The introduction of the Wegovy (semaglutide) tablet marks a significant milestone in obesity management, offering the first oral GLP-1 receptor agonist approved for weight loss. Patients who dislike injecting themselves now have a proven GLP option. Like its injectable counterpart, the tablet works by mimicking the GLP-1 hormone to regulate appetite and food intake.

In trials, Wegovy injections caused an average of 13-16% weight loss over 68 or more weeks, depending on the study. The Wegovy pill has been studied in one small trial (N=307), where it led to an average weight loss of 13.6% over 64 weeks. Notedly, Novo Nordisk has been advertising 17% weight loss with the pill in what it calls a "trial-product estimand" that estimates the pill's efficacy if every subject had adhered perfectly to therapy. This outcome is biased because it excludes patients who stopped the medication due to adverse events, lack of effectiveness, or a combination of the two. The pill's side effects are mainly gastrointestinal and similar to the shot. One side effect unique to the pill is dysesthesia (sensitive skin, hyperesthesia, and skin burning sensations), which was reported by 5% of subjects. The pill is taken once daily on an empty stomach in the morning with water, and patients should not eat or drink for 30 minutes afterwards. This may not be as convenient as the once-weekly injection for some patients.

Current pricing for each therapy is outlined below. It's likely GLP therapy prices will continue to decline, as Eli Lilly is set to release its own pill in the near future.

Wegovy injection

• 0.25 mg and 0.5 mg: $199/month for new patients, otherwise $349/month
• 1.0 mg, 1.7 mg, and 2.4 mg: $349/month

Wegovy pills

• 1.5 mg: $149/month
• 4 mg: $149/month for new patients, otherwise $199/month
• 9 mg and 25 mg: $299/month

• Wegovy review
• Article on webpage

For decades, conventional wisdom has held that coffee and caffeine act as triggers for heart rhythm disorders, particularly atrial fibrillation (AF). Patients with arrhythmias are routinely advised to avoid caffeinated beverages to reduce the risk of palpitations and AF episodes. This belief stems mainly from the known stimulant effects of caffeine and anecdotal patient reports. However, scientific evidence supporting this theory has been inconsistent. While caffeine can acutely raise heart rate, several large observational studies have actually suggested a neutral or even protective association between regular coffee consumption and the development of AF. Until recently, randomized clinical trial data to definitively settle this debate has been lacking.

The DECAF (Does Eliminating Coffee Avoid Fibrillation?) randomized clinical trial, published in JAMA in 2025, sought to address this gap. The study enrolled 200 adults who were regular coffee drinkers and had a history of persistent AF or atrial flutter. Following successful electrical cardioversion to restore normal sinus rhythm, participants were randomly assigned to either continue drinking caffeinated coffee (at least one cup daily) or to completely abstain from all coffee and caffeine products for six months. The primary outcome was the clinically detected recurrence of AF or atrial flutter. Surprisingly, the group randomized to coffee consumption experienced significantly fewer arrhythmia recurrences. Specifically, AF or atrial flutter recurred in 47% of the coffee consumption group compared to 64% of the abstinence group. This difference translated to a 39% lower hazard of recurrence for those who continued drinking coffee (Hazard Ratio 0.61; 95% CI, 0.42-0.89; P=.01). Adherence to the study protocols was good, with the coffee group consuming a median of 7 cups per week and the abstinence group reducing intake to near zero.

These findings directly contradict the long-standing assumption that coffee worsens AF. The authors suggest several potential mechanisms for this protective effect, including caffeine's blockade of adenosine receptors (adenosine can promote AF), coffee's anti-inflammatory properties, and potential diuretic effects. While the study had some limitations, such as its open-label design and modest sample size, it provides the strongest evidence to date that moderate caffeinated coffee consumption is safe and potentially beneficial for patients with atrial fibrillation. For patients who enjoy their daily cup, these results offer reassurance that coffee does not need to be on the restricted list.

• Caffeinated Coffee Consumption or Abstinence to Reduce Atrial Fibrillation: The DECAF Randomized Clinical Trial, JAMA (2025)
• Atrial fibrillation review
• Article on webpage

Lynkuet (elinzanetant), a nonhormonal treatment for vasomotor symptoms (VMS) due to menopause, was recently approved by the FDA. It is the second drug approved in the neurokinin (NK) receptor antagonists class, following Veozah (fezolinetant), approved in 2023. The drugs differ slightly in their NK receptor binding; Veozah selectively binds NK3 receptors while Lynkuet binds NK1 and NK3 receptors. During menopause, estrogen withdrawal increases neurokinin activity in the brain's thermoregulatory center, and NK receptor antagonists suppress neurokinin secretion.

In their respective phase 3 trials, both agents demonstrated a statistically significant reduction in VMS frequency and severity (≥ hot flashes over 24 hours) compared to placebo. In two 12-week trials, the placebo-subtracted reduction in VMS episodes (baseline ∼ 11 episodes/day) with Veozah was about 2.5 per 24 hours. Similarly, the placebo-subtracted reduction in VMS episodes (baseline ∼ 14 episodes/day) with Lynkuet was about 3.2 per 24 hours in 12-week trials. Notably, across all trials, the placebo group experienced reductions of 4 to 6 episodes per day, suggesting a significant psychological component in VMS improvement. Common side effects for both agents include gastrointestinal issues like abdominal pain and diarrhea, as well as nervous system effects such as insomnia, back pain, and headache. Lynkuet's label notes a central nervous system (CNS) depressant effect, with somnolence and dizziness occurring in ≥ 5% of patients. Veozah has a Boxed Warning for hepatotoxicity, with transaminase elevations >3X ULN reported in 2.3% of women in pooled clinical trials. In Linkuet trials, transaminase elevations ≥ 3X ULN occurred in 0.6% of Lynkuet-treated women and 0.4% of placebo-treated women. Both manufacturers recommend monitoring liver function tests during therapy. A major difference in drug-drug interactions stems from different metabolic profiles: Veozah is a CYP1A2 substrate and is contraindicated with CYP1A2 inhibitors, while Lynkuet is primarily metabolized by CYP3A4 and requires dosage modification or avoidance when used with CYP3A4 inhibitors or inducers.

Women suffering from menopause-related VMS now have two nonhormonal options; however, both medications are significantly more expensive than hormone replacement therapy (HRT) and often require prior authorization along with stepped therapy for insurance coverage. A study comparing Veozah or Lynkuet to HRT would be informative.

• Lynkuet (elinzanetant) review
• Veozah (fezolinetant) review
• HRT guidelines
• Article on webpage

Current treatment guidelines for provoked VTE (i.e., VTE after immobilization, surgery, extended travel, or pregnancy) recommend three months of anticoagulation. Anticoagulation beyond three months (extended anticoagulation) is typically reserved for patients with strong, persistent VTE risk factors, including active cancer or thrombophilia. The effects of extended anticoagulation on patients with provoked VTE who have minor chronic VTE risk factors (e.g., obesity, CVD) are unknown. To explore this clinical gap, researchers performed the HI-PRO trial, where 600 adults with provoked VTE and minor chronic VTE risk factors were randomized to 12 months of apixaban (2.5 mg twice daily) or placebo after completing at least 3 months of anticoagulation. The prevalence of minor risk factors and results after one year were as follows:

• Chronic VTE risk factors: Chronic inflammatory or autoimmune disorder - 52%, Obesity - 48%, CVD - 29%, Chronic lung disease - 22%, Chronic kidney disease - 11%
• Symptomatic recurrent VTE: Apixaban - 1.3%, Placebo - 10% (P<0.001)
• Major bleeding: Apixaban - 0.3%, Placebo - 0% (P>0.999)

In the HI-PRO trial, extended anticoagulation was superior to three months of anticoagulation in patients with provoked VTE who had minor chronic risk factors for recurrence (55% of participants had two or more risk factors). The first-year VTE recurrence rate in the placebo group was 10%, which is notably higher than the 1–6% rate observed in other studies enrolling patients with provoked VTE. The unexpectedly high placebo recurrence rate and the resulting clinical benefit from extended anticoagulation suggest that current risk stratification models may underestimate the impact of less significant chronic risk factors (e.g., chronic inflammatory disorders, CVD, obesity) when determining the need for indefinite anticoagulation following a provoked VTE. One limitation of the study is the 12-month treatment duration, which may not reflect the full risks and benefits of lifelong anticoagulation. It will be interesting to see how future guidelines incorporate data from this study. In the interim, providers may consider discussing the implications of this study with patients who present with provoked VTE and coexisting minor, long-term risk factors for recurrence.

• Extended Anticoagulation vs Standard Duration (3 months) after Provoked VTE, NEJM (2025)
• Article on webpage

Catheter ablation has become a common treatment for atrial fibrillation (AF), and many patients undergo the procedure in hopes of stopping anticoagulation. Catheter ablation success, defined as no atrial arrhythmias, depends on the type of AF and the length of follow-up. One-year success rates for paroxysmal AF are 70% to 85%, while persistent AF has a success rate of 50% to 70%. Over longer follow-up periods, success rates decline. Since catheter ablation is not 100% curative, and AF can come and go without symptoms, stopping anticoagulation after the procedure may increase stroke risk. Conversely, continuing anticoagulation increases bleeding risk. To examine the issue, researchers performed the ALONE-AF trial, where 840 patients (median CHA2DS2-VASc score of 2) with AF who had undergone catheter ablation and had no documented AF recurrence for at least one year were randomized to continuing anticoagulation (with apixaban or rivaroxaban) or stopping it. No atrial arrhythmia recurrence was documented with ECGs and at least two sessions of 24- to 72-hour Holter monitoring, with at least one performed within two months of enrollment. After two years, the primary outcome, a composite of stroke, systemic embolism, and major bleeding, was observed in 0.3% of the discontinue group and 2.2% of the continue group (P=0.02). Stroke was seen in 0.3% and 1.4%, respectively, and major bleeding in 0% and 1.4% (P=0.03).

Prior to this study, providers had limited data on the risks and benefits of stopping anticoagulation after ablation. The criteria used in the study for documenting no AF recurrence (at least two sessions of 24- to 72-hour Holter monitoring without atrial arrhythmia) serve as a starting point for selecting patients for anticoagulant discontinuation. Most patients in the study had paroxysmal AF (68%), which is more responsive to ablation. Although the study did not find differences in outcomes for patients with persistent AF, this subgroup was underrepresented.

• ALONE-AF Study: Discontinue vs Continue anticoagulation after ablation, JAMA (2025)
• Article on webpage