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Trial Title:
Prospective Clinical Validation of Next Generation Sequencing (NGS) and Patient-Derived Tumor Organoids (PDO) Guided Therapy in Patients With Advanced/ Inoperable Solid Tumors
NCT ID:
NCT06077591
Condition:
Hepatocellular Carcinoma
Colorectal Cancer
Conditions: Official terms:
Carcinoma, Hepatocellular
Study type:
Interventional
Study phase:
N/A
Overall status:
Not yet recruiting
Study design:
Allocation:
N/A
Intervention model:
Single Group Assignment
Intervention model description:
Intervention in this study is to perform tissue sampling to patient's tumor which are
then subjected to DNA extraction for whole exome sequencing, organoid culture, and drug
screen. An MDT board will review the drug screen results and excluded drug choice of poor
response. Then the referring oncologist has the final discretion on the choice of chemo-
or targeted agent as usual.
Primary purpose:
Treatment
Masking:
None (Open Label)
Intervention:
Intervention type:
Other
Intervention name:
Patient-Derived Tumor Organoids
Description:
Intervention in this study is to perform tissue sampling to patient's tumor which are
then subjected to DNA extraction for whole exome sequencing, organoid culture, and drug
screen. An MDT board will review the drug screen results and excluded drug choice of poor
response. Then the referring oncologist has the final discretion on the choice of chemo-
or targeted agent as usual.
Arm group label:
Patient-Derived Tumor Organoids (PDO) Guided Therapy
Summary:
Precision oncology aims to improve clinical outcome of patients by offering personalized
treatment through identifying druggable genomic aberrations within their tumors. This is
particularly valid when it comes to offering alternative treatment options for patients
with advanced tumors that are chemo-refractory. Patient-derived organoids (PDOs) are 3
dimensional tumoroids that can be expanded ex vivo and are both pheno- and genotypically
identical to patients' tumors. Observational studies have shown that PDO-based drug
screens can predict treatment response with high sensitivity and specificity.
Vlachogiannis G. reported a living biobank of patient-derived organoids (PDOs) from
patients with advanced GI cancers enrolled in clinical trials. PDOs can recapitulate
patients' clinical response to chemotherapeutic agents. In 19 tumor organoids, the group
performed molecular profiling and drug screens and then compared ex vivo organoid
responses to anticancer drugs. Drug response to PDO based orthotopic mouse tumor
xenografts correlated to the drug response of the patient in clinical trials. Further to
the study, there were other retrospective validation studies utilizing PDOs from patients
enrolled in clinical trials such as the TUMOROID, CinClare to predict clinical response.
Ooft studied PDOs from patients with metastatic colorectal cancers enrolled in the
TUMOROID study to predict response to irinotecan-based therapies. Yao generated a
organoid biobank of 80 locally advanced rectal cancers. These patients were derived from
a phase III study (CinClare) that compared neoadjuvant chemo-radiation using either
capecitabine or CAPIRI. Response to chemoradiation in patients matched to that of rectal
cancer organoids (sensitivity 78% and specificity 91.9%). In a systematic analysis of 17
studies (9 on advanced GI and pancreatic cancers, one on renal cell cancer and others on
miscellaneous cancers), the pooled sensitivity and specificity for discriminating
patients with a clinical response through PDO-based drug screen was 0.81 (95%CI
0.69-0.89) and 0.74 (95%CI 0.64-0.82) respectively. Within 4-6 weeks, PDO-based drug
screen creates a true personalised platform by predicting patient-specific drug response
with high accuracy. Recent technical advancements in growing these PDO 'avatars' from
biopsies have made it possible to test suitable anticancer drugs in patients with
advanced inoperable tumors, and explore the new possibilities for treatment options that
otherwise would be missed by standard conventional therapies. In 2019, our group embarked
on PDO research; investigators obtained tissues from patients with advanced/ inoperable
solid tumors, and performing drug screens on these PDOs ex vivo. In several patients,
investigators were able to identified drugs not otherwise used through sequencing data,
and observed remarkable clinical response in patients with PDO responsive tumors.
Investigators illustrate with cases that underwent PDO culture and drug screens. [ See
appendix ] In the literature, the clinical utility of treatment based on PDO informed
drug options has however not been fully established. Investigators therefore propose a
phase 2 proof-of-concept clinical trial to evaluate efficacy of NGS/ PDO guided treatment
in patients with inoperable or metastatic solid tumors..
Detailed description:
Under informed consents, patients undergo tissue sampling (radiologic, endoscopic or
surgical excision). DNA is extracted from tissue and sent for whole-exome sequencing
(WES), organoid culture and drug testing. DNA mutations in PDO models will be determined
using whole-exome sequencing (WES). Mutational burden and driver genes profile will be
assessed for similarities to those identified in primary cancers. The genetic data
generated will be interpreted for response to FDA-approved molecular targeting drugs.
Investigators would study PDO cultures resistant to available chemotherapeutic options.
They would be of exceptional value to study sensitivity to targeted agents, providing
alternative treatment options for chemo-refractory diseases. Based on past experience,
project team has developed a Standard Operational Protocol (SOP) in the area and
establish pipeline in integrative analysis with genome data. PDO Culture and
Genome-guided Drug Screen.To ensure clinical usefulness of our platform, investigators
aim to deliver drug options of each PDO within a meaningful timeframe. In this framework
of typically 4-6 weeks, investigators shall generate organoids, study their molecular
profile and undertake ex vivo drug screening that would allow us to individualize therapy
for each patient. Eligible patients are seen in an MDT board where patients' case
history, laboratory and radiologic results are reviewed. With informed consent to trial
participation, the patient undergoes tissue sampling to his tumor (by radiologic,
endoscopic, or surgical methods). Sampled tumors are then subjected to DNA extraction for
whole exome sequencing, organoid culture, and drug screen. This takes between 2- 4 weeks.
In the interim period, the patient is allowed to receive a chemotherapy agent, a target
agent or hormone therapy between the time of the biopsy and the availability of drug
screen results. An MDT will review the drug screen results and recommend the use of a
drug with a response in a PDO. When several drugs are shown to be efficacious, the
referring oncologist has the final discretion on the choice of chemo- or targeted agent.
Tumor assessments will be performed at baseline, every 8 weeks. Investigators report all
adverse events and serious adverse events (SAE) based on the definitions in NCI CTCAE.
Investigators report all SAEs to the Joint NTEC-CUHK CREC within 24 hours of their
occurrence. Senior physicians at CREC adjudicated all SAEs.
Investigators aim to determine clinical efficacy of NGS/ PDO drug screen guided treatment
in patients with inoperable/ advanced solid tumors refractory to conventional
chemotherapy. Investigators correlate PDO drug response ex vivo to clinical response in
these patients. Our hypothesis is that WES and PDO drug screen can accurately identify
candidate drugs that will reduce tumor size and confer benefits in these patients.
Investigators assume a treatment response with standard treatment be around 10%. A PDO
and NGS guided treatment will likely improve the response rate to about 30% or more. In
the first stage, 10 patients will be accrued, If there is one or fewer response, in these
10 patients, the study will be stopped. Otherwise an additional 19 patients will be
accrued for a total of 29. The null hypothesis will be rejected if 6 or more responses
are observed in 29 patients. This design yields a type 1 error rate of 0.05 and a power
of 80%. Investigators plan to enrol 40 or more patients over a period of 2 years, with
the assumption that in about 20% of patients, PDO culture is unsuccessful.
Criteria for eligibility:
Criteria:
Inclusion Criteria:
- patients with metastatic, inoperable or advanced solid tumors who are refractory to
at least one standard chemo- or targeted drugs.
- The disease is accessible for a biopsy (radiologic or endoscopic) or resection of a
metastatic site.
- These patients are seen at a multidisciplinary tumor board meeting prior to
referrals.
- aged >18 years, able to provide written consents to trial participation,
- with an Eastern cooperative oncology group performance status of 0 or 1,
- with measurable disease in accordance with response evaluation criteria in solid
tumors (RECIST) version 1.1.
- deem suitable for standard chemo-therapy; i.e. with a normal neutrophil count,
hemoglobin > 9g/dl, serum creatinine, <1.5 x upper limit of normal, bilirubin < 1.5
x normal, Aspartate and alanine aminotransferases (<3 x ULN or <5x
- those with liver metastasis) and with an ejection Fraction >50% of normal on
echocardiography.
Exclusion Criteria:
- unable to provide informed consent
Gender:
All
Minimum age:
18 Years
Maximum age:
100 Years
Healthy volunteers:
No
Locations:
Facility:
Name:
Endoscopy Centre, Prince of Wales Hospital
Address:
City:
Hong Kong
Country:
Hong Kong
Contact:
Last name:
James YW LAU, MD
Phone:
+852350522640
Email:
laujyw@surgery.cuhk.edu.hk
Contact backup:
Last name:
Bing-yee SUEN, MHSc
Phone:
+85235052640
Email:
suenbingyee@surgery.cuhk.edu.hk
Start date:
October 1, 2024
Completion date:
February 1, 2028
Lead sponsor:
Agency:
Chinese University of Hong Kong
Agency class:
Other
Source:
Chinese University of Hong Kong
Record processing date:
ClinicalTrials.gov processed this data on November 12, 2024
Source: ClinicalTrials.gov page:
https://clinicaltrials.gov/ct2/show/NCT06077591
