.org
Script revised: February 4, 2008
URL: http://www.dr-bob.org/cgi-bin/pb/mget.pl
Copyright 2006-17 Robert Hsiung.
Owned and operated by Dr. Bob LLC and not the University of Chicago.