Clinical Trials Register

Summary
EudraCT Number:	2018-001608-12
Sponsor's Protocol Code Number:	IOV-COM-202
National Competent Authority:	Spain - AEMPS
Clinical Trial Type:	EEA CTA
Trial Status:	Ongoing
Date on which this record was first entered in the EudraCT database:	2018-11-23
Trial results

Index
A. PROTOCOL INFORMATION
B. SPONSOR INFORMATION
C. APPLICANT IDENTIFICATION
D. IMP IDENTIFICATION
D.8 INFORMATION ON PLACEBO
E. GENERAL INFORMATION ON THE TRIAL
F. POPULATION OF TRIAL SUBJECTS
G. INVESTIGATOR NETWORKS TO BE INVOLVED IN THE TRIAL
N. REVIEW BY THE COMPETENT AUTHORITY OR ETHICS COMMITTEE IN THE COUNTRY CONCERNED
P. END OF TRIAL

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A. Protocol Information

A.1

Member State Concerned

Spain - AEMPS

A.2

EudraCT number

2018-001608-12

A.3

Full title of the trial

A Phase 2, Multicenter Study of Autologous Tumor Infiltrating Lymphocytes (LN-144 or LN-145) in Patients with Solid Tumors

Estudio en fase 2, multicéntrico, de linfocitos infiltrantes de tumores autólogos (LN-144 o LN-145) en pacientes con tumores sólidos.

A.3.1

Title of the trial for lay people, in easily understood, i.e. non-technical, language

A clinical study to investigate if the investigational products, called LN-144 and LN-145 (also known as Tumour Infiltrating Lymphocytes), are safe and beneficial in the treatment of patients with Solid Tumours.

Ensayo clínico para investigar si los productos en investigación, denominados LN-144 y LN-145 (también conocidos como linfocitos infiltrantes de tumores) son seguros y beneficiosos en el tratamiento de pacientes con tumores sólidos.

A.3.2

Name or abbreviated title of the trial where available

Study of LN-144 and LN-145 in the Treatment of Patients with Solid Tumours

Estudio de LN-144 y LN-145 en el tratamiento de pacientes con tumores sólidos

A.4.1

Sponsor's protocol code number

IOV-COM-202

A.7

Trial is part of a Paediatric Investigation Plan

A.8

EMA Decision number of Paediatric Investigation Plan

B. Sponsor Information
B.Sponsor: 1
B.1.1	Name of Sponsor	Iovance Biotherapeutics, Inc.
B.1.3.4	Country	United States
B.3.1 and B.3.2	Status of the sponsor	Commercial
B.4 Source(s) of Monetary or Material Support for the clinical trial:
B.4.1	Name of organisation providing support	Iovance Biotherapeutics, Inc.
B.4.2	Country	United States
B.5 Contact point designated by the sponsor for further information on the trial
B.5.1	Name of organisation	Iovance Biotherapeutics, Inc.
B.5.2	Functional name of contact point	IOV-COM-202 Study Manager
B.5.3	Address:
B.5.3.1	Street Address	999 Skyway Road, Suite 150
B.5.3.2	Town/ city	San Carlos
B.5.3.3	Post code	94070
B.5.3.4	Country	United States
B.5.4	Telephone number	+18665654410
B.5.6	E-mail	Clinical.Inquiries@iovance.com

D. IMP Identification
D.IMP: 1
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	No
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	LN-144
D.3.2	Product code	LN-144
D.3.4	Pharmaceutical form	Solution for infusion
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	Lifileucel
D.3.9.2	Current sponsor code	LN-144
D.3.9.3	Other descriptive name	Tumour Infiltrating Lymphocytes
D.3.10	Strength
D.3.10.1	Concentration unit	Other
D.3.10.2	Concentration type	range
D.3.10.3	Concentration number	3300000000 to 30000000000
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	No
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	Yes
D.3.11.3.1	Somatic cell therapy medicinal product	Yes
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	Yes
D.3.11.3.5.1	CAT classification and reference number	Somatic cell therapy medicinal product, ref #: H0004741
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 2
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	Yes
D.2.1.1.1	Trade name	Fludarabine Phosphate
D.2.1.1.2	Name of the Marketing Authorisation holder	Actavis Group PTC ehf.
D.2.1.2	Country which granted the Marketing Authorisation	Lithuania
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	Fludarabine Phosphate
D.3.4	Pharmaceutical form	Concentrate for solution for infusion
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	FLUDARABINE PHOSPHATE
D.3.9.1	CAS number	75607-67-9
D.3.9.3	Other descriptive name	Fludarabine Phosphate
D.3.9.4	EV Substance Code	SUB13897MIG
D.3.10	Strength
D.3.10.1	Concentration unit	mg/ml milligram(s)/millilitre
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	25
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	Yes
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 3
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	Yes
D.2.1.1.1	Trade name	Cyclophosphamide
D.2.1.1.2	Name of the Marketing Authorisation holder	Baxter Healthcare Ltd.
D.2.1.2	Country which granted the Marketing Authorisation	United Kingdom
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	Cyclophosphamide Injection
D.3.4	Pharmaceutical form	Powder for solution for injection
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	CYCLOPHOSPHAMIDE
D.3.9.1	CAS number	50-18-0
D.3.9.4	EV Substance Code	SUB06859MIG
D.3.10	Strength
D.3.10.1	Concentration unit	mg milligram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	1000
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	Yes
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 4
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	No
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	LN-145
D.3.2	Product code	LN-145
D.3.4	Pharmaceutical form	Solution for infusion
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	LN-145
D.3.9.2	Current sponsor code	LN-145
D.3.9.3	Other descriptive name	Tumour Infiltrating Lymphocytes
D.3.10	Strength
D.3.10.1	Concentration unit	Other
D.3.10.2	Concentration type	range
D.3.10.3	Concentration number	3300000000 to 30000000000
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	No
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	No
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	Yes
D.3.11.3.1	Somatic cell therapy medicinal product	Yes
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	No
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 5
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	Yes
D.2.1.1.1	Trade name	KEYTRUDA®
D.2.1.1.2	Name of the Marketing Authorisation holder	Merck Sharp & Dohme Limited
D.2.1.2	Country which granted the Marketing Authorisation	European Union
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.1	Product name	pembrolizumab
D.3.4	Pharmaceutical form	Powder for concentrate for solution for infusion
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	PEMBROLIZUMAB
D.3.9.3	Other descriptive name	KEYTRUDA
D.3.9.4	EV Substance Code	SUB167136
D.3.10	Strength
D.3.10.1	Concentration unit	mg milligram(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	50
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	No
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	Yes
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	Yes
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No
D.IMP: 6
D.1.2 and D.1.3	IMP Role	Test
D.2	Status of the IMP to be used in the clinical trial
D.2.1	IMP to be used in the trial has a marketing authorisation	Yes
D.2.1.1.1	Trade name	Proleukin
D.2.1.1.2	Name of the Marketing Authorisation holder	Novartis Pharmaceuticals UK Limited
D.2.1.2	Country which granted the Marketing Authorisation	United Kingdom
D.2.5	The IMP has been designated in this indication as an orphan drug in the Community	No
D.2.5.1	Orphan drug designation number
D.3 Description of the IMP
D.3.4	Pharmaceutical form	Powder for solution for injection/infusion
D.3.4.1	Specific paediatric formulation	No
D.3.7	Routes of administration for this IMP	Intravenous use
D.3.8 to D.3.10 IMP Identification Details (Active Substances)
D.3.8	INN - Proposed INN	Proleukin
D.3.9.1	CAS number	8000048-25-1
D.3.9.3	Other descriptive name	INTERLEUKIN-2
D.3.9.4	EV Substance Code	SUB14225MIG
D.3.10	Strength
D.3.10.1	Concentration unit	IU international unit(s)
D.3.10.2	Concentration type	equal
D.3.10.3	Concentration number	18000000
D.3.11 The IMP contains an:
D.3.11.1	Active substance of chemical origin	No
D.3.11.2	Active substance of biological/ biotechnological origin (other than Advanced Therapy IMP (ATIMP)	Yes
	The IMP is a:
D.3.11.3	Advanced Therapy IMP (ATIMP)	No
D.3.11.3.1	Somatic cell therapy medicinal product	No
D.3.11.3.2	Gene therapy medical product	No
D.3.11.3.3	Tissue Engineered Product	No
D.3.11.3.4	Combination ATIMP (i.e. one involving a medical device)	No
D.3.11.3.5	Committee on Advanced therapies (CAT) has issued a classification for this product	No
D.3.11.4	Combination product that includes a device, but does not involve an Advanced Therapy	No
D.3.11.5	Radiopharmaceutical medicinal product	No
D.3.11.6	Immunological medicinal product (such as vaccine, allergen, immune serum)	No
D.3.11.7	Plasma derived medicinal product	No
D.3.11.8	Extractive medicinal product	No
D.3.11.9	Recombinant medicinal product	Yes
D.3.11.10	Medicinal product containing genetically modified organisms	No
D.3.11.11	Herbal medicinal product	No
D.3.11.12	Homeopathic medicinal product	No
D.3.11.13	Another type of medicinal product	No

D.8 Information on Placebo

E. General Information on the Trial

E.1 Medical condition or disease under investigation

E.1.1

Medical condition(s) being investigated

Solid Tumours including advanced unresectable or metastatic melanoma (MM), advanced squamous cell carcinoma of the head and neck (HNSCC) and non-small cell lung cancer (NSCLC)

Tumores sólidos incluyendo melanoma metastásico avanzado (MM) o irresecable, carcinoma epidermoide de cabeza y cuello avanzado (CECC) y cáncer de pulmón no microcítico (CPNM)

E.1.1.1

Medical condition in easily understood language

Solid Tumours are growths of tissue which form a mass. In this study these solid tumours are cancerous.

Los tumores sólidos son crecimientos de tejido que forman una masa. En este estudio los tumores sólidos son cancerígenos.

E.1.1.2

Therapeutic area

Diseases [C] - Cancer [C04]

MedDRA Classification

E.1.2 Medical condition or disease under investigation

E.1.2	Version	20.0
E.1.2	Level	PT
E.1.2	Classification code	10060121
E.1.2	Term	Squamous cell carcinoma of head and neck
E.1.2	System Organ Class	10029104 - Neoplasms benign, malignant and unspecified (incl cysts and polyps)

E.1.2 Medical condition or disease under investigation

E.1.2	Version	20.0
E.1.2	Level	LLT
E.1.2	Classification code	10027481
E.1.2	Term	Metastatic melanoma
E.1.2	System Organ Class	10029104 - Neoplasms benign, malignant and unspecified (incl cysts and polyps)

E.1.2 Medical condition or disease under investigation

E.1.2	Version	20.0
E.1.2	Level	PT
E.1.2	Classification code	10061873
E.1.2	Term	Non-small cell lung cancer
E.1.2	System Organ Class	10029104 - Neoplasms benign, malignant and unspecified (incl cysts and polyps)

E.1.3

Condition being studied is a rare disease

E.2 Objective of the trial

E.2.1

Main objective of the trial

•To evaluate the efficacy of autologous TIL LN-144/LN-145 as a single-therapy in NSCLC patients or in combination with pembrolizumab in MM and HNSCC patients by determining the ORR, using the Response Evaluation Criteria in Solid Tumors (RECIST 1.1) as assessed by Investigator.
•To characterize the safety profile of TIL LN-144/LN-145 as a single-therapy in NSCLC patients or in combination with pembrolizumab in MM and HNSCC patients as measured by the incidence of Grade ≥3 treatment-emergent adverse events (TEAEs).

- Evaluar la eficacia de los LIT autólogos LN-144 y LN-145 en monoterapia en pacientes con CPNM o en combinación con pembrolizumab en pacientes con MM o CECC mediante la determinación de la tasa de respuestas objetivas (TRO) utilizando los Criterios de evaluación de la respuesta en tumores sólidos (RECIST 1.1) evaluados por el investigador.
- Describir el perfil de seguridad de los LIT LN-144 y LN-145 en monoterapia en pacientes con CPNM o en combinación con pembrolizumab en pacientes con MMo CECC , determinado por la incidencia de acontecimientos adversos aparecidos durante el tratamiento (AAAT) de grado ≥ 3.

E.2.2

Secondary objectives of the trial

• To further evaluate the efficacy of autologous TIL LN-144/LN-145 as a single-therapy in NSCLC patients or in combination with pembrolizumab in MM and HNSCC patients using CR rate, durations of response (DOR), disease control rates (DCR), PFS using RECIST 1.1 as assessed by Investigator, and OS.

Evaluar más a fondo la eficacia de los LIT autólogos LN-144y LN-145 en monoterapia o en combinación con pembrolizumab en pacientes con MM o CECC en cuanto a la tasa de respuesta completa (RC), la duración de la respuesta (DR), la tasa de control de la enfermedad (TCE), la supervivencia sin progresión (SSP) utilizando los criterios RECIST, versión 1.1, evaluados por el investigador, y la supervivencia global (SG).

E.2.3

Trial contains a sub-study

E.3

Principal inclusion criteria

1. All patients must have a histologically confirmed unresectable or metastatic melanoma (Cohort 1), recurrent or metastatic squamous cell carcinoma of the head and neck (Cohort 2, primary tumor histologic diagnosis confirmation required via pathology report), or recurrent or metastatic non-small cell lung cancer (Cohort 3).
2. Cohort 1 and Cohort 2 only: patients who have not received prior immunotherapy, including checkpoint inhibitors.With the excluded prior therapies cited, patients may have received from 1 to 3 prior systemic anticancer therapies:
• In Cohort 1: Patients with unresectable or metastatic melanoma; if BRAF mutation-positive, patients may have received a BRAF inhibitor.
• In Cohort 2: Patients with unresectable or metastatic HNSCC. Those who may have received initial chemo-radiotherapy are allowed.
3. Cohort 3 only: Patients with Stage III or Stage IV NSCLC (squamous, nonsquamous, adenocarcinoma, or large cell carcinoma) who have received from 1 to 3 prior systemic anticancer therapies including checkpoint inhibitors in the locally advanced or metastatic setting.
4. Patients must have at least 1 resectable lesion of a minimum 1.5 cm in diameter postresection for TIL investigational product production. It is encouraged that tumor tissue be obtained from multiple and diverse metastatic lesions, as long as the surgical resection it does not pose additional risks to the patient.
5. Patients must have a remaining measurable disease as defined by RECIST 1.1 following tumor resection for TIL manufacturing
6. Patients must be ≥18 years and ≤70 years of age at the time of consent. Enrollment of patients >70 years of age may be allowed after consultation with the Medical Monitor.
7. Patients must have an Eastern Cooperative Oncology Group performance status of 0 or 1, and an estimated life expectancy of ≥3 months in the opinion of the Investigator.
8. Patients of childbearing potential or their partners of childbearing potential must be willing to practice an approved method of birth control during treatment and for 12 months after receiving all protocol-related therapy
9. Patients must have the following hematologic parameters:
• Absolute neutrophil count ≥1000/mm3;
• Hemoglobin ≥9.0 g/dL;
• Platelet count ≥100,000/mm3.
10. Patients must have adequate organ function:
• ALT/ SGPT and AST/SGOT ≤3 times the upper limit of normal, patients with liver metastasis ≤5 times ULN;
• An estimated creatinine clearance ≥40 mL/min using the Cockcroft Gault formula at Screening;
• Total bilirubin ≤2 mg/dL;
• Patients with Gilbert’s Syndrome must have a total bilirubin ≤3 mg/dL.
11. Patients must be seronegative for HIV. Patients with positive serology for hepatitis B virus surface antigen, hepatitis B core antibody, or hepatitis C virus indicating acute or chronic infection may be enrolled if the viral load by PCR is undetectable with/without active treatment.
12. Patients must have a washout period from prior anticancer therapy(ies) of a minimum duration, as detailed below prior to the first study treatment (ie, start of NMA LD)
• Targeted therapy: prior targeted therapy with EGFR, MEK, BRAF, ALK, ROS1 or other-targeted agents is allowed provided the washout is a minimum of 21 days prior to the start of NMA-LD;
• Chemotherapy: adjuvant, neoadjuvant or definitive chemotherapy/ chemoradiation is allowed provided the washout is a minimum of 21 days prior to the start of NMA-LD;
• Immunotherapy for Cohort 3 only, prior checkpoint-targeted therapy with an anti-PD-1, other mAbs, or vaccines are allowed with a washout period of ≥21 days before the start of NMA-LD.
• Palliative radiation therapy: prior external beam radiation is allowed provided all
radiation-related toxicities are resolved to Grade 1 or baseline;
• Surgery/pre-planned procedure: previous surgical procedure(s) is permitted provided that wound healing has occurred, all complications have resolved, and at least 14 days have elapsed (for major operative procedures) prior to the tumor resection.
13. Patients must have recovered from all prior anticancer TRAEs to Grade ≤1, except for alopecia or vitiligo, prior to cohort assignment.
• For patients in Cohort 3 only, with documented Grade 2 or higher diarrhea or colitis as a result of a previous treatment with immune checkpoint inhibitor(s), must have been asymptomatic for at least 6 months or had a normal colonoscopy post-treatment by visual assessment prior to tumor resection.
14. Patients must have provided written authorization for use and disclosure of protected health information.
15. In the opinion of the Investigator, the patient must be able to complete all study required procedures and has the ability to understand the requirements of the study. Specifically, the patient has to provide written informed consent, and has to agree to abide by the study restrictions and return to the site for required assessments.

1.Diagnóstico de melanoma irresecable o metastásico confirmado histológicamente (cohorte 1), carcinoma epidermoide de cabeza y cuello recurrente o metastásico (cohorte 2, se requerirá confirmación histológica del diagnóstico del tumor primario basada en un informe anatomopatológico) o cáncer de pulmón no microcítico recurrente o metastásico (cohorte 3)
2.Solo cohortes 1 y 2: pacientes que no hayan recibido inmunoterapia previa con inhibidores de los puntos de control inmunitarios. A excepción de los tratamientos previos antes citados, los pacientes podrán haber recibido entre 1 y 3 tratamientos antineoplásicos sistémicos previos:
cohorte 1: pacientes con melanoma irresecable o metastásico; positivos para mutación BRAF, podrán haber recibido un inhibidor de BRAF
cohorte 2: pacientes con CECC irresecable o metastásico; podrán haber recibido quimioterapia o quimiorradioterapia inicial
3.Cohorte 3: pacientes con CPNM (epidermoide, no epidermoide, adenocarcinoma, carcinoma de células grandes) en estadio III-IV que hayan recibido entre 1 y 3 líneas de tratamiento previo con antineoplásicos sistémicos, como inhibidores de los puntos de control inmunitario en el contexto localmente avanzado o metastásico
4.Presentar al menos una lesión resecable con diámetro mínimo de 1.5 cm después de la resección para la producción de LIT
5.Presentar enfermedad residual mensurable según lo definido en los criterios RECIST tras la resección tumoral para la producción de LIT
6.Pacientes >= 18 y <=70 años. Se permite inclusión de pacientes >70 años previa consulta con monitor médico
7.Estado funcional ECOG de 0 ó 1 y esperanza de vida estimada de al menos 3 meses en opinión del investigador
8.Las pacientes en edad fértil, o las parejas en edad fértil de los participantes varones, deberán estar dispuestas a utilizar un método anticonceptivo aprobado durante el tratamiento y hasta 12 meses después de que finalice todo el tratamiento del protocolo
9. Presentar los parámetros hematológicos siguientes: RAN >= 1000/mm3;Hb >=9.0 g/dl;Plaquetas>=100.000/mm3
10.Función orgánica adecuada:
ALT/SGPT y AST/SGOT <= 3 veces el LSN, en pacientes con metástasis hepáticas <= 5 veces el LSN; Aclaramiento de creatinina estimado >=40 ml/min usando la fórmula de Cockcroft Gault; Bilirrubina total <= 2 mg/dl; Los pacientes con síndrome de Gilbert deben presentar una bilirrubina total ≤ 3 mg/dl
11.Seronegativo para VIH. Los pacientes con serología positiva para HBsAg, anti-HBc o anti-VHC, indicativos de infección aguda o crónica, podrán participar en el estudio si la carga viral determinada por la RCP es indetectable con o sin tratamiento activo
12.Los pacientes deberán tener un período de lavado del tratamiento antineoplásico previo
Se permite tratamiento dirigido previo con inhibidores de EGFR, MEK, BRAF, ALK, ROS1 u otros fármacos siempre que el período de lavado sea de 21 días antes del inicio de la terapia de LD NMA. Se permite quimioterapia/quimiorradioterapia adyuvante, neoadyuvante o definitiva siempre que el período de lavado sea de 21 días antes del inicio de la terapia LD NMA. Se permite Inmunoterapia previa, en cohorte 3 solo, dirigida a los puntos de control inmunitario anti-PD-1, otros AcMs o vacunas si el período de lavado del tratamiento es >=21 días previo al inicio de la terapia LD NMA. Se permite radioterapia paliativa externa previa siempre que toda la toxicidad relacionada con la radiación se haya resuelto a un grado 1 o basal. Se permiten los procedimientos quirúrgicos previos siempre que se haya producido la cicatrización de la herida, se hayan resuelto todas las complicaciones y hayan transcurrido al menos 14 días (para los procedimientos de cirugía mayor) antes de la resección del tumor
13. Los pacientes tendrán que haberse recuperado de todos los AEs relacionados con el tratamiento antineoplásico previo hasta un grado <=1, excepto alopecia o vitíligo, antes de la asignación de la cohorte
Cohorte 3, los pacientes que presenten diarrea o colitis documentada de grado 2 o superior como resultado de un tratamiento previo con inhibidores de los puntos de control inmunitario tendrán que haberse mantenido asintomáticos desde por lo menos 6 meses antes o haber tenido una colonoscopia normal después del tratamiento en la inspección visual realizada antes de la resección del tumor
14. Los pacientes deben de haber proporcionado la autorización por escrito para el uso y divulgación de información sanitaria protegida
15. El paciente tendrá que ser capaz, en opinión del investigador, de completar todos los procedimientos exigidos por el estudio y de comprender los requisitos del estudio. Tendrá que firmar el consentimiento informado y comprometerse a respetar las restricciones del estudio y acudir al centro para las evaluaciones exigidas

E.4

Principal exclusion criteria

1. Patients with melanoma of uveal/ocular origin.
2. Patients who have received an organ allograft or prior cell transfer therapy that included a nonmyeloablative or myeloablative chemotherapy regimen. Note: this criterion is not applicable for patients undergoing retreatment with TIL LN-144/LN-145.
3. Patients with symptomatic and/or untreated brain metastases,
• Patients with definitively-treated brain metastases will be considered for enrollment after discussion with Medical Monitor; if, prior to the start of NMA-LD the patient is clinically stable for ≥2 weeks, there are no new brain lesions via magnetic resonance imaging (MRI) post-treatment, and the patient does not require corticosteroid treatment >10 mg prednisone or equivalent per day.
4. Patients who are on a systemic steroid therapy at a dose of >10 mg of prednisone or equivalent per day.
• Short course of higher-dose steroid therapy is allowed in cases of exacerbation of a known disease or for treatment of new acute symptoms not related to brain metastases.
5. Patients who are pregnant or breastfeeding.
6. Patients who have an active medical illness(es), which in the opinion of the Investigator, would pose increased risks for study participation; such as systemic infections (eg, syphilis or any other infection requiring antibiotics), coagulation disorders, or other active major medical illnesses of the cardiovascular, respiratory, or immune systems.
7. Patients may not have active or prior documented autoimmune or inflammatory disorders (including inflammatory bowel disease [eg, colitis or Crohn’s disease], diverticulitis [with the exception of diverticulosis], systemic lupus erythematosus, sarcoidosis syndrome, or Wegener syndrome [granulomatosis with polyangiitis, Graves’ disease, rheumatoid arthritis, hypophysitis, uveitis, etc.]). The following are exceptions to this criterion:
• Patients with vitiligo or alopecia;
• Patients with hypothyroidism (eg, following Hashimoto syndrome) stable on hormone replacement;
• Any chronic skin condition that does not require systemic therapy; or
• Patients with celiac disease controlled by diet alone.
8. Patients who have received a live or attenuated vaccination within 28 days prior to the start of NMA-LD.
9. Patients who have any form of primary immunodeficiency (such as severe combined immunodeficiency disease [SCID] and acquired immune deficiency syndrome [AIDS]).
10. Patients with a history of hypersensitivity to any component of the study drugs. LN-144/LN-145 should not be administered to patients with a known hypersensitivity to any component of TIL product formulation including, but not limited to:
• NMA-LD (cyclophosphamide, mesna, and fludarabine);
• Proleukin®, aldesleukin, IL-2;
• Antibiotics of the aminoglycoside group (ie, streptomycin, gentamicin);
• Any component of the TIL product formulation including dimethyl sulfoxide [DMSO], human serum albumin [HSA], IL-2, and dextran-40; or
• Pembrolizumab.
11. Patients who have a left ventricular ejection fraction (LVEF) <45% or who are New York Heart Association (NYHA) Class II or higher. A cardiac stress test demonstrating any irreversible wall movement abnormality in any patients ≥60 years of age or in patients who have a history of ischemic heart disease, chest pain, or clinically significant atrial and/or ventricular arrhythmias.
• Patients with an abnormal cardiac stress test may be enrolled if they have adequate ejection fraction and cardiology clearance with approval of the Sponsor’s Medical Monitor.
12. Patients who have obstructive or restrictive pulmonary disease and have a documented FEV1 (forced expiratory volume in 1 second) ≤60% of predicted normal.
• If a patient is not able to perform reliable spirometry due to abnormal upper airway anatomy (ie, tracheostomy), a 6-minute walk test may be used to assess pulmonary function. Patients who are unable to walk a distance of at least 80% predicted for age and sex or demonstrates evidence of hypoxia at any point during the test (SpO2 <90%) are excluded.
13. Patients who have had another primary malignancy within the previous 3 years (except for curatively treated localized malignancy that has not required treatment for greater than 1 year, and in the judgment of the Investigator, does not pose a significant risk of recurrence including, but not limited to, nonmelanoma skin cancer or bladder cancer).
14. Participation in another clinical study with an investigational product within
21 days of the initiation of NMA-LD treatment.
15. Patients protected by the following constraints:
• Hospitalized persons without consent, or persons deprived of liberty because of a judiciary or administrative decision;
• Adult persons with a legal protection measure, or persons who cannot express their consent; or
• Patients in emergency situations who cannot consent to participate in the trial.

1.Pacientes con melanoma de origen uveal u ocular
2.Pacientes que hayan recibido un aloinjerto de un órgano o una terapia previo de transferencia celular que incluyera un régimen mieloablativo o no mieloablativo de quimioterapia. Nota: este criterio no es aplicable a los pacientes que repitan el tratamiento con LIT LN-144/LN-145
3.Pacientes con metástasis cerebrales sintomáticas o no tratadas
Se considerará la inclusión de pacientes con metástasis cerebrales tratadas definitivamente previa consulta con el monitor médico. Si, antes del inicio del tratamiento de LD NMA, el paciente se mantiene clínicamente estable >=2 semanas, no aparecen nuevas lesiones cerebrales en las imágenes de la RM después del tratamiento y no precisa tratamiento con corticosteroides > 10 mg de prednisona o equivalente al día
4.Estar recibiendo esteroides sistémicos en dosis superiores a 10 mg de prednisona o equivalente al día
Se permite una tanda corta de tratamiento con esteroides en dosis altas en caso de exacerbación de una enfermedad conocida o de síntomas agudos nuevos no relacionados con metástasis cerebrales
5.Pacientes embarazadas o en periodo de lactancia
6.Presentar enfermedades activas que, en opinión del investigador, supongan un mayor riesgo para el paciente en caso de participar en el estudio, como infecciones sistémicas (como sífilis o cualquier otra infección que requiera antibióticos), trastornos de la coagulación u otras enfermedades activas importantes del aparato cardiovascular o respiratorio o del sistema inmunitario
7.Presentar trastornos autoinmunitarios o inflamatorios (como enfermedad inflamatoria intestinal [por ejemplo, colitis o enfermedad de Crohn], diverticulitis [excepción diverticulosis], lupus eritematoso sistémico, sarcoidosis o síndrome de Wegener [granulomatosis con polivasculitis, enfermedad de Graves, artritis reumatoide, hipofisitis, uveítis, etc.]) confirmados, activos o previos. Son excepciones a este criterio las siguientes: Vitíligo o alopecia, Hipotiroidismo (por ejemplo, después de un síndrome de Hashimoto) estable con tratamiento de reposición hormonal, Cualquier enfermedad crónica de la piel que no requiera tratamiento sistémico, Enfermedad celíaca controlada solo con dieta
8. Pacientes que hayan recibido vacunas de virus vivos o atenuados en los 28 días previos al comienzo de la LD-NMA
9. Presentar una inmunodeficiencia primaria de cualquier tipo (por ejemplo, inmunodeficiencia combinada grave [IDCG] o SIDA)
10. Tener antecedentes de hipersensibilidad a cualquier componente de los fármacos del estudio.No deberá administrarse LN-144/LN-145 a pacientes con hipersensibilidad conocida a cualquier componente de la formulación del producto LIT, entre otros los siguientes:
NMA-LD (ciclofosfamida, mesna y fludarabina);
Proleukin®, aldesleukina, IL-2, Antibióticos del grupo de los aminoglucósidos (pej: estreptomicina, gentamicina).
Cualquier componente de la formulación del producto LIT: DMSO, albúmina sérica humana, IL-2 y dextrano-40;
Pembrolizumab
11. Tener una FEVI < 45% o pertenencia a la clase funcional II o superior de la NYHA. Una prueba de esfuerzo cardiaco en la que se demuestre una anomalía irreversible del movimiento de la pared en cualquier paciente de >= 60 años de edad o pacientes con antecedentes de cardiopatía isquémica, dolor torácico o arritmias auriculares o ventriculares clínicamente importantes
Se podrá incluir a pacientes con alguna anomalía en la prueba de esfuerzo cardíaco si presentan una FEVI adecuada y obtienen la autorización de cardiología y la aprobación del monitor médico del promotor
12. Presentar una enfermedad pulmonar obstructiva o restrictiva con un FEV1 documentado <= 60% del valor previsto normal
Si un paciente no puede realizar una espirometría fiable debido a una anatomía anormal de las vías respiratorias superiores, se podrá realizar una prueba de marcha durante 6 minutos para evaluar la función pulmonar. Se excluirá a los pacientes que no puedan recorrer al menos el 80% de la distancia prevista para la edad y el sexo o presenten signos de hipoxia en algún momento durante la prueba (SpO2 < 90%)
13. Haber tenido otra neoplasia maligna primaria en los 3 años anteriores (excepto una neoplasia maligna localizada que haya recibido tratamiento curativo, pero que no haya requerido tratamiento durante más de 1 año y que, a criterio del investigador, no tenga un riesgo importante de recurrencia, como un cáncer de piel distinto del melanoma o un cáncer de vejiga)
14. Haber participado en otro estudio clínico con un producto en investigación en los 21 días previos al inicio del tratamiento de la LD-NMA)
15. Personas hospitalizadas sin consentimiento, privadas de libertad por decisión judicial o administrativa. Personas adultas afectadas por una medida de protección legal o personas que no puedan expresar su consentimiento o
Personas en situaciones de emergencia que no puedan otorgar su consentimiento en el ensayo

E.5 End points

E.5.1

Primary end point(s)

The ORR is defined as the proportion of patients who achieve either a confirmed PR or CR as best response as assessed by Investigators per RECIST 1.1 among the AT population. Objective response will be evaluated per each disease assessment and the ORR will be expressed as a binomial proportion with the corresponding 2-sided 90% CI. The safety primary endpoint will be measured by any Grade 3 or higher TEAE incidence rate within each cohort expressed as binomial proportions with the corresponding 2-sided 90% CI.

El criterio de valoración principal de la eficacia en todas las cohortes será la TRO, evaluada por el investigador, y los pacientes que cumplan los criterios de RC o RP según los RECIST, versión 1.1, se clasificarán como pacientes con respuesta. La TRO, la incidencia de AAAT de grado 3 o superior, la tasa de RC y la TCE se resumirán mediante estimaciones puntuales y límites de confianza del 90% bilaterales.

E.5.1.1

Timepoint(s) of evaluation of this end point

The primary analysis for each cohort will occur when all treated patients per Cohort have an opportunity to be followed for 12 months, progressed/expired, or terminated early from the post-treatment follow-up.

El análisis principal de cada cohorte se realizará cuando todos los pacientes tratados por cohorte hayan tenido la oportunidad de ser seguidos durante 12 meses, hayan progresado o fallecido o retirados prematuramente del seguimiento post tratamiento.

E.5.2

Secondary end point(s)

Efficacy:
The secondary efficacy endpoints are defined as follows:
- CR rate is based on responders who achieved confirmed CR as assessed by Investigators. DCR is derived as the sum of the number of patients who achieved confirmed PR/CR or sustained SD (at least 6 weeks) divided by the number of patients in the efficacy analysis set × 100%. The CR rate and DCR will be summarized using a point estimate and its 2-sided 90% CI.
- DOR is defined among patients who achieved objective response. It is measured from the first-time response (PR/CR) criteria are met until the first date that recurrent or progressive disease is objectively documented, or receipt of subsequent anticancer therapy or the patient dies (whichever is first recorded). Patients not experiencing PD or have not died prior to the time of data cut or the final database lock will have their event times censored on the last date that an adequate assessment of tumor status is made.
- PFS is defined as the time (in months) from the time of lymphodepletion to PD, or death due to any cause, whichever event is earlier. Patients not experiencing PD or not having expired at the time of the data cut or the final database lock will have their event times censored on the last date that an adequate assessment of tumor status is made.
- OS is defined as the time (in months) from the time of lymphodepletion to death due to any cause. Patients not having expired by the time of data cut or the final database lock will have their event times censored on the last date of their known survival status.
- DOR, PFS, and OS will be subjected to right censoring. The Kaplan-Meier method will be used to summarize the time-to-event efficacy endpoints. The baseline data for the tumor assessment is the last scan before the lymphodepletion for all cohorts.

The above efficacy parameters will be estimated for applicable cohort for subsets defined by
baseline disease characteristics; BRAF status (Cohort 1 only), HPV status (Cohort 2 only),
squamous or non-squamous lung disease (Cohort 3 only), and anti-PD-L1 status.

Safety:

All AEs occurring after the patient has consented, but prior to tumor resection or the first study treatment dose, will be collected on the medical history eCRF unless the event is new and attributed to protocol-mandated procedures and assessments. All AEs occurring on or after tumor resection and after first study treatment dose in the study and either observed by the Investigator or reported by the patient (whether attributed to the use of lymphodepletion drugs, TIL LN-144/ LN-145, IL-2, or pembrolizumab or not) must be reported on the AE eCRF.
Safety collection of AEs will continue until completion of the assessment period. OS data will be collected until each patient’s EOS = death, lost to follow-up, withdrawal of consent, study termination by Sponsor, or 5 years (Month 60), whichever occurs first. AEs that occur after the response and follow-up period with a reasonable possibility that the event may have been caused by the study treatment may be reported at the Investigator’s discretion.
All AEs attributed to protocol-required procedures or treatment will be collected from the time of signing of the ICF through completion of the assessment period.
For safety, the commonly observed TEAEs will be summarized descriptively by cohort in comparison to historical data of TIL LN-144/LN-145 or pembrolizumab alone as single agents. Other safety parameters will include TEAEs by grade, SAEs, AEs leading to discontinuations, vital signs, physical examinations, and toxicity from clinical laboratory results.
Prevalence of AEs beyond the treatment-emergent period will be summarized separately. AE summaries will be based on patient incidence counts and percentages per the safety analysis set. In addition to the overall summary of AEs, breakdown summaries will be made by NCI-CTCAE grade of severity, seriousness, and relationship to the study treatment. All laboratory results will be summarized using descriptive statistics. Other safety parameters will include TEAEs by grade, SAEs, AEs leading to discontinuations, vital signs, physical examinations, and toxicity from clinical laboratory results.
Prevalence of AEs beyond the treatment-emergent period will be summarized separately. AE summaries will be based on patient incidence counts and percentages per the safety analysis set.
In addition to the overall summary of AEs, breakdown summaries will be made by NCI-CTCAE grade of severity, seriousness, and relationship to the study treatment. All laboratory results will be summarized using descriptive statistics.

Eficacia:
Los criterios de evaluación secundarios de eficacia son:
La tasa de respuesta completa (RC) está basada en los pacientes que hayan alcanzado una RC evaluada por los investigadores. La tasa de control de la enfermedad (TCE) se deriva de la suma del número de pacientes que alcancen una RP/RC confirmada o una duración de respuesta (DR) mantenida (al menos 6 semanas) divido por el número de pacientes en el grupo de análisis de eficacia x 100%.
La relación entre RC y TCE se resumirá mediante estimaciones puntuales y límites de confianza del 90% bilaterales.
Los análisis de la DR se realizarán en los pacientes que logren una respuesta objetiva. Se medirá desde que se alcancen los criterios de primera respuesta (RP/RC) hasta la primera fecha en la que se documente la recidiva o progresión de la enfermedad objetivamente, o se inicia un nuevo tratamiento antineoplásico o el paciente fallezca (lo que ocurra antes). Los pacientes que no hayan experimentado una progresión de enfermedad o no hayan muerto antes del corte de datos o cierre de la base de datos tendrán censurados sus eventos en la última fecha en la que se les haya realizado una evaluación tumoral adecuada.
La SG se define como el tiempo (en meses) desde la linfodepleción hasta la muerte por cualquier causa. Los pacientes que no hayan fallecido en el momento del corte de datos o cierre de la base de datos tendrán censurados sus eventos en la última fecha de supervivencia conocida.
La DR, SSP y SG están sujetas a censura. El método Kaplan-Meier se utilizará para resumir los criterios de valoración de la eficacia basados en el tiempo hasta el episodio. El dato basal para la evaluación tumoral es el último TAC antes de la linfodepleción para todas las cohortes.
Los parámetros de eficacia detallados arriba serán evaluados para cada cohorte para los subtipos definidos por las características de la enfermedad basal, positividad para BRAF (cohorte 1), VPH (cohorte 2), enfermedad de pulmón epidermoide o no epidermoide (cohorte 3), y estado de anti-PD-L1.
Evaluar más a fondo la eficacia de los LIT autólogos LN-144y LN-145 en monoterapia o en combinación con pembrolizumab en pacientes con MM o CECC en cuanto a la tasa de respuesta completa (RC), la duración de la respuesta (DR), la tasa de control de la enfermedad (TCE), la supervivencia sin progresión (SSP) utilizando los criterios RECIST, versión 1.1, evaluados por el investigador, y la supervivencia global (SG).
Seguridad:
Todos los AA que se produzcan después de que el paciente haya otorgado su consentimiento, pero antes de la resección tumoral, se registrarán en la página de antecedentes médicos del cuaderno de recogida de datos electrónico (CRDe), salvo que el acontecimiento sea nuevo y se atribuya a los procedimientos y las evaluaciones requeridos en el protocolo. Todos los AA que se produzcan en o después de la resección tumoral y después de la primera visita de tratamiento del estudio y se observen por el investigador o se reporten por el paciente (bien sean atribuibles al uso de medicamentos linfodepletores, TIL LN-144/LN-145, IL-2, prembrolizumab o no) deberán ser registrados en los AA del CRDe.
El registro de seguridad de AA continuará hasta la finalización del período de evaluación. Los datos de SG se recogerán hasta FDE = muerte, pérdida para el seguimiento, retirada del consentimiento, finalización del estudio por el promotor o 5 años (mes 60), lo que ocurra antes. Todos los AA que ocurran después de la respuesta y el período de seguimiento con una posibilidad razonable de que el evento haya sido causado por el tratamiento del estudio se reportará de acuerdo a la opinión del investigador. Se registrarán los AA de cualquier atribución desde el momento de la firma del DCI hasta la finalización del período de evaluación.
Para la seguridad, se resumirán descriptivamente los AAAT observados con frecuencia en cada cohorte en comparación con los datos históricos del tratamiento con LIT LN 144 o LN 145 o pembrolizumab en monoterapia. Otros parámetros de seguridad serán los AAAT según el grado, los AAG, los AA que motiven la suspensión de los tratamientos del estudio, las constantes vitales, las exploraciones físicas y los datos de toxicidad deducida a partir de los resultados de los análisis clínicos.
La prevalencia de AA tras el período de tratamiento se resumirá por separado. El resumen de AA se basará en la cuenta de la incidencia de pacientes por grupo de análisis de la seguridad. Además del recuento global de AA, se realizará un desglose por el grado NCI-CTCAE de intensidad, gravedad y relación con el tratamiento de estudio. Todos los resultados de laboratorio se resumirán utilizando estadística descriptiva. Otros parámetros de seguridad serán los AAAT según el grado, los AAG, los AA que motiven la suspensión de los tratamientos del estudio, las constantes vitales, las exploraciones físicas y los datos de toxicidad deducida a partir de los resultados de los análisis clínicos.

E.5.2.1

Timepoint(s) of evaluation of this end point

The timepoint for the secondary endpoint evaluation will occur when all treated patients per Cohort have an opportunity to be followed for 12 months, progressed/expired, or terminated early from the post-treatment follow-up.

El punto de evaluación del objetivo secundario del estudio será cuando todos los pacientes tratados en cada cohorte hayan tenido la oportunidad de ser seguidos durante 12 meses, hayan progresado/fallecido o se hayan retirado prematuramente del seguimiento post tratamiento.

E.6 and E.7 Scope of the trial

E.6

Scope of the trial

E.6.1

Diagnosis

E.6.2

Prophylaxis

E.6.3

Therapy

Yes

E.6.4

Safety

Yes

E.6.5

Efficacy

Yes

E.6.6

Pharmacokinetic

E.6.7

Pharmacodynamic

E.6.8

Bioequivalence

E.6.9

Dose response

E.6.10

Pharmacogenetic

E.6.11

Pharmacogenomic

E.6.12

Pharmacoeconomic

E.6.13

Others

E.7

Trial type and phase

E.7.1

Human pharmacology (Phase I)

E.7.1.1

First administration to humans

E.7.1.2

Bioequivalence study

E.7.1.3

Other

E.7.1.3.1

Other trial type description

E.7.2

Therapeutic exploratory (Phase II)

Yes

E.7.3

Therapeutic confirmatory (Phase III)

E.7.4

Therapeutic use (Phase IV)

E.8 Design of the trial

E.8.1

Controlled

E.8.1.1

Randomised

E.8.1.2

Open

Yes

E.8.1.3

Single blind

E.8.1.4

Double blind

E.8.1.5

Parallel group

E.8.1.6

Cross over

E.8.1.7

Other

E.8.2

Comparator of controlled trial

E.8.2.1

Other medicinal product(s)

E.8.2.2

Placebo

E.8.2.3

Other

E.8.2.4

Number of treatment arms in the trial

E.8.3

The trial involves single site in the Member State concerned

E.8.4

The trial involves multiple sites in the Member State concerned

Yes

E.8.4.1

Number of sites anticipated in Member State concerned

E.8.5

The trial involves multiple Member States

Yes

E.8.5.1

Number of sites anticipated in the EEA

E.8.6 Trial involving sites outside the EEA

E.8.6.1

Trial being conducted both within and outside the EEA

Yes

E.8.6.2

Trial being conducted completely outside of the EEA

E.8.6.3

If E.8.6.1 or E.8.6.2 are Yes, specify the regions in which trial sites are planned

Canada

France

Spain

Switzerland

United Kingdom

United States

E.8.7

Trial has a data monitoring committee

Yes

E.8.8

Definition of the end of the trial and justification where it is not the last visit of the last subject undergoing the trial

The study is expected to be completed approx. 5 years after the last patient receives their last dose of IL-2, or the study is terminated at Iovance’s discretion, whichever occurs first. The intent is that all patients in the efficacy analysis set will be followed-up for 5 years after their last respective doses of IL-2.
In addition a patient may reach EOS status for any of the following reasons, Death, Lost to follow-up, Withdrawal of consent.

La participación en el estudio durará un máximo de 5 años después de que el último paciente reciba su última dosis de IL-2, se cancele el estudio por Iovance, lo que ocurra antes. La intención es que todos los pacientes del grupo de análisis de eficacia sean seguidos durante 5 años después de su respectiva última dosis de IL-2.
Además, un paciente puede alcanzar el estado de fin de estudio por una de las siguientes razones, Muerte, Pérdida para el seguimiento, Retirada del consentimiento.

E.8.9 Initial estimate of the duration of the trial

E.8.9.1

In the Member State concerned years

E.8.9.1

In the Member State concerned months

E.8.9.1

In the Member State concerned days

E.8.9.2

In all countries concerned by the trial years

E.8.9.2

In all countries concerned by the trial months

E.8.9.2

In all countries concerned by the trial days

F. Population of Trial Subjects

F.1 Age Range

F.1.1

Trial has subjects under 18

F.1.1.1

In Utero

F.1.1.2

Preterm newborn infants (up to gestational age < 37 weeks)

F.1.1.3

Newborns (0-27 days)

F.1.1.4

Infants and toddlers (28 days-23 months)

F.1.1.5

Children (2-11years)

F.1.1.6

Adolescents (12-17 years)

F.1.2

Adults (18-64 years)

Yes

F.1.2.1

Number of subjects for this age range:

F.1.3

Elderly (>=65 years)

Yes

F.1.3.1

Number of subjects for this age range:

F.2 Gender

F.2.1

Female

Yes

F.2.2

Male

Yes

F.3 Group of trial subjects

F.3.1

Healthy volunteers

F.3.2

Patients

Yes

F.3.3

Specific vulnerable populations

Yes

F.3.3.1

Women of childbearing potential not using contraception

F.3.3.2

Women of child-bearing potential using contraception

Yes

F.3.3.3

Pregnant women

F.3.3.4

Nursing women

F.3.3.5

Emergency situation

F.3.3.6

Subjects incapable of giving consent personally

F.3.3.7

Others

F.4 Planned number of subjects to be included

F.4.1

In the member state

F.4.2

For a multinational trial

F.4.2.1

In the EEA

F.4.2.2

In the whole clinical trial

F.5

Plans for treatment or care after the subject has ended the participation in the trial (if it is different from the expected normal treatment of that condition)

None - Patients will be treated according to the standard of care in their respective country.

Ninguno - Los pacientes serán tratados de acuerdo a las prácticas habituales en cada país.

G. Investigator Networks to be involved in the Trial

N. Review by the Competent Authority or Ethics Committee in the country concerned

Competent Authority Decision

Authorised

Date of Competent Authority Decision

2018-11-30

Ethics Committee Opinion of the trial application

Favourable

Ethics Committee Opinion: Reason(s) for unfavourable opinion

Date of Ethics Committee Opinion

2018-10-25

P. End of Trial
P.	End of Trial Status	Ongoing

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IMP with orphan designation in the indication
Orphan Designation Number:
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