The American College of Physicians (ACP) recently published migraine prevention guidelines. The recommendations are based on a systematic review and network meta-analysis that they performed and are intended for nonpregnant adults with episodic migraine (defined as 1 to 14 headache days per month). Key recommendations include:

• First-line therapies: Beta-blocker (metoprolol or propranolol), valproate, venlafaxine, amitriptyline
• Second-line therapies: CGRP receptor antagonists (atogepant, rimegepant) or CGRP antibodies (eptinezumab, erenumab, fremanezumab, or galcanezumab)
• Third-line therapy: Topiramate

All of the guidelines are based on low-certainty evidence, as there are few meaningful head-to-head trials comparing migraine drugs. Their reasoning for recommending CGRP drugs over topiramate is that topiramate has a less favorable side effect profile.

Migraine prevention has always been the Wild West of pharmacotherapy, as a broad range of medications with seemingly unrelated mechanisms are used for treatment. Fortunately, most recommended drugs are affordable. The newer CGRP drugs are expensive and have modest efficacy in trials, reducing average migraine days per month by 1 - 2 compared to placebo. Notably, placebo typically performs well in migraine trials, likely reflecting overdiagnosis, as patients and some providers tend to label all headache syndromes as migraines.

• Migraine headache review
• Migraine headache medications
• Article on webpage

Bacterial vaginosis (BV), affecting up to 30% of young women, has a high recurrence rate, with over 50% of women experiencing reinfection within 12 weeks. The cause of BV is poorly understood, but women who report sex with a regular partner have twice the risk of those who are not sexually active. This observation has led to speculation that the condition is sexually transmitted. However, previous studies where females and their male partners were treated with oral therapy have not demonstrated a reduction in recurrence. One possible explanation for these findings is that oral therapies alone may not be sufficient to clear cutaneous penile carriage of bacterial vaginosis–associated organisms. To test this theory, Australian researchers randomized monogamous couples in which the woman had BV to female-only treatment (female-only group) or female and male partner treatment (partner-treatment group). In both groups, females received metronidazole 400 mg twice daily for 7 days or intravaginal metronidazole or clindamycin if contraindicated. In the partner-treatment group, males received the same metronidazole regimen along with 2% clindamycin cream applied to the penile skin twice daily for 7 days. During follow-up, females were tested for BV at day 8, week 4, week 8, week 12, and as needed for symptoms. At study conclusion, the primary outcome, BV recurrence within 12 weeks, was significantly lower in the partner-treatment group compared to the female-only group (35% vs 63%, p<0.001)

This study provides some insight into BV and sexual transmission. It also raises the question of whether topical therapy alone in male partners, including over-the-counter creams like Neosporin, could reduce recurrence. Lastly, it's important to note that 35% of women in the partner-treatment group had a recurrence, suggesting that some type of underlying predisposition plays a significant role in BV susceptibility.

• Male-Partner Treatment to Prevent Recurrence of Bacterial Vaginosis, NEJM (2025)
• Genitourinary infections
• Article on webpage

Spinal injections, frequently performed in pain medicine practices, are a common intervention for chronic back pain, with an estimated 9 to 11 million injections performed annually in the US alone. Despite their widespread use, studies examining their efficacy have been mixed, with placebo-controlled trials typically finding no effect. [PMID 21914755, PMID 24988555] To further explore the issue, the British Medical Journal convened a panel comprising four patients with chronic spine pain, 10 clinicians experienced in managing chronic spine pain, and eight methodologists. The group reviewed randomized controlled trials and observational studies involving spine procedures and issued the following recommendations:

• The following procedures have no proven benefit and should not be offered for radicular or axial spine pain in the cervical or lumbar region:
• Epidural injection of local anesthetic, steroids, or their combination
• Joint radiofrequency ablation with or without joint targeted injection of local anesthetic plus steroid
• Joint-targeted injection of local anesthetic, steroids, or their combination
• Intramuscular injection of local anesthetic with or without steroids
• Dorsal root ganglion radiofrequency with or without epidural injection of local anesthetic or local anesthetic plus steroids

These recommendations contradict those of the American Society of Interventional Pain Physicians (ASIPP), a professional organization that represents pain management physicians. The 2021 ASIPP guidelines strongly endorse spinal injections for treating chronic lumbar and cervical pain. In their discussion, the ASIPP authors argue that saline or short-acting local anesthetics, frequently used as controls in steroid injection studies, shouldn't be considered placebos because they have an actual therapeutic effect. They go on to contend that single-arm analysis (i.e., looking at therapies individually without comparing them to a control group) is most telling and should receive the majority of emphasis. Huh?

While it's a little comical and slightly disconcerting that a professional association would make an argument to disregard placebo controls in randomized trials, it's not surprising given that they represent doctors who put their kids through college performing these procedures. It also explains how two professional organizations can come to entirely different conclusions analyzing the same evidence. Like most things in life, all you have to do is follow the money.

• BMJ Practice Guideline on Interventional Procedures for Chronic Spine Pain (2025) [PubMed abstract]
• Low back pain review
• Article on a webpage

For decades, dopamine antagonists have been the primary treatment for psychotic disorders like schizophrenia. While effective, these drugs can have significant side effects. First-generation drugs like haloperidol can cause extrapyramidal symptoms (EPS), while second-generation agents like risperidone are known to induce weight gain and hyperprolactinemia. These adverse effects often limit patient compliance, underscoring the need for alternative therapies. Cobenfy, a combination of xanomeline and trospium chloride, is the first non-dopamine antagonist antipsychotic approved to treat schizophrenia. Xanomeline is a muscarinic cholinergic receptor agonist that preferentially stimulates cerebral M1 and M4 receptors, which are involved in schizophrenia pathophysiology. Trospium is a peripheral-acting antimuscarinic agent included to mitigate xanomeline's cholinergic effects. Cobenfy's side effects are primarily gastrointestinal and include nausea (19%), dyspepsia (18%), constipation (17%), and vomiting (15%). It is contraindicated in patients with liver disease and conditions that may be exacerbated by trospium's anticholinergic effects (e.g., urinary retention, reduced GI motility). It comes in a capsule taken twice daily, at least one hour before or two hours after a meal, as food reduces its absorption by 90%.

Providers treating schizophrenia now have an alternative to dopamine antagonists, which have been the only option since the approval of chlorpromazine in 1954. In two studies (see links below), Cobenfy reduced the score on the Positive and Negative Syndrome Scale (range 30 - 210, with higher scores indicating worse symptoms) by 11 points more than placebo. Head-to-head studies with dopamine antagonists are needed to truly define Cobenfy's therapeutic value.

• Xanomeline-Trospium vs Placebo for Schizophrenia in Adults, Lancet (2024) [Pubmed abstract]
• Xanomeline-Trospium vs Placebo for Schizophrenia in Adults, NEJM (2021) [Pubmed abstract]
• Cobenfy review
• Article on webpage

With the publication of two recent Zepbound (tirzepatide) studies, GLP weight-loss drugs continue their streak of positive trials in obesity-related conditions. In the first study, Zepbound was compared to placebo in 731 patients with heart failure with preserved ejection fraction (HFpEF). After two years of follow-up, the absolute risk of a composite of death from cardiovascular causes or worsening heart failure was 5.4% lower in the Zepbound group (9.9% vs 15.3%). [Pubmed abstract] The second trial (N=1032), a substudy of the SURMOUNT-1 weight-loss trial, found that over 3.4 years, Zepbound significantly reduced the incidence of diabetes compared to placebo in individuals with prediabetes (1.3% vs 13.3%). [Pubmed abstract] These studies add to a growing list of trials, summarized below, where Zepbound and Wegovy (semaglutide) have been found to improve outcomes in obesity-related conditions.

• Obstructive sleep apnea (OSA): In a 52-week trial enrolling overweight adults with OSA (N=469), Zepbound significantly reduced the apnea-hypopnea index, body weight, hypoxic burden, and systolic blood pressure compared to placebo. [Pubmed abstract] In December 2024, Zepbound received FDA approval for moderate to severe OSA in adults with obesity.
• Nonalcoholic steatohepatitis (NASH): In a 52-week study (N=190) enrolling adults with NASH, more patients treated with Zepbound had NASH resolution compared to placebo (62% [15 mg dose] vs 10%) [Pubmed abstract]
• Heart failure with preserved ejection fraction (HFpEF): Like Zepbound, Wegovy has also been shown to improve HFpEF. In a 52-week study (N=529) enrolling obese adults with HFpEF, Wegovy was superior to placebo for improving heart failure symptoms and physical endurance. [Pubmed abstract]
• Secondary prevention of cardiovascular disease (CVD): In a 40-month study (N=17,604) enrolling overweight adults with a history of CVD, Wegovy was superior to placebo for reducing a composite of CVD events (6.5% vs 8%). [Pubmed abstract] Based on this study, Wegovy received FDA approval for the secondary prevention of CVD events.
• Knee osteoarthritis (OA): In a 68-week study (N=407) enrolling obese adults with moderate knee OA, Wegovy was superior to placebo for improving knee pain. [Pubmed abstract]
• Prediabetes: As discussed above, Zepbound was significantly better than placebo at preventing progression to diabetes over 3.4 years in participants with prediabetes (1.3% vs 13.3%). [Pubmed abstract]

To date, the FDA has granted two non-obesity indications for Zepbound and Wegovy: OSA for Zepbound and secondary prevention of CVD events for Wegovy. However, more are sure to come as these highly effective weight-loss drugs continue to change people's lives.

• Article on a webpage