Finnish researchers at Aalto University showcasing a laser device for treating dry macular degeneration in a lab setting.
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Aalto University team reports laser approach that may slow dry macular degeneration

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Researchers in Finland say a temperature‑controlled, near‑infrared laser can trigger the eye’s repair responses and could slow early dry age‑related macular degeneration; animal data support human safety trials planned for spring 2026.

Age‑related macular degeneration (AMD) is a leading cause of vision loss in older adults. In the United States, an estimated 20 million people aged 40 and older live with AMD, and the disease becomes much more common with age. Public‑health data show rising prevalence in the 80s, while Aalto University’s release notes that roughly one‑third of people over 80 are affected. Most cases are the dry form. For late dry AMD (geographic atrophy), FDA‑approved drugs now slow progression, but there is still no therapy that reverses or halts early dry AMD. (pmc.ncbi.nlm.nih.gov)

Aalto University scientists report a non‑damaging laser method that gently warms retinal tissue by a few degrees while continuously monitoring temperature. The aim is to activate the eye’s own cleanup and repair pathways—heat‑shock proteins that help refold damaged proteins and autophagy, the cell’s waste‑disposal process—without injuring delicate structures. “We were able to show that we can activate not only the production of the heat shock proteins, but also autophagy using the heat shocks,” said Professor Ari Koskelainen. The team stresses that temperatures above about 45°C can harm tissue, so precise, real‑time control is central to the approach. (sciencedaily.com)

Peer‑reviewed animal data underpin the claim. In pigs, the group’s electroretinography‑guided, temperature‑controlled laser exposures to about 44°C for 60 seconds activated protective responses in the retinal pigment epithelium while avoiding oxidative stress, apoptosis and structural damage; visible lesions appeared above roughly 48°C. Earlier work from the team and collaborators established temperature‑monitoring techniques and heat‑response activation in mice. (pubmed.ncbi.nlm.nih.gov)

According to Aalto University, first‑in‑human trials in Finland are slated for spring 2026, beginning with safety assessments. The researchers expect the treatment would likely need to be repeated, because the cellular response can wane days after application. Aalto has also helped launch a spin‑off, Maculaser, to commercialize the technology; Koskelainen says an optimistic scenario could see hospital eye clinics adopt the method within about three years, with an eventual goal of availability at local ophthalmology practices. (eurekalert.org)

The pig study was published in Nature Communications on October 29, 2025. (pubmed.ncbi.nlm.nih.gov)

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Close-up photo of a retinal scan in a lab, highlighting eye vessels linked to heart risk and aging, with researcher analyzing data.
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Retinal scans may signal biological aging and cardiovascular risk

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Researchers at McMaster University and the Population Health Research Institute report that simple retinal scans, combined with genetic and blood data, may offer a non-invasive window into cardiovascular health and biological aging. An analysis of more than 74,000 people linked simpler eye-vessel patterns to higher heart-disease risk and faster aging. The study, published October 24, 2025, in Science Advances, points to potential early-detection tools that remain under investigation.

Scientists at the University of Southern California are starting a phase 2b clinical trial to test a microscopic stem cell implant aimed at restoring vision in patients with advanced dry age-related macular degeneration. The hair-thin patch seeks to replace damaged retinal cells, building on earlier research that showed safety and vision gains in some participants. Researchers hope it could offer a way to reverse vision loss where current treatments fall short.

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Scientists at the University of Missouri report that two natural molecules — agmatine and thiamine — are reduced in samples from glaucoma patients and could serve as early biomarkers. In preclinical work, the compounds also showed signs of protecting retinal cells, suggesting a path to earlier detection and potential neuroprotective therapies.

A Cold Spring Harbor Laboratory study demonstrated CAR T-cell therapy can reverse age-related intestinal decline in mice by targeting senescent cells. While promising, experts caution on safety risks, off-target effects, dosing, and costs for human use.

Imeripotiwa na AI Imethibitishwa ukweli

Stanford Medicine researchers report that blocking the enzyme 15-PGDH reversed age-related cartilage loss in older mice and reduced osteoarthritis-like damage after ACL-like knee injuries. In lab experiments, cartilage taken from knee replacement surgeries also showed early signs of regeneration after exposure to the inhibitor, findings published in *Science*.

A study published November 5 in Nature reports that a small subset of microglia marked by low PU.1 and expression of the receptor CD28 can dampen neuroinflammation and curb amyloid pathology in Alzheimer’s models, pointing to microglia-focused immunotherapy. The work draws on mouse experiments, human cells, and analyses of human brain tissue.

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An experimental gene therapy has demonstrated significant promise in slowing the progression of Huntington’s disease, a rare form of dementia, by about 75 percent in a late-stage trial. Researchers hailed the breakthrough as a major step forward, though challenges remain in delivery and regulatory approval. Efforts are underway to develop a more practical version of the treatment.

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