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Joseph Gordon
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Eligible for taxane monotherapy (i.e., absence of rapid clinical progression, life-threatening visceral metastases, or the need for rapid symptom and/or disease control)

Visceral crisis or lymphangitic spread\r\n* NOTE: Visceral crisis is not the mere presence of visceral metastases, but implies severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of disease

EXCLUSION CRITERIA FOR SECOND-LINE THERAPY: Life-threatening visceral disease or other severe concurrent disease

EXCLUSION CRITERIA FOR THIRD-LINE THERAPY: Life-threatening visceral disease or other severe concurrent disease

Visceral crisis or impending visceral crisis at time of screening

Subjects with bulky visceral disease defined as > 4 cm

Symptomatic or rapid visceral progression

Patients with active visceral, central nervous system, or any bone metastases melanoma (stage IVM1b or IVM1c)

Life-threatening visceral disease or other severe concurrent disease

Evidence of visceral metastasis to the liver.

have impending visceral crisis that requires chemotherapy;

Patients who have any liver metastases or visceral metastasis of ? 3 cm, plus evidence of progression meeting irRC 1.0 within 1 month before the first OBP-301 administration.

Patients who have noncanonical DNA repair defects and extensive visceral disease or symptomatic bone disease requiring urgent tumor response

Identified as having visceral crisis, lymphangitic spread, or leptomeningeal carcinomatosis; visceral crisis is not the mere presence of visceral metastases but implies severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of the disease

Requires urgent treatment with cytotoxic chemotherapy or other therapy is indicated (e.g., symptomatic visceral metastases)

Patients with parahepatic extension of disease with direct non-liver visceral involvement

No visceral crisis: Visceral crisis is moderate-to severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of disease

Development of visceral crisis since pre-registration.\r\n* NOTE: Visceral crisis is moderate-to-severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of disease.

Patients with definite liver metastasis > 1 cm or signs of visceral crisis or impending visceral crisis at the clinical discretion of the treating physician

Subjects with retroperitoneal and visceral sarcoma

Visceral crisis or rapidly progressive disease for which chemotherapy would be indicated

Symptomatic visceral KS (except for non-ulcerating disease restricted to the oral cavity)

Life-threatening visceral disease or other severe concurrent disease

Symptomatic liver or visceral organ metastasis

Life-threatening visceral disease or other severe concurrent disease

Evidence of liver metastases or visceral disease

Life-threatening visceral disease or other severe concurrent disease

Life-threatening, visceral metastases

Visceral metastases (e.g. lung, liver, brain, kidney, spleen)

Patients must be classified as having intermediate or poor-risk germ cell tumor, as follows:\r\n* Intermediate-risk (modified*)\r\n** Testis or retroperitoneal primary non-seminomatous germ cell tumors (NSGCT) with lymph node and/or lung metastasis but without non-pulmonary visceral metastasis AND any of the following pretreatment serum tumor marker (STM) values:\r\n*** Lactate dehydrogenase (LDH) from 3 to < 10 x upper limit of normal (ULN) (*this differs from the original International Germ Cell Cancer Collaborative Group [IGCCCG] criteria which includes patients with LDH from 1.5 to 10 x ULN)\r\n*** Serum human chorionic gonadotrophin (HCG) from 5,000 to < 50,000 MIU/mL\r\n*** Serum alpha-fetoprotein (AFP) from 1,000 to < 10,000 ng/mL\r\n** Seminoma histology regardless the primary site or serum tumor markers with any non-pulmonary visceral metastasis (liver, bone, brain, etc)\r\n* Poor-risk (any of the following):\r\n** Testis or retroperitoneal NSGCT primary with non-pulmonary visceral metastasis (liver, bone, brain, etc) regardless the STM values\r\n** Mediastinal NSGCT primary site of disease regardless the presence/absence of visceral metastasis or STM values\r\n** Testis or retroperitoneal NSGCT primary without non-pulmonary visceral metastasis but with poor-risk STM values:\r\n*** LDH >= 10 x ULN\r\n*** HCG >= 50,000 MIU/mL\r\n*** AFP >= 10,000 ng/mL

Visceral metastasis (excluding liver metastases) and/or lymphadenopathy

Presence of skeletal, and/or soft-tissue/visceral/nodal metastasis

have visceral crisis

No current evidence of visceral crisis or lymphangitic spread

No visceral crisis, lymphangitic spread or known brain metastases: visceral crisis is not the mere presence of visceral metastases, but implies severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of disease

Patients with immediately life-threatening visceral disease, for whom chemotherapy is the preferred treatment option.

Visceral (ie, liver or lung) metastases as only sites of metastases

Contraindications to angiography and selective visceral catheterization

Presence of unstable systemic disease (e.g., visceral crisis or rapid progression) in the judgment of the investigator

Have visceral crisis, lymphangitic spread, or leptomeningeal carcinomatosis

Patients with extensive advanced/metastatic, symptomatic visceral disease, or known uncontrolled or symptomatic CNS metastases

Pending visceral crisis, in the opinion of the treating investigator

Visceral (eg, lung, liver) metastatic disease. Adenopathy is allowed;

Has rapid progression of visceral disease and, thus is a candidate for docetaxel; this determination will be at the discretion of the treating physician

A visceral metastasis greater than 8 cm

A visceral metastasis that due to its location cannot be safely treated with SABR

Have visceral crisis, lymphangitic spread, or leptomeningeal carcinomatosis visceral crisis is not the mere presence of visceral metastases but implies severe organ dysfunction as assessed by symptoms and signs, laboratory studies, and rapid progression of the disease

History of visceral metastasis, or presence of visceral metastasis detected by screening imaging examinations

History of visceral metastasis, or visceral metastases

History of visceral metastasis, or visceral metastases

COHORT B: Visceral metastatic disease

Patients experiencing a visceral crisis including severe organ dysfunction as assessed by > grade (Gr) 2 symptomatic toxicities, laboratory studies, and/or rapid progression of disease originating from visceral metastasis

Symptomatic liver or visceral organ metastasis

Contraindications to angiography and selective visceral arterial catheterization

Patients with rapidly progressive or extensive symptomatic visceral metastatic disease

Pending visceral crisis, in the opinion of the treating investigator

Life-threatening visceral disease or other severe concurrent disease

Life-threatening visceral disease or other severe concurrent disease

Patients who require or may be expected to require urgent treatment with docetaxel during the study (e.g., patients with visceral metastases).

Presence of >= 1 metastatic site (nodal, visceral) that is amenable to core biopsy

Contraindications to angiography or selective visceral catheterization

Life-threatening visceral disease or other severe concurrent disease

Patients with visceral disease are ineligible

Patients in whom urgent treatment with docetaxel is indicated, per clinician discretion; this includes, but is not limited to patients with symptomatic visceral metastatic disease

Patients with paraspinal extension of disease with visceral involvement

Presence or history of visceral melanoma metastasis

Eligible for taxane monotherapy, as per local investigator assessment (e.g., absence of rapid clinical progression, life-threatening visceral metastases, or the need for rapid symptom and/or disease control which may require combination chemotherapy)

Life-threatening, visceral metastases

Cohort A: Patients must have at least one measurable visceral lesion (per RECIST 1.1); a visceral lesion is any solid organ except for skin, lymph node, and musculoskeletal tissue; at least one of these visceral lesions must be measurable per RECIST 1.1

Cohort B: Patients must not have any visceral lesions

Patients with immediately life-threatening visceral disease for whom chemotherapy is preferred treatment option.

Patients with metastatic castration resistant prostate carcinoma with skeletal, visceral and/or nodal involvement

AIM 3: Patients with either cutaneous, visceral or brain melanoma metastases

Visceral (e.g. lung, liver) metastases