
Five papers: June 22, 2026
Five papers from the June 22, 2026 window — the Nature Medicine drought ends with a large-biobank prospective study (N = 154,169 + 10,262 validation) linking generational increases in biological aging to early-onset cancer risk (HR 1.08 per SD PhenoAge; immune aging → lung HR 1.89), and a News & Views contextualizing Korean nationwide evidence that e-cigarettes after cessation may blunt lung cancer risk reduction. Nature Communications contributes three papers: higher IVF trigger-day hCG dose linked to reduced offspring DNA methylation and suboptimal neurodevelopment in 1,333 singletons, with EHMT1 rescue in mice; AREL1 identified as a cholesterol-regulated MASH fibrosis driver in a specific HSC subpopulation, targeted therapeutically by vitamin A-LNPs; and AOC1/spermidine/EIF5A hypusination as the placental pathway controlling labor timing, with spermidine preventing preterm birth in mice.
研究速览
1. Accelerated biological aging is rising across generations and prospectively predicts early-onset cancer risk


2. E-cigarette use after smoking cessation may blunt the lung cancer benefit of quitting
3. Higher trigger-day hCG dose in IVF links to reduced DNA methylation and suboptimal neurodevelopment in offspring
4. AREL1 drives MASH liver fibrosis via the ILK–PI3K–AKT axis; vitamin A–LNP knockdown is therapeutic in mice
5. Placental AOC1 and spermidine control labor timing; spermidine supplementation prevents preterm birth in mice
Notable mention
参考来源
- 1Biological aging and generational shifts in early-onset cancer risk
- 2Long-term health risks of e-cigarettes after smoking cessation
- 3Trigger-day hCG effects on DNA methylation and neurodevelopment in ART offspring
- 4PubMed PMID 42323302
- 5Therapeutic targeting of AREL1 in hepatic stellate cells attenuates MASH-related liver fibrosis
- 6PubMed PMID 42324266
- 7AOC1 regulates labor initiation through spermidine-induced autophagy of placental trophoblast cells via EIF5A hypusination
- 8IL-2 mutein promotes antigen-specific transplant acceptance in mice through expansion of ST2+ regulatory T cells




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