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Targeting Ischemia-Induced Autophagy Dependence in Hepatocellular Carcinoma

Phase 1
Not yet recruiting
Conditions
Hepatocellular Carcinoma
Interventions
Drug: Placebo
Registration Number
NCT05842174
Lead Sponsor
VA Office of Research and Development
Brief Summary

Trans-arterial chemoembolization (TACE) is the most commonly used therapy for patients with unresectable hepatocellular carcinoma (HCC). TACE is a minimally invasive procedure that involves placing a catheter into the artery in the liver that feeds the tumor, administering chemotherapeutics and then blocking the artery with embolics in order to kill tumor cells by depriving them of essential oxygen and nutrients. While TACE has a proven survival benefit, local recurrence is common, and long-term survival rates are poor. Prior studies demonstrate that HCC cells survive the oxygen and nutrient deprivation through autophagy, a process of cellular self-eating, to provide nutrients required for survival. The proposed project will leverage this dependency to develop a novel approach to TACE that integrates autophagy inhibition to improve therapeutic response by increasing tumor cell killing and enhancing anti-tumor immunity.

Detailed Description

Surgical resection or liver transplantation remain the only curative options for patients with hepatocellular carcinoma (HCC). However, fewer than 20% of patients with HCC are candidates for resection. Transarterial embolization with or without chemotherapy (TA(C)E) is an endovascular locoregional embolotherapy that involves hepatic artery embolization with intra-arterial infusion of a chemotherapeutic agent. TA(C)E is considered the standard of care for treating unresectable HCC in the remaining 80% of patients. While TA(C)E has a proven survival benefit, local recurrence is common, and long-term survival rates are poor. Moreover, only 44% of treated HCCs demonstrate extensive necrosis on pathology following TA(C)E, indicating tumor cells develop an adaptive metabolic stress response (MSR) enabling their survival under TA(C)E-induced nutrient and oxygen deprivation.

In preliminary studies, the investigators have demonstrated that HCC cells are pre-programmed to survive TA(C)E-induced ischemia through enhanced function of autophagy. Moreover, TA(C)E-induced ischemia results in quiescence in surviving HCC cells and a dependence on autophagy. As such, these data demonstrate that TA(C)E offers a unique opportunity to constrain metabolic phenotypes in order to generate this targetable dependency in HCC. The proposed project will build on this prior work to: 1) study a novel TA(C)E paradigm which targets this ischemia-induced dependency on autophagy using hydroxychloroquine (HCQ) and 2) characterizes the efficacy and evolution of autophagy inhibition using HCQ as well as associated alterations in anti-tumor immunity. To achieve these goals, this submission proposes a first in human, early phase prospective clinical trial to assess the safety and efficacy of autophagy inhibition using intra-arterial (IA) HCQ with TAE followed by maintenance of autophagy inhibition with daily oral HCQ for 6 weeks following embolization. Follow-up tumor biopsies and serum sampling 3-4 and 5-6 weeks after embolization will inform on the on-target efficacy of autophagy inhibition and its effect on the tumor microenvironment and immune response.

This trial will pursue three aims: (1) to establish the clinical safety of the combination of the autophagy inhibitor HCQ with TAE to treat patients with intermediate stage HCC (phase 1); (2) to compare the short-term efficacy of HCQ with TAE versus TAE alone in patients with intermediate stage HCC (phase 2); and (3) to characterize differences in local and systemic immune modulation following TAE as compared to IA HCQ TAE.

Recruitment & Eligibility

Status
NOT_YET_RECRUITING
Sex
All
Target Recruitment
93
Inclusion Criteria
  • Male or female, aged 18 years, meeting criteria for diagnosis of BCLC B HCC and referred to undergo TACE
  • HCC measuring 3 cm in minimum transverse diameter and meets LI-RADS 5 criteria based on cross-sectional imaging as determined by a board-certified, sub-specialty trained radiologist
  • Childs Pugh Turcotte A/B7, Performance Status 0
  • Informed of investigational nature of this study with provision of signed and dated informed consent form
  • Stated willingness to comply with all study procedures and availability for the duration of the study
Exclusion Criteria

  • QT prolongation on ECG

  • Retinopathy on ophthalmologic examination

  • Females who are pregnant or breast feeding at the time of screening will not be eligible for this study

    • a serum or urine pregnancy test will be performed in women of child-bearing potential at screening

  • Prior LRT or systemic therapy to the target lesion

  • Contraindication to contrast enhanced MRI or metallic implant within the liver.

  • HCQ allergy, porphyria, uncontrolled psoriasis, and existing retinopathy

  • Lesion not amenable to biopsy based on pre-TACE imaging as determined by treating interventional radiologist

  • Serious or unstable medical or psychological conditions that, in the opinion of the investigator, would compromise the subject's safety or successful participation in the study)

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Transarterial Embolization without HydroxychloquineLipiodolIntra-arterial Lipiodol + transarterial embolization followed by oral placebo
Transarterial Embolization without HydroxychloquinePlaceboIntra-arterial Lipiodol + transarterial embolization followed by oral placebo
Transarterial Embolization with HydroxychloroquineHydroxychloroquineIntra-arterial hydroxychloroquine in Lipiodol + transarterial embolization followed by oral hydroxychloroquine
Transarterial Embolization with HydroxychloroquineLipiodolIntra-arterial hydroxychloroquine in Lipiodol + transarterial embolization followed by oral hydroxychloroquine
Primary Outcome Measures
NameTimeMethod
Local Progression Free Survival6 months following treatment

Local progression free survival will be determined on a per lesion basis based on follow-up cross-sectional imaging and modified response evaluation criteria in solid tumors

Secondary Outcome Measures
NameTimeMethod

Trial Locations

Locations (1)

Corporal Michael J. Crescenz VA Medical Center, Philadelphia, PA

🇺🇸

Philadelphia, Pennsylvania, United States

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