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This week’s Medicine Key Highlights

This week’s Medicine Key Highlights

This week’s Medicine Key Highlights

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This week’s Medicine Key Highlights

Last updated: March 21, 2026 2:00 pm
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Key Highlights

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A new study has identified a specific molecular pathway, SEMA3C/PLXND1, that drives the excessive scar tissue formation in keloids by activating the TGF-β1 signaling pathway in skin cells. This discovery is significant because it reveals a potential new target for treatments that could stop the progression of these difficult-to-treat, painful scars.
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Researchers found that blocking the SEMA3C/PLXND1 interaction or inhibiting TGF-β1 in keloid cells significantly reduced their production of collagen, the main protein in scar tissue. This is important as it provides direct experimental evidence that targeting this pathway could be an effective strategy to slow down or prevent keloid growth.
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A large European study found that patients with a specific type of lung disease linked to certain autoimmune antibodies often have a scarring pattern on their lung scans known as usual interstitial pneumonia (UIP). This is crucial because the UIP pattern is associated with a faster decline in lung function, helping doctors identify patients who may need more aggressive treatment.
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The research showed that treatment with the immunosuppressant drug rituximab was linked to an improvement in lung function for these patients after one year. This finding is significant as it offers a promising treatment option that may help preserve breathing capacity in a disease that can otherwise lead to respiratory failure.
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A study in rats revealed that a deficiency in a small regulatory molecule called miR-23b-3p worsens a type of blood vessel inflammation (IgA vasculitis) by over-activating immune cells via the TLR4 pathway. This is important because it uncovers a precise molecular mechanism behind the disease and suggests that restoring levels of miR-23b-3p could be a new therapeutic approach.
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When researchers increased miR-23b-3p levels in the animal model, it reduced the overactive immune response and improved disease symptoms, including lowering harmful antibody levels. This demonstrates the potential of targeting this specific molecular pathway to calm the misdirected immune attack that characterizes this form of vasculitis.
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A large study of over 2,200 patients with cardiac amyloidosis found that nearly 40% did not have preserved heart function, challenging the common assumption that this disease only causes a certain type of heart failure. This is critical for diagnosis, as it means doctors should consider this condition even in patients whose hearts appear to pump normally or only mildly reduced.
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The research showed that combining measurements of heart pumping strength, subtle muscle strain, and blood flow created a decision tree that identified four distinct patient groups with very different survival risks. This matters because it provides doctors with a more precise, multi-faceted tool for predicting outcomes and personalizing care for this complex heart condition.
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A clinical trial confirmed that a modified dose of the COVID-19 antiviral nirmatrelvir/ritonavir is safe and maintains effective drug levels in patients with severe kidney impairment, including those on dialysis. This is a vital finding because this high-risk population has been largely excluded from previous studies, and it provides clear dosing guidance to protect them from severe COVID-19.
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The study demonstrated that the adjusted drug regimen achieved similar antiviral exposure in kidney patients as the standard dose does in people with normal kidney function, and it also substantially reduced levels of the SARS-CoV-2 virus. This offers reassurance to clinicians that they can use this life-saving treatment effectively and safely in one of the most vulnerable patient groups.
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