Evaluation of platelet dense granules by transmission electron microscopy in healthy pediatric donors and pediatric patients with suspected platelet disorders
Paediatrics
Evaluation of platelet dense granules by transmission electron microscopy in healthy pediatric donors and pediatric patients with suspected platelet disorders
Paediatrics

Evaluation of platelet dense granules by transmission electron microscopy in healthy pediatric donors and pediatric patients with suspected platelet disorders

Platelets. 2025 Dec;36(1):2590752. doi: 10.1080/09537104.2025.2590752. Epub 2025 Nov 28.

ABSTRACT

BACKGROUND: Whole mount (WM) platelet transmission electron microscopy (PTEM) is a standard method for evaluating platelet dense granules (DG). However, because of the lack of a pediatric/adolescent mean DG/platelet reference range (RR), the prevalence of platelet DG deficiency in patients with suspected inherited platelet disorders (IPD) is mostly unknown in our practice. This study aimed to establish a local pediatric/adolescent RR for mean DG/platelet in a cohort of pediatric patients with clinical suspicion of IPD, which was used to determine the prevalence and clinical and laboratory features of platelet DG deficiency.

METHODS: WM-PTEM was performed on healthy donors. The mean DG/platelet RR was calculated by averaging the DG of 100 platelets per donor. Patients who underwent laboratory evaluation of suspected IPD were evaluated. PTEM results, clinical histories, other laboratory testing results, and pediatric ISTH BAT scores (normal < 3; abnormal ≥3) were collected and analyzed.

RESULTS: Healthy donors (n = 77, 41.6% female), ages 3-18 years, had a mean of 2.7 DG/platelet (±0.5), ranging from 1.9 to 3.8 per platelet. The mean DG/platelet did not correlate with age or gender. The tentative RR was calculated to be 1.9 to 3.8 DG/platelet. Of the 72 patients with suspected IPD (age 3-18 years, 69.4% female), 31 patients had BAT scores < 3 and 41 patients had BAT scores ≥3 (range 0-11). Eighteen patients (25%) were diagnosed with DG deficiency. The mean DG/platelet in patients with bleeding scores ≥3 vs. those with bleeding scores < 3 was similar. There was no difference in the number of patients with normal or abnormal bleeding scores in groups with normal vs decreased mean DG/platelet (p = .42) based on the pediatric DG/platelet RR. Platelet DG deficiency was also not correlated with abnormal platelet function testing results.

CONCLUSIONS: Approximately 25% of pediatric patients with suspected IPD were found to have platelet DG deficiency. However, the mean DG/platelet did not correlate with the ISTH BAT scores or platelet function testing results.

PMID:41312564 | DOI:10.1080/09537104.2025.2590752