A Prospective, Observational Study to Examine the Effects of Ageing on the Clinical Outcomes of People Living With HIV in South Korea

Study Design: Multicentre, prospective, observational study over 3 years. Our study will describe the impact of advancing age on the experience of living with HIV in South Korea. To address this we will establish cohorts of HIV-positive people aged >50 and <50 years as well as demographically matched HIV-negative people aged >50 years. Although 2 years of follow up duration is short period to evaluate the effect of aging, this period could give us an insights for necessity of longer follow up study.

Setting:

Subjects will be recruited from three clinics: Severance Hospital; Seoul Medical Center; National Medical Center.

Number of Patients: Older HIV-positive cohort (n=500); Younger HIV-positive cohort (n=250); HIV-negative cohort (n=250). We arbitrarily decided these numbers of subjects considering the numbers of subjects of POPPY-UK study (1000, 500, and 500 subjects, respectively), feasibility of recruitment, and possible budget. Our choice of sample size is largely pragmatic, reflecting the number of older patients receiving care and the proportion that are expected to participate. Detailed sample size calculations are difficult given the wide range of topics and methodological approaches proposed.

Sample size was chosen pragmatically based on

1. the number of HIV pts of three participating hospitals (NMC≒1200, severance≒700, SMC≒300) 2) feasibility of recruitment 3) and possible budget

1. Screening

   Each subject must sign an Informed Consent Form prior to the conduct of any screening procedures.

   The purpose of the screening visit is to evaluate that the subject meets study inclusion/exclusion criteria. HIV antibody testing will be undertaken for subjects undergoing screening for the HIV-negative cohort.

2. Visit 1 (Baseline visit)

   The baseline visit will perform evaluations as per schedule of visits.

   The baseline visit is expected to take 1-2 hours; if possible the subject should attend fasted. The following information will be collected:

   • Baseline demographics: age; sex; sexual orientation; date of birth; education.

   • Socio-economic status: employment; household dependents; household income; housing.

   • Quality of life questionnaire.

   • Anthropometrics: height; weight; body mass index; waist circumference.

   • Lifestyle factors: current/past cigarette smoking; alcohol use; recreational drug use.

   • Full clinical history: to include cardiovascular events (hypertension, myocardial infarction, angina or acute coronary syndromes, cardiogenic arrhythmias, coronary artery stenting/bypass grafting, peripheral vascular disease), renal failure, liver failure, diabetes, malignancies, falls, fractures, joint disease or joint replacements.

   • Simple measurement of walking speed over a distance of 15 feet (457 cms).

   • Blood pressure will be estimated using an automated device.

   • Family medical history: to include any cardiovascular disease, type 2 diabetes mellitus, malignancies, mental illness, dementia or Alzheimer's disease, parental hip fractures.

   • Current and recent (over past 12 months) antiretroviral use: type of antiretroviral; start/stop dates; dose; frequency of dosing; side effects; reasons for prior changes/discontinuations.

   • Duration of HIV infection and date of HIV-seroconversion if known

   • Adherence assessment
   • Use of any other medications (including, but not limited to, anti-hypertensives, anti-depressants, vitamin D and/or calcium replacement therapy, lipid-lowering drugs, regular use of analgesics, herbal remedies, other over-the-counter drugs): type of drug; start/stop dates; dose; frequency of dosing; side effects.
   • Neurocognitive function: specific memory and cognitive testing assessing cortical and sub-cortical function.
   • Pain assessment: regional and widespread pain collected using a validated mannequin; nature of onset; duration; intensity; resulting disability
   • Falls risk (study questionnaire)
   • Fracture risk (study questionnaire)
   • Frailty assessment (study questionnaire)
   • Most recent laboratory tests will be recorded (assessed in the HIV-negative cohort): renal, liver, lipid and bone profiles, glucose, full blood count, sexual health screen, hepatitis C serology. These tests should have been performed within a year of the clinic visit.
   • Blood (serum, plasma, and PBMC) and urine samples: stored for subsequent projects of the potential pathogenic mechanisms underlying age-related diseases. This will include assessment of vitamin-D and PTH
   • Blood (plasma) will be collected for pharmacokinetic analysis (including but not limited to antiretroviral drug exposure)

3. Visit 2 (1st year follow up visit)

   This follow up visit will be performed as per schedule of visits. Only HIV-positive cohorts will be invited to undertake this visit with this visit expected to take 1 hour.

   The following will be assessed:

   • Changes to lifestyle and socio-economic status over the past year.
   • Significant clinical events occurring over the past year: dates of onset and resolution, use of medical services, changes to antiretroviral and other medications, and resulting ongoing health concerns.
   • Blood pressure will be estimated using an automated device.
   • Details of access to health care services over the past year: visits to hospital, and medical investigations performed (information obtained by direct questioning and through medical records review).
   • Most recent laboratory tests will be recorded: renal, liver, lipid and bone profiles, glucose, full blood count, sexual health screen, hepatitis C serology (Within the past year)
   • Concomitant medications: start/stop dates; dose; dosing frequency; side effects.
   • Fracture occurrence and fracture risk (see study questionnaire in appendix 1)
   • Regional and widespread pain.

3a Visit 2 (1st year follow up visit) for HIV negative participants.

These participants will be contacted by telephone by arrangement with the study nurse. They may be asked to attend the clinic in order to facilitate this visit.

Details of any changes in circumstances or illnesses and medication will be documented.

4 Visit 3 (2nd year follow up visit)

This follow up visit will be performed as per schedule of visits (2.0).

This visit is expected to take 1-2 hours; if possible the subject should attend fasted. The following information will be collected:

• Changes to lifestyle and socio-economic status over the past year.

• Significant clinical events occurring over the past year: dates of onset and resolution, use of medical services, treatments, and resulting ongoing health concerns.

• Details of access to health care services over the past year: visits to hospital, and medical investigations performed (information obtained by direct questioning and through medical records review).

• Simple measurement of walking speed over a distance of 15 feet (457 cms).

• Blood pressure will be estimated using an automated device.

• Concomitant medications: start/stop dates; dose; dosing frequency; side effects.

• Fracture occurrence and fracture risk (see study questionnaire in appendix 1).

• Neurocognitive function: specific memory and cognitive testing assessing cortical and sub-cortical function.

• Respiratory questionnaire

• Regional and widespread pain.

• Quality of life questionnaire.

• Most recent laboratory tests will be recorded (assessed in the HIV-negative cohort): renal, liver, lipid and bone profiles, glucose, full blood count, sexual health screen, hepatitis C serology (within the previous year)

• Blood (serum, plasma, and PBMC) and urine samples: stored for subsequent projects of the potential pathogenic mechanisms underlying age-related diseases. This will included assessment of vitamin-D and PTH

• Blood (plasma) will be collected for pharmacokinetic analysis (including but not limited to antiretroviral drug exposure)

  5 MRI Sub-study

• A sub-study will be conducted at the Severance Hospital site for participants equal to and over the age of 50 both HIV +ve (n=20) and HIV -ve (n=20). Matching criteria would be age, sexual orientation, and socio-economic status (i.e. insurance coverage status).

The study will comprise of three study visits:

1. Screening
2. Visit 1 (Baseline visit)
3. Visit 2 (Follow up visit after 2 years) The study visits will include the following assessments Blood (serum, plasma, and PBMC), urine, CSF and stool samples stored for future analysis (genetic polymorphism associated with neurocognitive dysfunction, CSF concentrations of antiretrovirals, biomarkers such as CSF neurofilament light (NFL) chain concentration, microbiome of stool, etc) Neurocognitive testing Lumbar puncture examination Cerebral MRI scan Respiratory function and cardiac function assessments

6 Withdrawal of subjects from study

Subjects are allowed to decline further participation in the study at any time. This will not affect their future care.

7 Study timelines

Recruitment and baseline visits (visit 1) will take place from months 1-12, with annual visits from months 13-24 (visit 2) and 25-36 (visit 3)