Pulmonary Arterial Hypertension Clinical Trial
Official title:
A Nation-wide Multicenter Registry and Biobank Program for Deep Phenotyping of Idiopathic and Hereditary Pulmonary Arterial Hypertension in Korea: the PAH Platform for Deep Phenotyping in Korean Subjects (PHOENIKS) Cohort
A total of 16 regional hospitals will be registering clinical data and biological specimens of idiopathic pulmonary arterial hypertension (IPAH)/heritable pulmonary arterial hypertension (HPAH) patients across Korea. The diagnosis of pulmonary arterial hypertension(PAH) will be based on right heart catheterization, where PAH caused by etiology other than HPAH or IPAH will be excluded. All clinical data will be stored to a government-based online database. Each participating hospitals will be collecting whole blood from each patient, through which DNA, RNA, serum, plasma, and peripheral blood mononuclear cells will be extracted from the buffy coat layer for further multi-omics analysis.
Study Objectives The current study is a multicenter registry and biobank based on South
Korean populations to construct a database for the elucidation the molecular and genetic
modifiers of PAH. The ultimate goal is to utilize deep phenotypic data for prognosis
prediction and discovery of biomarkers and targeted therapies.
Study Sample The current study will initially exclude the most frequent form of PAH in Korea,
the connective tissue disease (CTD)-related PAH, and focus on the diagnosis and deep
phenotyping of idiopathic PAH (IPAH) and heritable PAH (HPAH) patients. The inclusion
criteria are as follows: (1) over 18 years of age, (2) mean pulmonary arterial pressure of
25mmHg or higher confirmed by right heart catheterization (RHC), (3) pulmonary vascular
resistance ≥ 240 dynes∙s∙cm-5, (4) left ventricle diastolic pressure (LVDEP) or pulmonary
capillary wedge pressure (PCWP) ≤ 15mmHg. Exclusion criteria are: (1) patients with
drug-induced-PAH, (2) CTD, human immunodeficiency virus (HIV) infection, portal hypertension,
congenital heart disease, or Schistosomiasis associated-PAH, (3) long-term responders to
calcium channel blockers, (4) PAH patients with overt features of venous capillaries
involvement, leaving IPAH and HPAH patients among group 1 of PH to be evaluated. HPAH will be
diagnosed by identifying patients with heterozygous pathogenic variants of predetermined
genes such as BMPR2, ACVRL1, ENG, CAV1, SMAD1, SMAD4, SMAD9, KCNK3, and EIF2AK4. Patients
without a specific genetic mutation will then be categorized as IPAH patients. The genomic
data of family members across 3 pedigrees of an HPAH patient will also be analyzed. All
clinical and biological data will be reported to a customized web-based case report form
called the iCReaT system managed by the Korean Center for Disease Control. All collected
biospecimens will be stored at the Korean National Institute of Health main storage. Although
the current analysis is planned to be limited to IPAH and HPAH patients, our steering
committee plans to expand to all types of PAH in subsequent studies. This study was approved
by the institutional ethics committee of each participating institutions and complied with
the Declaration of Helsinki (6th revision). An informed consent will be received by each
patient.
Baseline Data and Biospecimen Collection The baseline data from the registered patients
across the 16 regional hospitals will include the following: WHO functional classification,
6-minute walking test, blood sample, electrocardiogram, chest X-ray, echocardiography,
optional pulmonary-cardio exercise test, optional Cardiac MRI, and RHC. Detailed information
of each exams are specified in Table 2. The registered patient will be followed up on a
regular basis for further data and biospecimen collection.
With the patient's blood sample, DNA, RNA, serum, plasma, and peripheral blood mononuclear
cells (PBMC) from the buffy coat will be separated and be extracted for further storage and
studies. For the DNA sample, 2.5ml of the whole blood will be stored in a PAX gene DNA tube
at the collecting site, and it will be carried to the main center at 4~10 C. At the main
center, it will, then, be transferred to a 2ml cryotube to be stored at -70~80C. For
patient's RNA collection, 2.5 mL of whole blood will be collected at PAX gene RNA tube, and
it will be sent to the main center at 4~10 C, which will also be further transferred to a
cryotube to be stored at -70~80C.
Patient's serum, plasma and the buffy coat will also be collected. At the respective
collection sites, serum will be collected at a serum separation tube, and after 30 minutes of
venipuncture, it will be centrifuged and stored at -20C. For patient's plasma, cell
preparation tube will be used within 2 hours of blood collection. Then, each sample will be
ready to be stored at -20C by treating the samples with human serum type antibody, DMSO, and
freezing medium. To separate and extract PBMC, white buffy coat layer will be separated and
be stored at a 1.5ml tube with a freezing medium at -20C. The collected baseline data will
then go through a clean-up process and further evaluation of its quality will be done. In
addition, five patients will be selected to do a whole-genome sequencing. All the collected
biospecimen will be donated to NIH center storage, and will be further used for a multi-omics
studies in order to deep phenotype the patient's specimens.
Patient Follow Up All patients will be followed up twice or more a year, with expected 80%
follow up rate. During the second and third year, patient registry and data collection will
be continued with the same protocol. To maintain the credibility of collected data, the
steering committee will continuously monitor and audit the collected data. Protocol may be
further crafted after evaluating the previous year's data. In addition, effective data
management strategies, including a guideline to standardize patient's body measurement and
blood sample will be developed. Ten patient samples will be selected for a next generation
sequencing, and we will be utilized in discovering novel genetic mutations.
Genetic Mutation Analysis across Three-Pedigrees for HPAH Patients In order to determine
patients with HPAH, a familial genetic study will be performed. A three-generation pedigree
for each PAH patient with with or without the existence of a BMPR2, ACVRL1, ENG, CAV1, SMAD1,
SMAD4, SMAD9, KCNK3, and/or EIF2AK4 mutation will be evaluated. Blood samples from family
members of patients with a HPAH will be collected for genetic screening.
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