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FDA APPROVES WEGOVY FOR METABOLIC DYSFUNCTION–ASSOCIATED STEATOHEPATITIS (MASH)

obese woman with weight-loss injection
Metabolic dysfunction–associated steatohepatitis (MASH), formerly known as nonalcoholic steatohepatitis, is a common condition, affecting an estimated 25% of American adults and up to 90% of people with a BMI of 40 or greater. Until recently, the only FDA-approved MASH therapy was Resmetirom (Rezdiffra), a thyroid hormone receptor-beta (THR-β) partial agonist. On August 15, 2025, the FDA approved Wegovy for MASH based on an interim analysis of the ESSENCE study that compared Wegovy to placebo in 1,197 patients with MASH and fibrosis stage 2 or 3. At 72 weeks, resolution of steatohepatitis without worsening of fibrosis was observed in 63% of Wegovy-treated patients and 34% of placebo-treated patients (P<0.001). A reduction in liver fibrosis without worsening of steatohepatitis occurred in 37% and 22%, respectively (P<0.001). The Wegovy group lost 10.5% of their body weight compared to 2% in the placebo group.

Less than 20% of commercial health insurance plans cover Wegovy for weight loss, so a MASH indication is encouraging since it may increase access. However, a looming question is what criteria will insurance companies require for a MASH diagnosis. In the ESSENCE study, MASH was diagnosed with a liver biopsy, and only patients with stage 2 or 3 fibrosis were enrolled. Prior authorization criteria for Rezdiffra, which has the exact same indication as Wegovy, vary by insurance, but I know some plans require the following: (1) diagnosis by liver biopsy, Fibroscan, or magnetic resonance elastography (MRE), (2) prescribed by a gastroenterologist or hepatologist. Fibroscan is a specialized ultrasound typically found in gastroenterology practices, and MRE is a specific type of MRI that is not widely available. If insurance companies have the same criteria for Wegovy, it will create a significant barrier to access, especially in primary care.

Tirzepatide (Zepbound) has also been shown to improve MASH, and Eli Lilly is in the process of pursuing a MASH indication for it.
Cancer study shows profound effect of exercise
woman exercising
The benefits of exercise on a wide range of conditions, including everything from ADHD to osteoporosis, have long been known. Now, a randomized controlled trial published in the New England Journal of Medicine has found that exercise improves survival in patients with colorectal cancer. The CHALLENGE study randomized 889 patients with resected colon cancer (stage III or high-risk stage II) who had completed adjuvant chemotherapy to a structured exercise program with required visits over 3 years (exercise group) or general health-education materials (control group). After a median follow-up of 7.9 years, the primary endpoint, 5-year disease-free survival, was 80.3% in the exercise group and 73.9% in the control group (difference, 6.4 percentage points; 95% CI 0.6 to 12.2). Eight-year overall survival was 90.3% and 83.2%, respectively. Notably, weight loss did not differ significantly between groups, so it does not explain the observed effect.

Exercise improved overall survival among colorectal cancer patients by 7%. The study authors note that this effect size is similar to what is observed with many approved drug therapies, minus the side effects and costs. This study provides yet another reason for people to exercise.

IS THE FDA REMOVING ARMOUR THYROID AND SIMILAR PRODUCTS FROM THE MARKET?

Armour thyroid and Nature-Throid bottle
Animal-derived thyroid products, including Armour Thyroid, NP Thyroid, WP Thyroid, and Nature-throid, are not FDA-approved to treat hypothyroidism; however, they existed before the Food, Drug, and Cosmetic Act of 1938 and, therefore, were grandfathered into the FDA's list of prescription drug medications without going through the formal approval process. The products are produced from dried, ground thyroid glands, typically from pigs. The FDA contends that due to a lack of safety and efficacy data, these products may be unsafe because of variations in purity and potency and the presence of contaminants. The agency sent letters to manufacturers on August 6, 2025, notifying them of their intent to take action against unapproved animal-derived thyroid medications. The FDA is also encouraging healthcare providers to transition patients from animal-derived products to synthetic levothyroxine.

An estimated 1.5 million Americans receive prescriptions for animal-derived combination products each year. However, all major professional organizations recommend synthetic levothyroxine products (e.g., Synthroid) for treating hypothyroidism. Reasons they are preferred over combination products include:

  • Combination products (e.g. Armour Thyroid) have a T4 to T3 ratio of 4:1, while physiologic ratios secreted by the thyroid gland are around 14:1.
  • Combination therapy leads to supraphysiologic levels of T3, which may lead to symptoms of thyrotoxicosis
  • T3 has a shorter half-life than T4, which can lead to fluctuations in T3 levels, with a peak occurring shortly after dosing
  • There is substantially more data from trials on the use of levothyroxine compared to combination therapy

In my experience, patients who are on animal-derived combination products have already tried synthetic levothyroxine and feel that the combination products control their symptoms better. However, blinded studies comparing levothyroxine to combination products have not found a difference in symptom control. Despite this, it can be difficult to change patient perceptions, especially with regard to subjective symptoms. I anticipate significant pushback when trying to switch these patients to levothyroxine products.
Dapagliflozin evaluated for metabolic dysfunction-associated steatohepatitis in small study
illustration of a liver
Metabolic dysfunction–associated steatohepatitis (MASH), formerly known as nonalcoholic steatohepatitis, is a chronic liver disease strongly associated with obesity and diabetes. Dapagliflozin (Farxiga), an SGLT2 inhibitor approved to treat type 2 diabetes, has been associated with modest weight loss in clinical trials. A small study (N=154) conducted in China evaluated the effects of dapagliflozin on MASH in Chinese adults with or without type 2 diabetes who had biopsy-diagnosed MASH (average BMI 29.2 | type 2 diabetes - 45%). Subjects were randomized to dapagliflozin 10 mg once daily or placebo for 48 weeks. At the end of the trial, the primary outcome, MASH improvement without worsening of liver fibrosis, occurred in 53% of dapagliflozin-treated patients and 30% of placebo-treated patients (p=0.006). Fibrosis improvement without worsening MASH was seen in 45% and 20%, respectively (p=0.001). Over the course of the trial, the dapagliflozin group lost an average of 9.4 lbs, while the placebo group lost 1.7 lbs.

In the small study above, dapagliflozin improved MASH in Chinese people with and without diabetes. An exploratory mediation analysis of the results found that weight loss largely accounted for the higher proportion of MASH improvement and MASH resolution in the dapagliflozin group. However, fibrosis improvement without worsening of MASH was found to be independent of weight loss. Proposed mechanisms by which dapagliflozin may improve MASH independent of weight loss include: (1) modulation of energy homeostasis and improvement of insulin resistance, (2) anti-inflammatory, anti-oxidant, and anti-fibrotic effects, (3) systemic metabolic reprogramming and negative energy balance, and (4) promotion of ketone body synthesis.

Weight loss in the dapagliflozin group was much greater in this trial than what has been observed in diabetes and heart failure trials. Reasons for this are unclear. Larger studies in more diverse populations are needed to further evaluate the effects of SGLT2 inhibitors on MASH.

FINERENONE (KERENDIA®) APPROVED FOR HEART FAILURE WITH PRESERVED EJECTION FRACTION

illustration of human heart
In 2021, the SGLT2 inhibitor empagliflozin (Jardiance) became the first drug FDA-approved to treat heart failure with preserved ejection fraction (HFpEF). Several years later, another SGLT2 inhibitor, dapagliflozin (Farxiga), was approved. Now, Finerenone (Kerendia), a nonsteroidal mineralocorticoid receptor antagonist, has become the third drug and the first non-SGLT2 inhibitor to be approved. Approval was based on results from the FINEARTS-HF Study, where 6016 patients with heart failure and an ejection fraction (EF) of 40% or greater (average EF 53%) were randomized to finerenone or placebo. Over a median follow-up of 32 months, the incidence of the primary composite outcome (total worsening heart failure events and death from cardiovascular causes) was 14.9 events per 100 patient-years in the finerenone group and 17.7 events per 100 patient-years in the placebo group (P=0.007). There was no significant difference in overall mortality. Hyperkalemia was more common in the finerenone group (14.3% vs 6.9%) as was hypotension (18.5% vs 12.4%).

Finerenone blocks aldosterone receptors, similar to spironolactone, an inexpensive aldosterone antagonist that has been available for decades. Spironolactone, which is FDA-approved for heart failure with reduced ejection fraction (HFrEF), has also been studied in HFpEF. In the TOPCAT study, which enrolled 3445 patients with heart failure and an EF ≥ 45% (median EF 56%), spironolactone was not superior to placebo for a composite of CVD events; however, it did significantly reduce heart failure hospitalizations. The trial was plagued by discordant data in certain geographic regions (Russia, Georgia), and post-hoc analyses have found that when these regions were excluded, spironolactone significantly improved the primary outcome. The ACC 2023 HFpEF guidelines recommend spironolactone in some patients. Other drugs, including Entresto, Wegovy, and Zepbound, have demonstrated improvements in HFpEF outcomes in clinical trials but have not received FDA approval for the condition.

Finerenone is the third drug and only non-SGLT2 inhibitor approved for HFpEF. Providers should note that finerenone dosing recommendations for HFpEF, which are based on GFR and potassium levels, differ from those used in diabetic kidney disease. For patients who cannot afford finerenone, spironolactone likely offers similar benefits. Potassium levels should be monitored closely with either drug.
Corrected calcium levels in hypoalbuminemia are misleading and inaccurate
tube of blood
In plasma, approximately 50% of calcium circulates in the active ionized form, 10% is complexed with anions, and the remaining 40% is bound to protein, mainly albumin. If albumin levels are low, total calcium levels may not accurately reflect the amount of ionized calcium. In medical training, providers are often taught to correct calcium levels in the setting of hypoalbuminemia using formulas that incorporate albumin and total calcium levels. The most widely used formula is the simplified Payne formula: Corrected calcium (mg/dL) = measured total Ca (mg/dL) + 0.8 (4.0 - serum albumin [g/dL]). Despite this widely accepted practice, studies have not found these corrections to be accurate. To further evaluate the issue, a recent cross-sectional study published in the JAMA Network evaluated lab results from 22,658 patients who had their total calcium and ionized calcium levels measured simultaneously. The accuracy of 10 adjustment formulas for correcting total calcium levels was then measured. The results showed that unadjusted total calcium levels correlated as well and sometimes better with ionized calcium levels than the formula-adjusted values. For example, unadjusted total calcium showed a correlation (on a continuous numerical scale) with ionized calcium of 71.7% compared to 68.9% with the simplified Payne formula. When classifying patients into calcium status categories (hypocalcemia, normocalcemia, hypercalcemia), unadjusted total calcium agreed 74.5% of the time with ionized calcium compared to 63% with the simplified Payne formula. Furthermore, subgroup analysis in patients with concomitant hypoalbuminemia showed that formula-adjusted values were even less accurate than unadjusted levels in these subjects.

Corrected calcium levels are a cautionary tale on how easily some practices can become widely accepted in medicine despite a lack of rigorous scientific evaluation. Providers concerned about the accuracy of total calcium levels in the setting of hypoalbuminemia should check ionized levels directly and avoid using correction formulas.

NEWS IN BRIEF

Twice-yearly injection approved for HIV pre-exposure prophylaxis (PrEP)

red hiv awareness ribbon
The FDA recently approved lenacapavir (Yeztugo), a twice-yearly subcutaneous injection, for the prevention of HIV. In a study enrolling 5338 African women, no new HIV infections were observed over 104 weeks in the lenacapavir group (N=2134), compared to 39 in the Descovy group (N=2136) and 16 in the Truvada group (N=1068). In another study among 3265 high-risk men and women, the incidence of HIV infection was 0.10%/year in the lenacapavir group and 0.93%/year in the Truvada group. The most common side effect reported was injection site reactions (e.g., nodule, pain, erythema), which occurred in 69% of patients. Upon initiation, it is recommended that patients take 2 days of oral lenacapavir to achieve therapeutic levels more quickly.

While oral and injectable forms of HIV PrEP are highly effective, studies have found that up to 70% of PrEP users discontinue therapy or exhibit suboptimal adherence within six months of initiation. Yeztugo's twice-yearly dosing schedule will likely improve compliance and lower infection rates compared to other approved therapies, which include daily oral pills Descovy and Truvada, and the every-two-month IM injection Apretude (cabotegravir).

Combination of finerenone and empagliflozin improves proteinuria in DKD more than either drug alone

illustration of the kidneys
Finerenone, a nonsteroidal mineralocorticoid receptor antagonist, has been shown to improve outcomes in diabetic kidney disease (DKD). Empagliflozin, an SGLT2 inhibitor, has also been proven to improve DKD outcomes. A recent study compared a combination of the two drugs to either one alone in diabetics with DKD.

In the CONFIDENCE trial, 818 diabetics with DKD and a median urinary albumin-to-creatinine ratio (UACR) of 579 were randomized to finerenone (10 or 20 mg/day), empagliflozin (10 mg/day), or a combination of finerenone and empagliflozin. After 180 days, the average UACR reduction in the combination group was 29% greater than with finerenone alone and 32% greater than with empagliflozin alone.

Longer studies evaluating hard clinical outcomes are needed to fully elucidate the effects of this combination regimen.

Dietary sodium restriction lowers blood pressure in small trial

salt shaker
Sodium reabsorption in the nephron promotes fluid retention, thereby raising blood pressure. Reduced dietary sodium reverses this effect. A recent crossover study (N=102) compared the effects of a diet with 1500 mg/day of sodium to one with 3700 mg/day in diabetics. Participants crossed over between diets every 5 weeks and were provided all of their food with instructions not to eat outside food. At the end of the 5-week period, systolic blood pressure (SBP) was lower by 4.6 mmHg on the 1500 mg diet compared to the 3700 mg one, while diastolic blood pressure (DBP) was 2.3 mmHg lower.

These results are consistent with a 2023 study (N=213), which found that one week of a low sodium diet (500 mg/day) lowered SBP and DBP by 8 and 3 mmHg, respectively, compared to a high sodium diet (> 5000 mg/day).

Dietary sodium restriction has a modest effect on BP. Average sodium consumption in the U.S. is between 3600 and 4800 mg per day, so achieving these reductions would require significant dietary adjustments for most people.

Third large trial compares bedtime vs morning antihypertensive dosing

blood pressure machine with pills
Cardiovascular disease (CVD) events are more common in the morning when blood pressure (BP) rises due to the morning cortisol surge. Morning BP medication dosing causes trough levels in the AM, leading some researchers to speculate that evening dosing (with peak levels in the morning) may be more protective. A 2019 study (N=19,084) caused a small stir when it found that bedtime dosing of BP medications lowered the risk of a composite of CVD events compared to morning dosing. However, a subsequent 2022 study (N=21,104) did not find a benefit with evening dosing. A third trial (N=3357) examining the issue was recently published, and like the 2022 study, it also found no benefit with evening dosing.

The effects of bedtime versus morning dosing of antihypertensives on CVD events were mixed in three large trials, with one showing a benefit and the other two finding none. Patients should be advised to take their medications at a time that optimizes their compliance.

NEW DRUGS

POPULAR BUT UNPROVEN

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  • Pneumonia vaccines in adults - vaccine manufacturers, the CDC, and Medicare want everyone to get a pneumonia vaccine, so they must be highly effective, right?

Semaglutide (Wegovy) improves MASH in ongoing study
illustration of a fatty liver
Currently, resmetirom (Rezdiffra®), a thyroid hormone receptor beta partial agonist, is the only FDA-approved medication for the treatment of metabolic dysfunction-associated steatohepatitis (MASH), formally known as nonalcoholic steatohepatitis or fatty liver disease. MASH is a progressive liver condition with an estimated global prevalence of 4 to 6%. Its strong association with obesity has prompted researchers to evaluate the effects of weight-loss GLP therapies, specifically semaglutide and tirzepatide, on MASH pathology. A 72-week interim analysis from a placebo-controlled semaglutide study (N=800) in MASH patients with stage 2 or 3 fibrosis was recently published. The analysis found that semaglutide (2.4 mg) caused resolution of steatohepatitis without worsening of fibrosis in 62.9% of patients, compared to 34.3% in the placebo group (p<0.001). A reduction in liver fibrosis without worsening of steatohepatitis occurred in 36.8% and 22.4%, respectively (p<0.001). Semaglutide-treated patients lost 10.5% of their body weight compared to 2.0% with placebo (p<0.001). As expected, gastrointestinal adverse events were more frequent in the semaglutide group.

These results are consistent with a previous 52-week study (N=190) involving tirzepatide, where MASH resolution without worsening of fibrosis was observed in 62% of tirzepatide-treated patients (15 mg) and 10% of placebo-treated patients (p<0.001). Weight loss in this study was 15.6% and 0.8%, respectively.

While results from different studies are not comparable linearly, nothing in resmetirom's pivotal trial suggests that it is superior to semaglutide or tirzepatide. Furthermore, it does not cause weight loss, giving it no benefit in other obesity-related conditions. Resmetirom also has drug interactions and requires lab monitoring, while GLP-1 therapies generally do not. The effects of these drugs on long-term clinical outcomes like cirrhosis and liver failure are being evaluated in ongoing studies. MASH indications for semaglutide and tirzepatide are likely forthcoming.


Zepbound beats Wegovy in battle of weight-loss drug titans
woman injection weight-loss drug
Three GLP-1 drugs, Zepbound (tirzepatide), Wegovy (semaglutide), and Saxenda (liraglutide), are currently approved for weight loss. Zepbound and Wegovy have demonstrated superior weight loss (16% to 22%) compared to Saxenda (8%), making them two of the most discussed medications in decades. Now, they have been compared head-to-head in an open-label trial, where 751 overweight, nondiabetic adults were randomized to Zepbound (target dose 10 mg or 15 mg/week) or Wegovy (target dose of 1.7 mg or 2.4 mg/week). The primary outcome, percent change in weight from baseline to week 72, was -20.2% with Zepbound and -13.7% with Wegovy (p<0.001). Key secondary outcomes, including average weight loss (50 lbs vs 33 lbs) and the proportion of participants achieving a weight reduction of 20% or more (48% vs 27%), also favored Zepbound. Side effects, including nausea (44% vs 44%), constipation (28% vs 29%), diarrhea (24% vs 23%), and vomiting (15% vs 21%), were similar between groups and mainly occurred during the therapy titration phase. Drug discontinuation due to adverse events was slightly higher in the Wegovy group (6.1% vs 8%).

These results corroborate findings from placebo-controlled studies, which showed that both drugs are highly effective, but Zepbound is superior. Patients sometimes ask me if one of the two has fewer side effects, and I can now confidently say they are similar in that regard. For those who are unaware, current cash pricing for both drugs is detailed below.

Zepbound Cash pay: Eli Lilly offers Zepbound in two forms: pens and vials. The pens are pressed against the skin, and the medication is injected when a button is pushed. The vials require the patient to draw the medication into a syringe and inject it themselves. Pens cost $650/month with the Zepbound savings card (see Zepbound coverage and cost). The vials are available in 4 doses from LillyDirect at the following prices:
  • 2.5 mg: $349 per month
  • 5 mg: $499 per month
  • 7.5 mg: $499 per month
  • 10 mg: $499 per month

Wegovy cash pay: Novo Nordisk now offers all doses of Wegovy for $499/month through their online mail-order pharmacy NovoCare Pharmacy. Wegovy is available from other pharmacies for $650/month with the Wegovy savings card.

CLINICAL CHALLENGE

A 45-year-old female comes to see you for her annual physical. She reports having gastric bypass surgery three years ago and says she followed up with her surgeon once and never went back. She asks you to order her routine lab work.

Given her history of gastric bypass, what lab work is recommended? Are any other studies indicated? Find out at the link below.