ClinicalTrials.gov
History of Changes for Study: NCT05693129
Pediatric Patients Aged 1 to 6 Years With APDS
Latest version (submitted March 20, 2024) on ClinicalTrials.gov
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Study Record Versions
Version A B Submitted Date Changes
1 January 12, 2023 None (earliest Version on record)
2 April 20, 2023 Contacts/Locations and Study Status
3 June 8, 2023 Sponsor/Collaborators and Study Status
4 August 30, 2023 Contacts/Locations, Study Status and Sponsor/Collaborators
5 October 2, 2023 Recruitment Status, Contacts/Locations, Study Status and Oversight
6 November 1, 2023 Study Status and Contacts/Locations
7 November 28, 2023 Contacts/Locations and Study Status
8 December 14, 2023 Contacts/Locations and Study Status
9 December 20, 2023 Contacts/Locations and Study Status
10 January 31, 2024 Study Status and Contacts/Locations
11 March 20, 2024 Contacts/Locations and Study Status
Comparison Format:
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Changes (Side-by-Side) for Study: NCT05693129
December 20, 2023 (v9) -- January 31, 2024 (v10)

Changes in: Study Status and Contacts/Locations
Open or close this module Study Identification
Unique Protocol ID: LE 3302 LE 3302
Brief Title: Pediatric Patients Aged 1 to 6 Years With APDS Pediatric Patients Aged 1 to 6 Years With APDS
Official Title: An Open-label, Single Arm Study of the Safety, Pharmacokinetics, Pharmacodynamics, and Efficacy of Leniolisib in Pediatric Patients (Aged 1 to 6 Years) With APDS (Activated Phosphoinositide 3-Kinase Delta Syndrome) Followed by an Open-label Long-term Extension An Open-label, Single Arm Study of the Safety, Pharmacokinetics, Pharmacodynamics, and Efficacy of Leniolisib in Pediatric Patients (Aged 1 to 6 Years) With APDS (Activated Phosphoinositide 3-Kinase Delta Syndrome) Followed by an Open-label Long-term Extension
Secondary IDs:
Open or close this module Study Status
Record Verification: December 2023 January 2024
Overall Status: RecruitingRecruiting
Study Start: August 30, 2023 August 30, 2023
Primary Completion: September 30, 2025 [Anticipated] September 30, 2025 [Anticipated]
Study Completion: November 28, 2025 [Anticipated] November 28, 2025 [Anticipated]
First Submitted: October 17, 2022 October 17, 2022
First Submitted that
Met QC Criteria:		 January 12, 2023 January 12, 2023
First Posted: January 20, 2023 [Actual] January 20, 2023 [Actual]
Last Update Submitted that
Met QC Criteria:		 December 20, 2023 January 31, 2024
Last Update Posted: December 21, 2023 [Actual] February 1, 2024 [Actual]
Open or close this module Sponsor/Collaborators
Sponsor: Pharming Technologies B.V. Pharming Technologies B.V.
Responsible Party: Sponsor Sponsor
Collaborators: CMIC Co, Ltd. Japan
Labcorp Central Laboratory
Fortrea
Aixial Group 		CMIC Co, Ltd. Japan
Labcorp Central Laboratory
Fortrea
Aixial Group
Open or close this module Oversight
U.S. FDA-regulated Drug: YesYes
U.S. FDA-regulated Device: NoNo
Data Monitoring: Yes Yes
Open or close this module Study Description
Brief Summary: This is a 2-part, prospective, open-label, single arm, multicenter study to evaluate the safety, tolerability, pharmacokinetics (PK), pharmacodynamics (PDx), and efficacy of leniolisib in at least 15 pediatric patients (aged 1 to 6 years) with activated phosphoinositide 3-kinase delta (PI3Kδ) syndrome (APDS) This is a 2-part, prospective, open-label, single arm, multicenter study to evaluate the safety, tolerability, pharmacokinetics (PK), pharmacodynamics (PDx), and efficacy of leniolisib in at least 15 pediatric patients (aged 1 to 6 years) with activated phosphoinositide 3-kinase delta (PI3Kδ) syndrome (APDS)
Detailed Description:

Part I will consist of a 12-week period to assess the safety and efficacy of treatment with leniolisib. Part II will consist of a 1-year, long-term, safety follow-up extension with a possible interim analysis.

The leniolisib doses to be used in study were selected based on safety, tolerability, PK, and PDx data from the adult Phase 2/3 study, as well as PK modeling data. In both parts of the study, leniolisib will be administered orally based on weight.

Part I will consist of a 12-week period to assess the safety and efficacy of treatment with leniolisib. Part II will consist of a 1-year, long-term, safety follow-up extension with a possible interim analysis.

The leniolisib doses to be used in study were selected based on safety, tolerability, PK, and PDx data from the adult Phase 2/3 study, as well as PK modeling data. In both parts of the study, leniolisib will be administered orally based on weight.
Open or close this module Conditions
Conditions: APDS APDS
Keywords:
Open or close this module Study Design
Study Type: InterventionalInterventional
Primary Purpose: TreatmentTreatment
Study Phase: Phase 3Phase 3
Interventional Study Model: Single Group Assignment Single Group Assignment
Number of Arms: 11
Masking: None (Open Label)None (Open Label)
Allocation: N/AN/A
Enrollment: 15 [Anticipated] 15 [Anticipated]
Open or close this module Arms and Interventions
Arms Assigned Interventions
Experimental: Leniolisib
Leniolisib film-coated granules in 10, 15 and 20 mg strengths administered orally BID by body weight for 12 weeks for Part I and for 1 year for Part II.
 Drug: Leniolisib
The doses selected will range from 10 to 50 mg twice daily (BID) (resulting in total daily doses ranging from 20 to 100 mg per day).
Open or close this module Outcome Measures
Primary Outcome Measures:
1. Part I & II: Number of Participants with Treatment-emergent adverse events (TEAEs), Serious Adverse Events (SAEs) , and Adverse Events (AEs)
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year, plus 30 days ]

To assess number of Participants with TEAEs, SAEs, and AEs leading to discontinuation of study drug 		Part I & II: Number of Participants with Treatment-emergent adverse events (TEAEs), Serious Adverse Events (SAEs) , and Adverse Events (AEs)
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year, plus 30 days ]

To assess number of Participants with TEAEs, SAEs, and AEs leading to discontinuation of study drug
2. Part I & II: Change from baseline in clinical laboratory test results
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in clinical laboratory test results (hematology, blood 		Part I & II: Change from baseline in clinical laboratory test results
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in clinical laboratory test results (hematology, blood
3. Part I & II: Change from baseline in vital signs
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in vital signs 		Part I & II: Change from baseline in vital signs
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in vital signs
4. Part I & II: Change from baseline in physical examination findings
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in physical examination findings 		Part I & II: Change from baseline in physical examination findings
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in physical examination findings
5. Part I & II: Change from baseline in electrocardiograms (ECGs)
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year, plus 30 days ]

Number of Participants with change in electrocardiograms (ECGs) 		Part I & II: Change from baseline in electrocardiograms (ECGs)
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year, plus 30 days ]

Number of Participants with change in electrocardiograms (ECGs)
6. Part I & II: Change from baseline in growth and physical development
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in growth and physical development 		Part I & II: Change from baseline in growth and physical development
[ Time Frame: From baseline to end of 12 weeks, & From baseline to through study completion, an average of 1 year ]

Number of Participants with change in growth and physical development
7. Part I & II: Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Part I: Baseline and Day 85 Part II: at Day 252, through study completion, an average of 1 year ]

To assess the impact of leniolisib on lymphadenopathy, patients will be scanned in an MRI or a CT scanner as based on clinical practice and local regulation. Index lesions will be selected from measurable nodal and extra nodal lesions as per the Cheson methodology. The same imaging modality will be used throughout the study for the same patient. Patients will be assessed by MRI, or in sites where local practice and local authorities/IECs/IRBs approve CT scans for research purposes using a low-dose CT scan. 		Part I & II: Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Part I: Baseline and Day 85 Part II: at Day 252, through study completion, an average of 1 year ]

To assess the impact of leniolisib on lymphadenopathy, patients will be scanned in an MRI or a CT scanner as based on clinical practice and local regulation. Index lesions will be selected from measurable nodal and extra nodal lesions as per the Cheson methodology. The same imaging modality will be used throughout the study for the same patient. Patients will be assessed by MRI, or in sites where local practice and local authorities/IECs/IRBs approve CT scans for research purposes using a low-dose CT scan.
8. Part I: A Percentage of Inhibition of Unstimulated and Stimulated pAkt Levels in B Cells
[ Time Frame: Part I: Baseline, Days 29, 57 and 85 ]

To assess change in the PDx effect of leniolisib will be assessed using ex vivo stimulated and unstimulated 		Part I: A Percentage of Inhibition of Unstimulated and Stimulated pAkt Levels in B Cells
[ Time Frame: Part I: Baseline, Days 29, 57 and 85 ]

To assess change in the PDx effect of leniolisib will be assessed using ex vivo stimulated and unstimulated
Secondary Outcome Measures:
1. Part I: To evaluate changes in mTOR pathway through changes in pAkt
[ Time Frame: From baseline to end of 12 weeks of treatment ]

To evaluate changes in mammalian target of rapamycin (mTOR) pathway pharmacodynamics (PDx) parameters 		Part I: To evaluate changes in mTOR pathway through changes in pAkt
[ Time Frame: From baseline to end of 12 weeks of treatment ]

To evaluate changes in mammalian target of rapamycin (mTOR) pathway pharmacodynamics (PDx) parameters
2. Part I: To assess the total drug exposure (AUC) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients. 		Part I: To assess the total drug exposure (AUC) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients.
3. Part I: To assess the maximum concentration (Cmax) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients. 		Part I: To assess the maximum concentration (Cmax) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients.
4. Part I: To assess the time to maximum concentration (Tmax) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients. 		Part I: To assess the time to maximum concentration (Tmax) of leniolisib in pediatric patients (aged 4 to 11 years) with APDS
[ Time Frame: From baseline to end of 12 weeks of treatment ]

Population pharmacokinetics (popPK) model that describes the appropriate covariates (eg, body weight and age) that influence leniolisib PK in pediatric patients.
5. Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in lymphadenopathy as a key secondary endpoint of Part II may include 3D volume of index and measurable non-index lesions selected as per the Cheson methodology. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time. 		Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in lymphadenopathy as a key secondary endpoint of Part II may include 3D volume of index and measurable non-index lesions selected as per the Cheson methodology. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time.
6. Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in 3D volume and bi-dimensional or 3D sizes of spleen, where appropriate. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time. 		Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in 3D volume and bi-dimensional or 3D sizes of spleen, where appropriate. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time.
7. Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in 3D volume and bi-dimensional or 3D sizes of liver, where appropriate. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time. 		Part II: Changes from baseline for Reduction in lymphadenopathy as measured by MRI or low-dose CT
[ Time Frame: Day 85 to through study completion, an average of 1 year ]

Parameters for reduction in 3D volume and bi-dimensional or 3D sizes of liver, where appropriate. Summary statistics will be provided by visit. Arithmetic mean with SD of absolute values and change from baseline values may be plotted across time.
8. Part I and II: Key secondary efficacy outcomes for Part I include incidence of infections and use of antibiotics.
[ Time Frame: Part I: Baseline to Day 85 Part II: through study completion, an average of 1 year ]

The number and percentage of patients with infections, and the total number of infections will be summarized. The number and percentage of antibiotics taken will be presented along with number of patients for Part I. Use of immunoglobulin replacement therapy over time will be summarized. 		Part I and II: Key secondary efficacy outcomes for Part I include incidence of infections and use of antibiotics.
[ Time Frame: Part I: Baseline to Day 85 Part II: through study completion, an average of 1 year ]

The number and percentage of patients with infections, and the total number of infections will be summarized. The number and percentage of antibiotics taken will be presented along with number of patients for Part I. Use of immunoglobulin replacement therapy over time will be summarized.
9. Part I and II: Pediatric Quality of Life Inventory (PedsQLTM) Parent Report for Children Questionnaire 4.0 Generic Core Scales
[ Time Frame: Part I: Baseline, Day 29, 57, & 85 Part II: through study completion, an average of 1 year ]

To assess the ability of leniolisib to modify health related quality of life in pediatric patients with APDS 		Part I and II: Pediatric Quality of Life Inventory (PedsQLTM) Parent Report for Children Questionnaire 4.0 Generic Core Scales
[ Time Frame: Part I: Baseline, Day 29, 57, & 85 Part II: through study completion, an average of 1 year ]

To assess the ability of leniolisib to modify health related quality of life in pediatric patients with APDS
Open or close this module Eligibility
Minimum Age: 1 Year 1 Year
Maximum Age: 6 Years 6 Years
Sex: All All
Gender Based:
Accepts Healthy Volunteers: NoNo
Criteria:

Inclusion Criteria:

  1. Patient is male or female and between the age of 1 to 6 years old at time of the first study procedure.
  2. Patient weighs ≥8 and ≤37 kg at baseline.
  3. Patient has a confirmed PI3Kδ genetic mutation of either the PIK3CD (APDS1) or PIK3R1 (APDS2) gene.
  4. Patient has at least 1 measurable nodal lesion on MRI or low-dose CT within 6 months of screening.
  5. Patient has nodal or extranodal lymphoproliferation and clinical findings consistent with APDS (eg, a history of repeated oto-sino-pulmonary infections or organ dysfunction consistent with APDS).
  6. Patient has the ability to ingest unaltered study-related medications without difficulty in the investigator's opinion.
  7. At screening, vital signs (body temperature, systolic BP, diastolic BP, and pulse rate [PR]) will be assessed in the sitting position after the patient has been at rest for at least 3 minutes. Patient's sitting vital signs should be within the following ranges:
    1. Systolic BP: Less than the 95th percentile adjusted for sex, age, and height percentile. See Section 10.5, Appendix 5 to determine BP percentiles adjusted for sex, age, and height percentile. (National High Blood Pressure Education Program Working Group on High Blood Pressure in Children and Adolescents, 2004). See Section 10.5, Appendix 5 to determine height percentiles.
    2. Diastolic BP: Less than the 95th percentile adjusted for sex, age, and height percentile. See Section 10.5, Appendix 5 to determine BP percentiles adjusted for sex, age, and height percentile. See Section 10.6, Appendix 6 to determine height percentiles.
    3. Pulse rate (Fleming 2011):

    i. Age <2 years: 100 to 190 bpm ii. Age 2 to 6 years: 60 to 140 bpm

  8. Institutional review board- or IEC-approved written informed consent or assent and privacy language as per national and local regulations must be obtained from the patient and/or parent or legal guardian prior to any study-related procedures.
  9. Patient parent or legal guardian is willing and able to complete the informed consent or assent process and comply with study procedures and visit schedule.
  10. Patient parent or legal guardian agrees patient will not participate in any other interventional study while enrolled in this study.

Exclusion Criteria:

  1. Patient has previous or concurrent use of immunosuppressive medication such as:
    1. an mTOR inhibitor (eg, sirolimus, rapamycin, everolimus) or a PI3Kδ inhibitor (selective or non-selective PI3K inhibitors) within 6 weeks prior to first dose.

      o Short-term use for up to a total of 5 days is allowed but only up to 1 month prior to enrollment in the study.

    2. B cell depleters (eg, rituximab) within 6 months prior to first dose of study medication.

      o If patient has received prior treatment with a B cell depleter, absolute B lymphocyte counts in the blood must have regained normal values.

    3. Belimumab or cyclophosphamide within 6 months prior to first dose of study medication.
    4. Cyclosporine A, mycophenolate, 6-mercaptopurine, azathioprine, or methotrexate within 3 months prior to first dose of study medication.
    5. Glucocorticoids above a dose equivalent to either ≥2 mg/kg of body weight for weights less than 10 kg or ≥20 mg/day for weights ≥ 10 kg of prednisone or prednisolone or equivalent within 2 weeks prior to first dose of study medication.
    6. Other immunosuppressive medication where effects are expected to persist at start of dosing of study medication.
  2. Patient has a history or current diagnosis of ECG abnormalities indicating significant risk of safety for patients participating in the study such as:
    1. History of familial long QT syndrome or known family history of Torsades de Pointes.
    2. Concomitant clinically significant cardiac arrhythmias, eg, sustained ventricular tachycardia, and clinically significant second or third degree atrioventricular block without a pacemaker.
    3. Resting QTc (Fridericia preferred, but Bazett acceptable) >460 msec if the measurement is confirmed with an additional ECG repeated as soon as possible.
    4. Concomitant use of agents known to prolong the QT interval unless it can be permanently discontinued for the duration of the study.
  3. Patient is currently using a medication known to be strong inhibitor or moderate or strong inducer of isoenzyme CYP3A (see Table 2), if treatment cannot be discontinued or switched to a different medication prior to starting study treatment.
  4. Patient is currently using medications that are metabolized by isoenzyme CYP1A2 and have a narrow therapeutic index (NTI) (drugs whose exposure response indicates that increases in their exposure levels by the concomitant use of potent inhibitors may lead to serious safety concerns [eg, Torsades de Pointes]).
  5. Patient had been administered live vaccines (this includes any attenuated live vaccines) starting from 6 weeks before the anticipated first study drug administration, during the study, and up to 7 days after the last dose of leniolisib.
  6. Patient has clinically significant abnormalities in hematology or clinical chemistry (blood chemistry or urinalysis) parameters as determined by the investigator or medical monitor.
  7. Patient has liver disease or liver injury as indicated by clinically significant abnormal liver function tests (LFTs) (alanine aminotransferase and aspartate aminotransferase >2.5 times upper limit of normal), history of renal injury or renal disease (eg, renal trauma, glomerulonephritis, or one kidney only), or presence of impaired renal function as indicated by a serum creatinine level >1.5 mg/dL (133 μmol/L).
  8. Patient has moderate or severe hepatic impairment (Child-Pugh Class B or C).
  9. Patient is receiving concurrent treatment with another investigational therapy or use of another investigational therapy less than 4 weeks from the first study procedure.
  10. Patient has active hepatitis B (eg, hepatitis B surface antigen reactive) or active hepatitis C (eg, hepatitis C virus RNA [qualitative] is detected) at screening.
  11. Patient has human immunodeficiency virus (HIV) infection (HIV 1 or 2) at screening.
  12. Patient has a positive COVID-19 result (polymerase chain reaction or antigen) within 1 week prior to first dose. The patient can be rescreened after a subsequent negative result.
  13. Patient has a history of malignancy (except lymphoma) within 3 years before the first study procedure or has evidence of residual disease from a previously diagnosed malignancy.
  14. Patient has a previous diagnosis of lymphoma that has been treated with chemotherapy, radiotherapy, or transplant within 1 year of the first study procedure or is anticipated to require lymphoma treatment within 6 months of the first study procedure.
  15. Patient has a history of uncontrolled diabetes mellitus within 3 months of the first study procedure.
  16. Patient has had major surgery requiring hospitalization or radiotherapy within 4 weeks prior to the first study procedure.
  17. Patient has uncontrolled chronic or recurrent infectious disease (with the exception of those that are considered to be characteristic of APDS) or evidence of tuberculosis infection as defined by a positive QuantiFERON Gold test at screening. If presence of latent tuberculosis is established, then treatment according to local country guidelines must have been completed before patients can be considered for enrollment.
  18. Patient has a known allergy or hypersensitivity to study defined medications or their excipients.
  19. Patient has a planned or expected major surgical procedure.
  20. Patient or parent or legal guardian is unable or unwilling to comply with study procedures or is unable to travel for repeat visits.
  21. Patient or parent or legal guardian is unwilling to keep study results or observations confidential or to refrain from posting confidential study results or observations on social media sites.
  22. Patient or parent or legal guardian refuses to sign consent or assent form.
  23. Patient has other underlying medical condition that, in the opinion of the investigator, would impair the ability of the patient to receive or tolerate the planned procedures or follow-up.

    -

Inclusion Criteria:

  1. Patient is male or female and between the age of 1 to 6 years old at time of the first study procedure.
  2. Patient weighs ≥8 and ≤37 kg at baseline.
  3. Patient has a confirmed PI3Kδ genetic mutation of either the PIK3CD (APDS1) or PIK3R1 (APDS2) gene.
  4. Patient has at least 1 measurable nodal lesion on MRI or low-dose CT within 6 months of screening.
  5. Patient has nodal or extranodal lymphoproliferation and clinical findings consistent with APDS (eg, a history of repeated oto-sino-pulmonary infections or organ dysfunction consistent with APDS).
  6. Patient has the ability to ingest unaltered study-related medications without difficulty in the investigator's opinion.
  7. At screening, vital signs (body temperature, systolic BP, diastolic BP, and pulse rate [PR]) will be assessed in the sitting position after the patient has been at rest for at least 3 minutes. Patient's sitting vital signs should be within the following ranges:
    1. Systolic BP: Less than the 95th percentile adjusted for sex, age, and height percentile. See Section 10.5, Appendix 5 to determine BP percentiles adjusted for sex, age, and height percentile. (National High Blood Pressure Education Program Working Group on High Blood Pressure in Children and Adolescents, 2004). See Section 10.5, Appendix 5 to determine height percentiles.
    2. Diastolic BP: Less than the 95th percentile adjusted for sex, age, and height percentile. See Section 10.5, Appendix 5 to determine BP percentiles adjusted for sex, age, and height percentile. See Section 10.6, Appendix 6 to determine height percentiles.
    3. Pulse rate (Fleming 2011):

    i. Age <2 years: 100 to 190 bpm ii. Age 2 to 6 years: 60 to 140 bpm

  8. Institutional review board- or IEC-approved written informed consent or assent and privacy language as per national and local regulations must be obtained from the patient and/or parent or legal guardian prior to any study-related procedures.
  9. Patient parent or legal guardian is willing and able to complete the informed consent or assent process and comply with study procedures and visit schedule.
  10. Patient parent or legal guardian agrees patient will not participate in any other interventional study while enrolled in this study.

Exclusion Criteria:

  1. Patient has previous or concurrent use of immunosuppressive medication such as:
    1. an mTOR inhibitor (eg, sirolimus, rapamycin, everolimus) or a PI3Kδ inhibitor (selective or non-selective PI3K inhibitors) within 6 weeks prior to first dose.

      o Short-term use for up to a total of 5 days is allowed but only up to 1 month prior to enrollment in the study.

    2. B cell depleters (eg, rituximab) within 6 months prior to first dose of study medication.

      o If patient has received prior treatment with a B cell depleter, absolute B lymphocyte counts in the blood must have regained normal values.

    3. Belimumab or cyclophosphamide within 6 months prior to first dose of study medication.
    4. Cyclosporine A, mycophenolate, 6-mercaptopurine, azathioprine, or methotrexate within 3 months prior to first dose of study medication.
    5. Glucocorticoids above a dose equivalent to either ≥2 mg/kg of body weight for weights less than 10 kg or ≥20 mg/day for weights ≥ 10 kg of prednisone or prednisolone or equivalent within 2 weeks prior to first dose of study medication.
    6. Other immunosuppressive medication where effects are expected to persist at start of dosing of study medication.
  2. Patient has a history or current diagnosis of ECG abnormalities indicating significant risk of safety for patients participating in the study such as:
    1. History of familial long QT syndrome or known family history of Torsades de Pointes.
    2. Concomitant clinically significant cardiac arrhythmias, eg, sustained ventricular tachycardia, and clinically significant second or third degree atrioventricular block without a pacemaker.
    3. Resting QTc (Fridericia preferred, but Bazett acceptable) >460 msec if the measurement is confirmed with an additional ECG repeated as soon as possible.
    4. Concomitant use of agents known to prolong the QT interval unless it can be permanently discontinued for the duration of the study.
  3. Patient is currently using a medication known to be strong inhibitor or moderate or strong inducer of isoenzyme CYP3A (see Table 2), if treatment cannot be discontinued or switched to a different medication prior to starting study treatment.
  4. Patient is currently using medications that are metabolized by isoenzyme CYP1A2 and have a narrow therapeutic index (NTI) (drugs whose exposure response indicates that increases in their exposure levels by the concomitant use of potent inhibitors may lead to serious safety concerns [eg, Torsades de Pointes]).
  5. Patient had been administered live vaccines (this includes any attenuated live vaccines) starting from 6 weeks before the anticipated first study drug administration, during the study, and up to 7 days after the last dose of leniolisib.
  6. Patient has clinically significant abnormalities in hematology or clinical chemistry (blood chemistry or urinalysis) parameters as determined by the investigator or medical monitor.
  7. Patient has liver disease or liver injury as indicated by clinically significant abnormal liver function tests (LFTs) (alanine aminotransferase and aspartate aminotransferase >2.5 times upper limit of normal), history of renal injury or renal disease (eg, renal trauma, glomerulonephritis, or one kidney only), or presence of impaired renal function as indicated by a serum creatinine level >1.5 mg/dL (133 μmol/L).
  8. Patient has moderate or severe hepatic impairment (Child-Pugh Class B or C).
  9. Patient is receiving concurrent treatment with another investigational therapy or use of another investigational therapy less than 4 weeks from the first study procedure.
  10. Patient has active hepatitis B (eg, hepatitis B surface antigen reactive) or active hepatitis C (eg, hepatitis C virus RNA [qualitative] is detected) at screening.
  11. Patient has human immunodeficiency virus (HIV) infection (HIV 1 or 2) at screening.
  12. Patient has a positive COVID-19 result (polymerase chain reaction or antigen) within 1 week prior to first dose. The patient can be rescreened after a subsequent negative result.
  13. Patient has a history of malignancy (except lymphoma) within 3 years before the first study procedure or has evidence of residual disease from a previously diagnosed malignancy.
  14. Patient has a previous diagnosis of lymphoma that has been treated with chemotherapy, radiotherapy, or transplant within 1 year of the first study procedure or is anticipated to require lymphoma treatment within 6 months of the first study procedure.
  15. Patient has a history of uncontrolled diabetes mellitus within 3 months of the first study procedure.
  16. Patient has had major surgery requiring hospitalization or radiotherapy within 4 weeks prior to the first study procedure.
  17. Patient has uncontrolled chronic or recurrent infectious disease (with the exception of those that are considered to be characteristic of APDS) or evidence of tuberculosis infection as defined by a positive QuantiFERON Gold test at screening. If presence of latent tuberculosis is established, then treatment according to local country guidelines must have been completed before patients can be considered for enrollment.
  18. Patient has a known allergy or hypersensitivity to study defined medications or their excipients.
  19. Patient has a planned or expected major surgical procedure.
  20. Patient or parent or legal guardian is unable or unwilling to comply with study procedures or is unable to travel for repeat visits.
  21. Patient or parent or legal guardian is unwilling to keep study results or observations confidential or to refrain from posting confidential study results or observations on social media sites.
  22. Patient or parent or legal guardian refuses to sign consent or assent form.
  23. Patient has other underlying medical condition that, in the opinion of the investigator, would impair the ability of the patient to receive or tolerate the planned procedures or follow-up.

    -
Open or close this module Contacts/Locations
Central Contact Person: Anurag Relan, MD
Telephone: +31 71 5247 400
Email: medical-information@pharming.com		Anurag Relan, MD
Telephone: +31 71 5247 400
Email: medical-information@pharming.com
Central Contact Backup: Lesia Waynick, BSBA
Email: L.Waynick@pharming.com		Lesia Waynick, BSBA
Email: L.Waynick@pharming.com
Locations: United States, CaliforniaUnited States, California
University of California Los Angeles
[Not yet recruiting]
Los Angeles, California, United States, 90095
Contact:Contact: Manish L Butte, MD
Contact:Contact: Alexis Stephens 310-210-8771 avstephens@mednet.ucla.ed		University of California Los Angeles
[Not yet recruiting]
Los Angeles, California, United States, 90095
Contact:Contact: Manish L Butte, MD
Contact:Contact: Alexis Stephens 310-210-8771 avstephens@mednet.ucla.ed
United States, MarylandUnited States, Maryland
National Institutes of Health
[Not yet recruiting]
Bethesda, Maryland, United States, 20814
Contact:Contact: Koneti Rao, MD
Contact:Contact: Alanvin Orpia alanvin.orpia@nih.gov		National Institutes of Health
[Not yet recruiting]
Bethesda, Maryland, United States, 20814
Contact:Contact: Koneti Rao, MD
Contact:Contact: Alanvin Orpia alanvin.orpia@nih.gov
United States, North CarolinaUnited States, North Carolina
The University of North Carolina
[Not yet recruiting]
Chapel Hill, North Carolina, United States, 27599
Contact:Contact: Amika Sood, MD
Contact:Contact: Miriam Davis Miriam.davis@unc.edu		The University of North Carolina
[Not yet recruiting]
Chapel Hill, North Carolina, United States, 27599
Contact:Contact: Amika Sood, MD
Contact:Contact: Miriam Davis Miriam.davis@unc.edu
United States, OhioUnited States, Ohio
Rainbow Childrens Hospital
[Recruiting]
Shaker Heights, Ohio, United States, 44122
Contact:Contact: Joao Lopes, MD
Contact:Contact: Erica Denallo erica.denallo@UHHospitals.org		Rainbow Childrens Hospital
[Recruiting]
Shaker Heights, Ohio, United States, 44122
Contact:Contact: Joao Lopes, MD
Contact:Contact: Erica Denallo erica.denallo@UHHospitals.org
United States, TexasUnited States, Texas
Texas Children's Hospital
[Not yet recruiting]
Houston, Texas, United States, 77030
Contact:Contact: Lisa Forbes- Satter, MD 832-824-1319
Contact:Contact: Sadaf Batla 832-824-4372 sadaf.batla@bdm.edu		Texas Children's Hospital
[Not yet recruiting]
Houston, Texas, United States, 77030
Contact:Contact: Lisa Forbes- Satter, MD 832-824-1319
Contact:Contact: Sadaf Batla 832-824-4372 sadaf.batla@bdm.edu
BrazilBrazil
ÍMPAR SERVIÇOS HOSPITALARES S/A - Hospital 9 de Julho,
[Not yet recruiting]
São Paulo, Brazil, 01409-902
Contact:Contact: Gabriela Joia 55 (11) 3147-9982 gjoia@h9j.com.br
Contact:Principal Investigator: Mendonca Leonardo, MD 		ÍMPAR SERVIÇOS HOSPITALARES S/A - Hospital 9 de Julho,
[Not yet recruiting]
São Paulo, Brazil, 01409-902
Contact:Contact: Gabriela Joia 55 (11) 3147-9982 gjoia@h9j.com.br
Contact:Principal Investigator: Mendonca Leonardo, MD
JapanJapan
Kyoto University Hospital
[Recruiting]
Kyoto, Japan, 606-8507		Kyoto University Hospital
[Recruiting]
Kyoto, Japan, 606-8507
Tokyo Medical and Dental University Hospital
[Recruiting]
Tokyo, Japan, 113-8519		Tokyo Medical and Dental University Hospital
[Recruiting]
Tokyo, Japan, 113-8519
PortugalPortugal
Hospital Pediátrico Do Centro Hospitalar Da Universidade de Coimbra
[Not yet recruiting]
Coimbra, Portugal
Contact:Contact: Sandra Ferreria, MD
Contact:Contact: Inês Silva inesmatos.silva@blueclinical.pt		Hospital Pediátrico Do Centro Hospitalar Da Universidade de Coimbra
[Not yet recruiting]
Coimbra, Portugal
Contact:Contact: Sandra Ferreria, MD
Contact:Contact: Inês Silva inesmatos.silva@blueclinical.pt
SpainSpain
Hospital Universitario Virgen del Rocío
[Not yet recruiting]
Sevilla, Spain, 41013
Contact:Contact: Blanca Taboada +34656285633 blancataboadanoguer@hotmail.com
Contact:Principal Investigator: Olaf Neth, MD 		Hospital Universitario Virgen del Rocío
[Not yet recruiting]
Sevilla, Spain, 41013
Contact:Contact: Blanca Taboada +34656285633 blancataboadanoguer@hotmail.com
Contact:Principal Investigator: Olaf Neth, MD
TurkeyTurkey
Marmara University Pendik Research and Training Hospital
[Not yet recruiting]
Istanbul, Turkey, 34899
Contact:Contact: Elif Aydiner, MD 00902166259090
Contact:Contact: Arzu Takak 00905330298916 arzu.takak@ethic-cro.com		Marmara University Pendik Research and Training Hospital
[Not yet recruiting]
Istanbul, Turkey, 34899
Contact:Contact: Elif Aydiner, MD 00902166259090
Contact:Contact: Arzu Takak 00905330298916 arzu.takak@ethic-cro.com
United KingdomUnited Kingdom
Great Ormond Street Hospital
[Not yet recruiting]
London, United Kingdom, WC1N3JH
Contact:Contact: Jade Sugars Jade.Sugars@gosh.nhs.uk
Contact:Principal Investigator: Austen Worth, MD 		Great Ormond Street Hospital
[Recruiting]
London, United Kingdom, WC1N3JH
Contact:Contact: Jade Sugars Jade.Sugars@gosh.nhs.uk
Contact:Principal Investigator: Austen Worth, MD
Open or close this module IPDSharing
Plan to Share IPD: No No
Open or close this module References
Citations:
Links:
Available IPD/Information:
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