Leniolisib is an FDA-approved PI3Kδ inhibitor used to treat activated phosphoinositide 3-kinase delta syndrome (APDS) in patients aged ≥12 years who weigh ≥45 kg. Pediatric patients aged 4 to 11 years with APDS were enrolled in a two-part, prospective, open-label, single-arm, international study to evaluate the safety and efficacy of leniolisib (NCT05438407).
Here we report safety and efficacy outcomes following the completion of 12 weeks of leniolisib treatment (part 1). Twenty-six patients were screened; 21 patients enrolled across the United States, France, and Japan (Table 1). Leniolisib was administered orally twice daily (BID) as tablets in 10- and 30-mg strengths, with doses ranging from 20 to 70 mg BID based on weight. Co-primary outcomes were change from baseline (CFB) at 12 weeks in log10-transformed sum of product of diameters (SPD) of index lymph nodes and normalization of naïve B cells. Additional outcomes included changes in spleen volume and quantitative immunoglobulin (Ig) levels, including IgM.
Patient demographics and baseline characteristics.
| Patient Characteristic (N=21) | Value |
|---|---|
| Age at time of study, median (range), y | 7.0 (4-11) |
| Sex, male to female, n | 13:8 |
| Self-identified race, n (%) | |
| White | 9 (42.9) |
| Asian | 4 (19.0) |
| Other | 1 (4.8) |
| Not reported/unknown/missing | 7 (33.3) |
| Self-identified ethnicity, n (%) | |
| Hispanic | 3 (14.3) |
| Non-Hispanic | 12 (57.1) |
| Not reported | 6 (28.6) |
| Weight at baseline, median (range), kg | 23.9 (15.4-44.5) |
| Time since APDS diagnosis, median (range), mo | 32.9 (2.2-142.2) |
| APDS variant distribution, n (%) | |
| PIK3CD | 17 (81.0) |
| PIK3R1 | 4 (19.0) |
| Patient Characteristic (N=21) | Value |
|---|---|
| Age at time of study, median (range), y | 7.0 (4-11) |
| Sex, male to female, n | 13:8 |
| Self-identified race, n (%) | |
| White | 9 (42.9) |
| Asian | 4 (19.0) |
| Other | 1 (4.8) |
| Not reported/unknown/missing | 7 (33.3) |
| Self-identified ethnicity, n (%) | |
| Hispanic | 3 (14.3) |
| Non-Hispanic | 12 (57.1) |
| Not reported | 6 (28.6) |
| Weight at baseline, median (range), kg | 23.9 (15.4-44.5) |
| Time since APDS diagnosis, median (range), mo | 32.9 (2.2-142.2) |
| APDS variant distribution, n (%) | |
| PIK3CD | 17 (81.0) |
| PIK3R1 | 4 (19.0) |
APDS, activated phosphoinositide 3-kinase delta syndrome; PIK3CD, phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit delta; PIK3R1, phosphoinositide-3-kinase regulatory subunit 1.
Both primary end points improved from baseline after 12 weeks of treatment with leniolisib across all dose levels. Mean CFB of log10-transformed SPD reduced by -0.1956 (n = 19). Mean CFB of naïve B cells (CD19+CD27-CD10-) from total B cells was 33.3% (SD, 13.1; n = 11). Mean CFB of spleen log10 volume reduced was -0.1222 (n = 21). Mean Ig levels (n = 14) changed from baseline after 12 weeks of leniolisib treatment: IgM, 2.7 g/L to 1.6 g/L; IgG, 10.1 g/L to 11.1 g/L; and IgA, 0.88 g/L to 0.83 g/L. Leniolisib was well tolerated (Table 2). Twenty patients had treatment-emergent adverse events (AEs). All were grades 1 or 2; none were serious. Five patients had treatment-related AEs, including headache, palpitations, abdominal pain, diarrhea, nausea, pruritus, fatigue, decreased neutrophil count, and increased aspartate aminotransferase. No AEs led to discontinuation of study drug treatment.
Summary of Treatment-Emergent Adverse Events.
| Adverse Events Category | Total No. of Patients, n (%) |
|---|---|
| Any TEAE | 20 (95.2) |
| Grade 1 | 20 (95.2) |
| Grade 2 | 8 (38.1) |
| Grade 3 | 0 |
| Grade 4 | 0 |
| Grade 5 | 0 |
| Any study treatment-related TEAE | 5 (23.8) |
| Leading to discontinuation of study treatment | 0 |
| Leading to death | 0 |
| Any serious TEAE | 0 |
| Adverse Events Category | Total No. of Patients, n (%) |
|---|---|
| Any TEAE | 20 (95.2) |
| Grade 1 | 20 (95.2) |
| Grade 2 | 8 (38.1) |
| Grade 3 | 0 |
| Grade 4 | 0 |
| Grade 5 | 0 |
| Any study treatment-related TEAE | 5 (23.8) |
| Leading to discontinuation of study treatment | 0 |
| Leading to death | 0 |
| Any serious TEAE | 0 |
TEAE, treatment-emergent adverse event.
Overall, leniolisib was well tolerated, reduced lymphoproliferation, and improved normalization of naïve B cells, meeting the co-primary end points. All 21 patients completed part 1, and 20 transitioned to the 1-year treatment extension (one patient discontinued due to social reasons).
