PIN in Combination With Anti-PD1 in Previously Treated Solid Tumor

Last updated: June 5, 2025
Sponsor: Chinese PLA General Hospital
Overall Status: Active - Recruiting

Phase

1

Condition

Neoplasms

Neuroblastoma

Treatment

PIN +anti-PD1

Clinical Study ID

NCT06883149
CHN-PLAGH-BT-094
  • Ages 18-75
  • All Genders

Study Summary

In this single-center,open-label, phase I study, the safety and efficacy of PIN in combination with programmed cell death protein antibody (anti-PD1) therapeutic regimen will be evaluated in patients with late-stage advanced solid tumors . A total of 20 to 30 patients are planned to be enrolled and receive PIN plus anti-PD1 combined treatment. It aims to: 1).assess the safety and antitumor effects of the above combined treatment regimen. 2).detect the dynamic changes and molecular characteristics of PIN-induced CD8+ T cells with special phenotype in peripheral blood (PB) and transformation of tumor microenvironment (TME) after the treatment with PIN. 3).evaluate the immunological or clinical predictive biomarkers for toxicity and efficacy.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  1. Age 18-75 (inclusive).

  2. Eastern Cooperative Oncology Group (ECOG) performance status ≤2 and Estimated lifeexpectancy of more than 3 months.

  3. Histopathological confirmed advanced or metastatic solid tumors failed to at leastfirst-line treatment or initially diagnosed advanced/metastatic solid tumors thathave no National Comprehensive Cancer Network (NCCN) guideline recommended standardfirst-line therapy.

  4. Patients with previous anti-PD-1/ PD-L1 antibodies treatmentresistance,non-response,or low response tumor types (such as hepatic carcinoma,etal) .

  5. At least one measurable lesion at baseline according to RECIST 1.1.

  6. Patients with injectable lesions (those suitable for direct injection or injectionwith the assistance of medical imaging), defined as follows: at least one injectablelesion in the skin, mucous membrane, subcutaneous tissue, lymph node or visceralorgan with a longest diameter ≥10 mm.

  7. Subjects are willing to accept tumor rebiopsy in the process of this study.

  8. Adequate organ function as defined by the following criteria:

  • Absolute neutrophil count (ANC) ≥ 1 x 10^9/L, Platelet count ≥50 x 10^9/ L,hemoglobin (Hgb) ≥ 80g/L ;

  • Serum creatinine≤1.5 upper limit of normal (ULN) or creatinine clearance (asestimated by Cockcroft Gault) ≥60 mL/min;

  • Serum aspartate amino transferase (AST) and alanine aminotransferase (ALT), ≤3.0 x ULN (≤5 x ULN for patients with liver cancer or metastases); Total serumbilirubin ≤1.5 x ULN(≤3 x ULN for patients with liver cancer or metastases);

  • Cardiac ejection fraction ≥ 50%, no evidence of pericardial effusion asdetermined by an echocardiogram (ECHO), and no clinically significantelectrocardiogram (ECG) findings;

  • International Normalized Ratio (INR) ≤ 1.5 times the upper limit of normal (ULN), and Activated Partial Thromboplastin Time (APTT) ≤ 1.5 times ULN;

  • Baseline oxygen saturation >91% on room air.

  1. Previous treatment must be completed for more than 4 weeks prior to the enrollmentof this study, and subjects have recovered to <= grade 1 Toxicity (except forhematological toxicities and clinically non-significant toxicities such asalopecia).

  2. Pregnancy tests for women of childbearing age shall be negative; Both men and womenagreed to use effective contraception during treatment and during the subsequent 1year.

  3. Voluntarily participate in this clinical trial and sign an informed consent form.

Exclusion

Exclusion Criteria:

  1. Subjects are being treated with either corticosteroids (>10 mg daily prednisoneequivalent) or other immunosuppressive medications within 14 days of enrollment.

  2. Active central nervous system disease involvement (but allow patients with priorbrain metastases treated at least 4 weeks prior to enrollment that are clinicallystable and do not require intervention), or prior history of Common TerminologyCriteria for Adverse Events (CTCAE) Grade ≥3 drug-related Central Nervous System (CNS) toxicity.

  3. Presence or suspicion of fungal, bacterial, viral, or other infection that isuncontrolled or requiring intravenous (IV) antimicrobials for management.

  4. Any serious underlying medical (eg, pulmonary, renal, hepatic,gastrointestinal, orneurological) or psychiatric condition or any issue that would limit compliance withstudy requirements.

  5. Major surgery or trauma occurred within 28 days prior to enrollment, or major sideeffects have not been recovered.

  6. Received cytotoxic chemicals, monoclonal antibodies, immunotherapy or otherintervene within 4 weeks or 5 half-lives before enrollment.

  7. Received radiotherapy within 3 months before enrollment.

  8. Patients with primary immunodeficiency or autoimmune diseases requiringimmunosuppressive therapy.

  9. The presence of uncontrollable serous membrane fluid, such as massive pleuraleffusion or ascites.

  10. Previous or concurrent cancer within 3 years prior to treatment start except forcuratively treated cervical cancer in situ, non-melanoma skin cancer, superficialbladder tumors [Ta (non-invasive tumor), Tis (carcinoma in situ) and T1 (tumorinvades lamina propria)].

  11. Known positive test result for human immunodeficiency virus (HIV) or acquired immunedeficiency syndrome (AIDS).

  12. Prior organ allograft transplantations or allogeneic hematopoietic stem celltransplantation.

  13. History of allergy or intolerance to study drug components.

  14. Pregnant or breast-feeding. Women of childbearing potential must have a pregnancytest performed within 7 days before the enrollment, and a negative result must bedocumented.

  15. Being participating any other trials or withdraw within 4 weeks.

  16. Researchers believe that other reasons are not suitable for clinical trials.

Study Design

Total Participants: 25
Treatment Group(s): 1
Primary Treatment: PIN +anti-PD1
Phase: 1
Study Start date:
March 19, 2025
Estimated Completion Date:
December 01, 2030

Study Description

Several clinical studies have found that oncolytic viruses can provide clinical benefits to patients with different types, stages, and even advanced metastatic tumors. Especially when used in combination with immunotherapy, oncolytic viruses can sensitize tumor types that were initially unresponsive to immune checkpoint inhibitors.To date, there are hundreds of projects in clinical trial stages, especially in recent years, new generations of oncolytic viruses developed or in clinical stages have shown better safety and stronger anti-tumor capabilities. Through genetic engineering, oncolytic viruses can express target genes that have anti-tumor effects, such as granulocyte-macrophage colony-stimulating factor (GM-CSF), interleukin-12(IL-12),etc, further enhancing their anti-tumor effects. Despite these advances, how to obtain a more durable anti-tumor immune response and long-term benefits is still an urgent clinical issue.

Previous studies have confirmed that the Newcastle disease oncolytic virus (NDV) can selectively infect tumor cells while sparing normal cells, demonstrating an acceptable safety profile. In this study, investigators have developed a nove PIN . Preclinical studies have shown that combining PIN with anti-PD1 therapy can reverse the immunosuppressive microenvironment and transform "cold" tumors into "hot" tumors, thereby triggering local and systemic anti-tumor immune responses and significantly improving the efficacy of the immune checkpoint inhibitor(ICI). Based on these preclinical findings, investigators are conducting this clinical trial to evaluate the safety and anti-tumor activity of the PIN and anti-PD1 combination therapy in vivo.

In this study, 20 to 30 subjects will be enrolled. The initial dose for the first cycle will be determined as 4e9 or 8e9 viral particles based on the number of injectable lesions, their longest diameter, and the tumor volume capacity. Following the first cycle of treatment, the subsequent dose and injection sites of PIN will be adjusted based on the permissible volume of the injected tumor mass, according to the following principles:

PIN injection frequency: day 0 and day 3, per 3 weeks for 8 cycles; unless unavailability of injection lesion, disease progression (PD) or serious intolerable adverse events (AEs).

PIN injection dosage:

  1. a.For patients with a single injectable lesion with a maximum diameter of <8 cm, the initial cycle's PIN dose is 4e9 viral particles. Subsequent cycles will maintain this dose of 4e9 or increase it to 8e9 viral particles based on the lesion's capacity to accommodate the injection volume;

    b. For patients with a single injectable lesion with a maximum diameter of ≥8 cm, the initial cycle's PIN dose is 8e9 viral particles. Subsequent cycles will maintain this dose of 8e9 viral particles based on the lesion's capacity to accommodate the injection volume.

  2. a.For patients with two injectable lesions, injections will alternate between the two lesions after two cycles. The initial cycle's PIN dose is 4e9 viral particles, and the second cycle will maintain this dose of 4e9 or increase it to 8e9 viral particles based on the tumor volume's capacity;

    b.For patients with injectable lesions with a maximum diameter of ≥8 cm, the initial cycle's PIN dose is 8e9 viral particles, and subsequent cycles will maintain this dose of 8e9 or decrease it to 4e9 viral particles based on the lesion's capacity.

  3. a.For patients with multiple injectable lesions (≥ 3), after 1-2 cycles of injections in each injectable lesion, injections are alternated between lesions. The initial injection dose for each lesion is determined by the size of the lesion;

    b.For lesions <3 cm, the initial cycle's dose is 4e9 viral particles, and the second cycle will maintain this dose of 4e9 or increase it to 8e9 viral particles based on the tumor volume's capacity;

    c.For lesions ≥3 cm, the initial cycle's injection dose is selected as 8e9 viral particles, and subsequent cycles will maintain this dose of 8e9 or decrease it to 4e9 viral particles based on the tumor volume's capacity.

  4. After injections, if the tumor shrinks by 0.5-1 cm in diameter, the injection dose should be adjusted to 2e9 viral particles until the tumor disappears.

Anti-PD1 infusion frequency: day -3, per 3 weeks for 8 cycles; until unacceptable toxicity occurred or PD.

Objectives:

The primary objective are to assess the safety and adverse event profile of the combination regimen.

The coprimary objective is immue response, assessed by CD8+T cells with special phenotype by Fluorescence Activating Cell Sorter (FACS).

The secondary objectives are to evaluate disease control rate (DCR), objective response rate (ORR), duration of response (DOR), progression-free survival (PFS), overall survival (OS), and quality of life.

Connect with a study center

  • Biotherapeutic Department of Chinsese PLA Gereral Hospital

    Beijing, Beijing
    China

    Active - Recruiting

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