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The New England Journal Of Medicine[JOURNAL]

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Phase 3 Trial of Oral Infigratinib in Children with Achondroplasia.

Savarirayan R, Hoover-Fong J, Irving M … +31 more , Arundel P, de Bergua JM, Campeau PM, Candler T, Cocanougher BT, Cormier-Daire V, Edouard T, Fredwall SO, Harmatz P, Hoernschemeyer D, Irgens HU, Jamuar S, Kannu P, Legare JM, Leiva-Gea A, McDevitt H, Onesimo R, Phillips J, Del Pino M, Robinson ME, Rossi M, Skae M, Ward LM, White KK, Schmidt J, Lystig T, Salvatici A, Bai Y, Butler PW, van Veenhuyzen D, Rogoff D

N Engl J Med · 2026 Jun · PMID 42370681 · Publisher ↗

BACKGROUND: Achondroplasia is a genetic skeletal condition caused by pathogenic variants. Infigratinib, an oral FGFR1-3 tyrosine kinase inhibitor, down-regulates key pathways in the pathogenesis of achondroplasia. METHO... BACKGROUND: Achondroplasia is a genetic skeletal condition caused by pathogenic variants. Infigratinib, an oral FGFR1-3 tyrosine kinase inhibitor, down-regulates key pathways in the pathogenesis of achondroplasia. METHODS: In this phase 3, multicenter, double-blind, placebo-controlled trial, we randomly assigned children with achondroplasia (3 to 17 years of age) in a 2:1 ratio to receive infigratinib (at a dose of 0.25 mg per kilogram of body weight) or placebo once daily for 52 weeks. The primary end point was the change from baseline in the annualized height velocity in the infigratinib group as compared with the placebo group at week 52. Key secondary end points were the change from baseline in the height z score and in the upper-to-lower body segment ratio at week 52. The primary analysis evaluated the treatment effect at week 52 in the full analysis population, with missing data handled with a prespecified imputation approach. RESULTS: In all, 114 patients underwent randomization: 75 patients to receive infigratinib (with 1 withdrawal before treatment) and 39 patients to receive placebo. The difference between infigratinib and placebo in the least-squares mean change from baseline to week 52 was 1.74 cm per year (95% confidence interval [CI], 1.31 to 2.17; P<0.001) for the annualized height velocity, 0.32 (96% CI, 0.23 to 0.41; P<0.001) for the height z score, and -0.02 (96% CI, -0.06 to 0.01) for the upper-to-lower body segment ratio. Adverse events occurred in 71 of 74 patients (96%) in the infigratinib group and in 37 of 39 patients (95%) in the placebo group; serious adverse events occurred in 4 of 74 patients (5%) and 1 of 39 patients (3%), respectively. No serious adverse events or adverse events leading to treatment discontinuation were considered by the investigator to be related to infigratinib or placebo. CONCLUSIONS: In children with achondroplasia, treatment with once-daily oral infigratinib for 52 weeks resulted in a significantly greater increase from baseline in the annualized height velocity than placebo. (Funded by BridgeBio Pharma; PROPEL 3 ClinicalTrials.gov number, NCT06164951; EudraCT number, 2023-506130-67.).

Cat Scratch Disease.

Wadhwa RD, Loving VA

N Engl J Med · 2026 Jul · PMID 42370680 · Publisher ↗

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Declarations of Independence - Physicians and the U.S. Body Politic, 1776-2026.

Podolsky SH, Jones DS, Barr J

N Engl J Med · 2026 Jul · PMID 42370669 · Publisher ↗

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Clinical Characteristics of Patients Infected with Bundibugyo Virus, DRC 2026.

Akilimali P, Ebengo DM, Scarpino SV … +12 more , Amuri-Aziza A, Wawina-Bokalanga T, Matondo-Mbundu P, Kanku B, Kinganda-Lusamaki E, Makangara JC, Mukadi-Bamuleka D, Rojek A, Kraemer MUG, Ngandu C, Mwamba D, Mbala-Kingebeni P

N Engl J Med · 2026 Jun · PMID 42341323 · Publisher ↗

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Long-Acting Treatment and Advanced HIV Disease - Addressing a Public Health Priority.

Falconer J, Bekker LG, Jarvis JN

N Engl J Med · 2026 Jun · PMID 42341320 · Publisher ↗

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Immediate or Deferred Nonculprit-Lesion PCI in Myocardial Infarction.

N Engl J Med · 2026 Jun · PMID 42341317 · Publisher ↗

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The Physiology of Pulsus Paradoxus Revisited. Reply.

Yu R, Cook G, Atwood JE

N Engl J Med · 2026 Jun · PMID 42341316 · Publisher ↗

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The Physiology of Pulsus Paradoxus Revisited.

Govig B

N Engl J Med · 2026 Jun · PMID 42341315 · Publisher ↗

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Clinical Implications of Minipuberty. Reply.

Juul A

N Engl J Med · 2026 Jun · PMID 42341314 · Publisher ↗

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Clinical Implications of Minipuberty.

Movsas T

N Engl J Med · 2026 Jun · PMID 42341313 · Publisher ↗

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Stopping Beta-Blockers after Myocardial Infarction. Reply.

Choi KH, Kang D, Hahn JY

N Engl J Med · 2026 Jun · PMID 42341312 · Publisher ↗

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Stopping Beta-Blockers after Myocardial Infarction.

Wu W, Xu G, Gao X

N Engl J Med · 2026 Jun · PMID 42341311 · Publisher ↗

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Stopping Beta-Blockers after Myocardial Infarction.

Messerli FH, Maqsood MH, Bangalore S

N Engl J Med · 2026 Jun · PMID 42341310 · Publisher ↗

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Stopping Beta-Blockers after Myocardial Infarction.

Pivato CA, Pensato U, Stefanini GG

N Engl J Med · 2026 Jun · PMID 42341309 · Publisher ↗

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Stopping Beta-Blockers after Myocardial Infarction.

Vignati C, Galotta A, Pezzuto B

N Engl J Med · 2026 Jun · PMID 42341308 · Publisher ↗

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Response to Crizotinib in Infantile Fibrosarcoma with Gene Fusion.

Sri Haran S, Cain L, Darmanian A … +10 more , Krivanek M, Wright D, Nicholls W, Lowe M, Dalla-Pozza L, Goodwin B, McEniery J, Hardin K, Sullivan A, Omer N

N Engl J Med · 2026 Jun · PMID 42341307 · Publisher ↗

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Catheter Ablation for Persistent Atrial Fibrillation.

Sapp JL

N Engl J Med · 2026 Jun · PMID 42341306 · Publisher ↗

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Case 18-2026: A 53-Year-Old Man with Leg Weakness, Pain, and Weight Loss.

Geha R, Omid-Fard N, Slama MCC … +1 more , Reda HM

N Engl J Med · 2026 Jun · PMID 42341305 · Publisher ↗

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Kwashiorkor.

Kolathil JA, Varma GM

N Engl J Med · 2026 Jun · PMID 42341304 · Publisher ↗

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Prevention and Treatment of Peanut Allergy.

Du Toit G, Lack G

N Engl J Med · 2026 Jun · PMID 42341303 · Publisher ↗

Early introduction of peanut protein reduces allergy prevalence by approximately 80%, with efficacy diminishing as introduction is delayed. Appropriate prevention involves ingestion of approximately 2 g of peanut protein... Early introduction of peanut protein reduces allergy prevalence by approximately 80%, with efficacy diminishing as introduction is delayed. Appropriate prevention involves ingestion of approximately 2 g of peanut protein weekly for infants at low risk and 4 to 6 g weekly for infants at high risk. Population-level implementation that targets all infants achieves greater reduction in disease burden than approaches that target only high-risk groups, although disparities exist among some ethnic groups and groups with restricted access to care. Peanut immunotherapy initiated in younger children (1 to 3 years of age) shows superior efficacy and higher rates of clinical remission as compared with immunotherapy initiated in older children. The natural history of untreated peanut allergy follows a trajectory of increasing peanut-specific IgE levels and clinical reactivity over time, underscoring the importance of early intervention during this narrow developmental window.
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