Exercise linked to decreased mortality, heart events in those with new type 2 diabetes but no previous heart disease

New research to be presented at this year’s Annual Meeting of the European Association for the Study of Diabetes (EASD) in Vienna, Austria (15-19 September) shows that among people recently diagnosed with type 2 diabetes and no previous cardiovascular disease, a clear association exists between a person’s self-reported physical activity and their risk of all-cause mortality and major adverse cardiac events (MACE), which includes heart attacks and strokes.

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Genetic testing reduces risks from chemotherapy for gastrointestinal cancer patients

For some patients with gastrointestinal (GI) cancers like colorectal and pancreatic cancer, chemotherapy can cause severe, sometimes life-threatening side effects in those who carry certain genetic variants that can impact how their bodies process the drugs used to treat their disease.

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Genetic testing reduces risks from chemotherapy for gastrointestinal cancer patients

For some patients with gastrointestinal (GI) cancers like colorectal and pancreatic cancer, chemotherapy can cause severe, sometimes life-threatening side effects in those who carry certain genetic variants that can impact how their bodies process the drugs used to treat their disease.

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Flea-borne typhus infections are on the rise in Southern California: How to protect yourself and your pets

Pet owners, beware: Flea-borne typhus is on the rise in parts of Southern California.

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Flea-borne typhus infections are on the rise in Southern California: How to protect yourself and your pets

Pet owners, beware: Flea-borne typhus is on the rise in parts of Southern California.

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RFK Jr. is wrong about mRNA vaccines: A scientist explains how they make COVID less deadly

US health secretary Robert F. Kennedy Jr. has announced he is canceling US $500 million (£374 million) of research into mRNA vaccines, citing unproven concerns about their safety and long-term effects.

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National study urges expanded vaccine screening in emergency departments

About 49% of people are unaware of one or more vaccines recommended for them. Further, 86% have not received one or more of these vaccines.

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FDA Approves Inclisiran as First-Line LDL-C Treatment Without Statins

The FDA has approved inclisiran (Leqvio) for first-line use in lowering LDL cholesterol, even without combining it with statins, according to Novartis.

The FDA proactively requested the label update based on the robust LDL-C lowering data for PCSK9-targeting therapies.

“This first-line label update reinforces Leqvio’s proven ability to effectively lower LDL-C, a critical risk factor for heart disease,” said Victor Bultó, President, US, Novartis. “With this new indication enabling Leqvio’s use as monotherapy along with diet and exercise, we now have the potential to help even more patients achieve their LDL-C lowering goals earlier in their treatment journey.”

With its twice-yearly, health care provider-administered dosing, Leqvio is uniquely positioned to help support patient adherence and long-term LDL-C management, including goal attainment. This is a critical unmet need, as up to 80% of ASCVD patients in the US struggle to reach the LDL-C guideline-recommended target of <70 mg/dL. This need is heightened by the latest 2025 ACC/AHA Joint Committee Clinical Practice Guideline for the Management of Patients with Acute Coronary Syndromes, which recommends more aggressive treatment to achieve LDL-C targets.

The updated label removes the requirement for Leqvio to be used on top of or in combination with statin therapy. Other updates include revising “primary hyperlipidemia” to the more specific term of “hypercholesterolemia” throughout the label, to more accurately focus on LDL-C reduction.

After an initial dose and another at three months.

About Leqvio

Leqvio is an injectable prescription medicine indicated as an adjunct to diet and exercise to reduce low-density lipoprotein cholesterol (LDL-C) in adults with hypercholesterolemia, including heterozygous familial hypercholesterolemia (HeFH).

Novartis has obtained global rights to develop, manufacture and commercialize Leqvio under a license and collaboration agreement with Alnylam Pharmaceuticals, a leader in RNAi therapeutics.

About Atherosclerotic Cardiovascular Disease (ASCVD)

Cardiovascular disease (CVD) affects hundreds of millions of people and claims more lives globally than cancer, chronic lung disease and diabetes combined. Around 80% of premature cardiovascular deaths can be prevented by addressing factors that cause or worsen CVD.

ASCVD accounts for 85% of all CV deaths. Its burden in the US is greater than that of any other chronic diseases. ASCVD is caused by the development and growth of plaques in the inner lining of the arteries. The atherosclerotic plaque is mainly composed of low-density lipoprotein cholesterol (LDL-C) that accumulates over time. Cumulative exposure to LDL-C can increase one’s risk of cardiovascular events such as a heart attack or stroke.

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How does metformin lower blood sugar?

Although metformin has been the go-to medication to manage type 2 diabetes for more than 60 years, researchers still do not have a complete picture of how it works. Scientists at Baylor College of Medicine and international collaborators have discovered a previously unrecognized new player mediating clinically relevant effects of metformin: the brain. By uncovering a brain pathway involved in metformin’s anti-diabetic action, researchers have discovered new possibilities for treating diabetes more effectively and precisely. The study appeared in Science Advances.

“It’s been widely accepted that metformin lowers blood glucose primarily by reducing glucose output in the liver. Other studies have found that it acts through the gut,” said corresponding author Dr. Makoto Fukuda, associate professor of pediatrics – nutrition at Baylor. “We looked into the brain as it is widely recognized as a key regulator of whole-body glucose metabolism. We investigated whether and how the brain contributes to the anti-diabetic effects of metformin.”

The team focused on a small protein called Rap1, found in a specific part of the brain known as the ventromedial hypothalamus (VMH). The researchers discovered that metformin’s ability to lower blood sugar at clinically relevant doses depends on turning off Rap1 in this brain region.

To test this, the Fukuda lab and his colleagues used genetically modified mice that lacked Rap1 in their VMH. These mice were fed a high-fat diet to mimic type 2 diabetes. When given low doses of metformin, the drug failed to lower their blood sugar. However, other diabetes medications like insulin and GLP-1 agonists still worked.

To further show that the brain is a key player, the researchers injected tiny amounts of metformin directly into the brains of diabetic mice. The result was a significant drop in blood sugar, even with doses thousands of times smaller than what’s typically given by mouth.

“We also investigated which cells in the VMH were involved in mediating metformin’s effects,” Fukuda said. “We found that SF1 neurons are activated when metformin is introduced into the brain, suggesting they’re directly involved in the drug’s action.”

Using brain slices, the scientists recorded the electrical activity of these neurons. Metformin made most of them more active, but only if Rap1 was present. In mice lacking Rap1 in these neurons, metformin had no effect, showing that Rap1 is essential for metformin to “switch on” these brain cells and lower blood sugar.

“This discovery changes how we think about metformin,” Fukuda said. “It’s not just working in the liver or the gut, it’s also acting in the brain. We found that while the liver and intestines need high concentrations of the drug to respond, the brain reacts to much lower levels.”

Although few anti-diabetic drugs act on the brain, this study shows that widely used metformin has been doing so all along. “These findings open the door to developing new diabetes treatments that directly target this pathway in the brain,” Fukuda said. “In addition, metformin is known for other health benefits, such as slowing brain aging. We plan to investigate whether this same brain Rap1 signaling is responsible for other well-documented effects of the drug on the brain.”

Reference:

Hsiao-Yun Lin et al. ,Low-dose metformin requires brain Rap1 for its antidiabetic action.Sci. Adv.11,eadu3700(2025).DOI:10.1126/sciadv.adu3700

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Prepregnancy cardiovascular risk factor clusters increased the risk of stillbirth: JAHA

A new study published in the Journal of American Heart Association revealed that clusters of cardiovascular risk factors during pregnancy markedly increased the probability of stillbirth.

It is often acknowledged that stillbirth, which is the intrauterine death of a fetus that usually happens between 20 and 28 weeks of gestation, is a crucial sign of the calibre and efficacy of health care systems throughout pregnancy and childbirth. It has been determined that one modifiable and controllable risk factor for stillbirth is the cardiovascular health of the mother before to pregnancy.

It is still unclear how certain clusters of prenatal cardiovascular risk factors relate to stillbirth, especially when it comes to different racial and ethnic groupings. With a focus on racial inequities, this study sought to assess the relationship between stillbirth and 16 different cardiovascular risk groups.

Using the Centers for Disease Control and Prevention Natality and Fetal Death Data Files (2014–2022), researchers carried out a population-based analysis across the country that included 131,047 stillbirths (defined as births that occurred at least 20 weeks gestation) and 31,408,776 singleton births. 16 mutually incompatible clusters were created using the prepregnancy cardiovascular risk factors (smoking, hypertension, diabetes, and nonideal body mass index). 

Pregnancy diabetes posed the highest risk, followed by prepregnancy hypertension (95% CI, 2.27–2.63), smoking (95% CI, 1.58–1.67), and unhealthy body mass index (95% CI, 1.31–1.35). These findings were obtained from the analysis of 16 groups defined by the four binary risk factors. 2 out of 6 risk combinations, mostly those involving diabetes, showed the absolute extra risk related to the biological interaction between 2 risk variables.

There were clear racial differences, with non-Hispanic Black women having the highest absolute and relative odds of stillbirth-nearly twice as high as non-Hispanic White mothers.

Overall, this study demonstrated a substantial correlation between the risk of stillbirth, specific risk clusters, and prepregnancy cardiovascular risk factor scores. This research created 16 different risk clusters by combining four binary risk variables, and they discovered that the relationships between these clusters with stillbirth varied, with some single risk factors (where no other factors were present) exhibiting larger connections.

Source:

Nie, J., Rezende, L. F. M., Ferrari, G., Qiu, Y., Wang, X., Huang, W., Niu, Z., Chen, X., & Aune, D. (2025). Association of prepregnancy cardiovascular risk factors clusters with stillbirth risk across racial and ethnic groups: A nationwide population-based study of 31.4 million singleton births and 131 047 stillbirths. Journal of the American Heart Association. https://doi.org/10.1161/JAHA.124.042319

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