ANZCTR - Registration

Registration number

ACTRN12622001509752

Ethics application status

Approved

Date submitted

6/10/2022

Date registered

5/12/2022

Date last updated

5/12/2022

Date data sharing statement initially provided

5/12/2022

Type of registration

Retrospectively registered

Titles & IDs

Public title

SARS-CoV-2 (COVID-19) vaccination and the immune responses in patients with haematological malignancy and other immune deficiency.

Scientific title

COVAXI - 2: SARS-CoV-2 vaccination and the immune responses in patients with haematological malignancy and other immune deficiency.

Secondary ID [1]

PBI-101

Universal Trial Number (UTN)

Trial acronym

COVAXI-2

Linked study record

Health condition

Health condition(s) or problem(s) studied:

Haematological malignancy

Immunosuppression

COVID-19

Condition category

Condition code

Blood

Haematological diseases

Cancer

Leukaemia - Chronic leukaemia

Cancer

Lymphoma (non Hodgkin's lymphoma) - High grade lymphoma

Cancer

Lymphoma (non Hodgkin's lymphoma) - Low grade lymphoma

Cancer

Myeloma

Inflammatory and Immune System

Other inflammatory or immune system disorders

Intervention/exposure

Study type

Observational

Description of intervention(s) / exposure

This is an observational Cohort study to assess the immune response to the SARS-CoV-2 vaccination and the prevalence of clotting related antibodies in hematology and other immunosuppressed patients.
Participants in this study will be assigned to one of the following groups:
- Group A: Patients with haematology and other immunosuppressed conditions who have received at least 3 doses of SARS-COV-2 vaccination according to Australian Government Vaccine Guidelines.
- Subgroup 1a: Immuno-suppressed haematology patients in Group A who have received or eligible to receive standard of care Australian Government Therapeutic Goods Administration approved COVID prevention subcutaneous injection (Evusheld - Cilgavimab and Tixagevimab) according to the WA Health Department Guidelines.
- Group B: General Population patients without haematological disorders who have received at least 3 doses of SARS-COV-2 vaccination according to Australian Government Vaccine Guidelines.
After informed consent, demographic and clinical information (Disease history for immunocompromised patients only, general medical history, concomitant medications, COVID-19 vaccination status/virus positivity status and vital signs) will be collected at registration and blood taken Day 30 to 120 post 3 or 4th vaccine for initial measurement of established protective antibody response. At 6 months or before further additional booster vaccination further clinical review (Disease history for immunocompromised patients only, concomitant medications, COVID-19 vaccination status/virus positivity status and vital signs) and blood draw to measure of the duration of the protective antibody response. A third blood sample will be taken Day 30 to 120 post 4 or 5th vaccine to measure of protective antibody response after next vaccination. In the eligible immunosuppressive haematology patients receiving Evusheld (Cilgavimab and Tixagevimab), a pre vaccination blood test and a day 30 post injection blood test in addition will be taken.
Frequency of Blood sample collection-
For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

As of the current guidelines, the participants will receive 4 vaccinations; but this may change according to the standard COVID-19 vaccination guidelines in the future.

Intervention code [1]

Early Detection / Screening

Comparator / control treatment

- Subgroup 1a: Immuno-suppressed haematology patients in Group A who have received or eligible to receive standard of care Australian Government Therapeutic Goods Administration approved COVID prevention subcutaneous injection (Evusheld - Cilgavimab and Tixagevimab) according to the WA Health Department Guidelines.

- Group B: General Population patients without haematological disorders who have received at least 3 doses of SARS-COV-2 vaccination according to Australian Government Vaccine Guidelines. Group B will serve as the comparator group

Control group

Active

Outcomes

Primary outcome [1]

-Determine the strength of the IgG response to receptor binding domain (RBD) of the S1 subunit of the spike protein of SARS-CoV-2 from blood samples collected in immunocompromised haematology patients overtime and compare to matched controls.

Timepoint [1]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [1]

We will assess nucleocapsid protein antibody concentration of the spike protein of SARS-CoV-2 bound IgG concentration.

Timepoint [1]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [2]

We will assess SARS-CoV-2 antibody titre concentration.

Timepoint [2]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [3]

We will determine the SARS-CoV-2 antibody assay validity coefficient based on WHO International Standard.

Timepoint [3]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [4]

We will assess a single secondary outcome- full blood count prior to additional vaccination.

Timepoint [4]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [5]

We will assess coagulation markers including PF4 antibodies concentrations

Timepoint [5]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [6]

We will assess the incidence of patients testing positive for SARS-CoV-2 infection by rapid antigen test, PCR test, etc.

Timepoint [6]

By doing rapid antigen test or PCR test

Secondary outcome [7]

We will assess the receptor-binding domain (RBD) of the S1 subunit of the spike protein of SARS-CoV-2 bound IgG concentration.

Timepoint [7]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [8]

We will assess coagulation markers including platelet glycoprotein VI

Timepoint [8]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Secondary outcome [9]

We will assess coagulation markers including thrombin generation.

Timepoint [9]

For Group A and B:
- A single blood sample will be collected between Day 30 to 120 post 3 or 4th vaccine
-A single blood sample will be collected up to 6 months before further additional booster vaccination
- A single blood sample will be collected between Day 30 to 120 post 4 or 5th vaccine

For sub group 1a
- A single pre-vaccination sample will be collected up to 7 days prior to Evusheld administration.
- A single blood sample will be collected between Day 20-30 post Evusheld

Eligibility

Key inclusion criteria

• Age > or = 18.
• Are eligible to receive or have received at least 3 doses of the standard of care SARS-COV-2 vaccine as per current Australian Government Therapeutic Goods Administration Vaccine Guidelines. Currently in Australia vaccines choices include Astra Zeneca (ChAdOx1), Pfizer (BNT162b2) Moderna (mRNA -1273) and Novavax.
• Patients with haematology disorders including CLL (Chronic lymphocytic leukemia), lymphoma, other B cell lymphoproliferative disorders, myeloma, MGUS (Monoclonal gammopathy of undetermined significance), myeloproliferative disorders and other immunosuppressed patients.
• Patients who present to primary care without haematological disorders who have received at least 3 doses of SARS-COV-2 vaccination according to Australian Government Vaccine Guidelines.
• Able and willing to provide Written and Informed Consent.

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Yes

Key exclusion criteria

• People with vaccine allergies.
• Pregnant or breast-feeding woman.

Study design

Statistical methods / analysis

IgG titres to the RBD of the S1 subunit of the spike protein of SARS-CoV-2 will be the primary data point to be used in estimating sample size and our data analysis. We use the following assumptions and principles in our sample size calculation and data analyses. Haematological patients will have a lower rate of seroconversion compared to controls (e.g., up to 40% vs over 90%). Haematological patients will have a much faster pace to reduce their antibody titres over a 12 to 24-month period. Two time points are available for antibody titres (up to 120 days, 6 months). We use repeated measures of ANOVA (one-way in assessing changes over time and two-way interaction in determining differences between 2 groups: haematological, control over time). We assume up to about 20% of the individuals may not have a complete set of data at all two time-points. Because of multiple testing for changes in titres over time for each of the three groups of participants, and, we are interested to compared between groups, in their differences in titres over time, we assume the alpha-value to be <0.01 as significant and 95% power as acceptable.

Any Response to COVID Vaccination (>50BAU/ml): We are planning a study of independent cases and controls with 1 control(s) per case. Prior data indicate that the probability of exposure among controls is 0.95. If the actual probability of exposure among cases is 0.3, we will need to study 9 case patients and 9 control patients to be able to reject the null hypothesis that the exposure rates for case and controls are equal with probability (power) 0.9. The Type I error probability associated with this test of this null hypothesis is 0.05. We will use an uncorrected chi-squared statistic to evaluate this null hypothesis.

Protective Response to COVID Vaccination (>600 BAU/ml): We are planning a study of independent cases and controls with 1 control(s) per case. Prior data indicate that the probability of exposure among controls is 0.98. If the actual probability of exposure among cases is 0.15, we will need to study 5 case patients and 5 control patients to be able to reject the null hypothesis that the exposure rates for case and controls are equal with probability (power) 0.9. The Type I error probability associated with this test of this null hypothesis is 0.05. We will use an uncorrected chi-squared statistic to evaluate this null hypothesis.
Assuming those 15% responding over 600 BAU/ml median was 800 immediately after the 4th dose vaccination which dropped to 200 BAU/ml at 6 months. Assuming the reduction in the titre is linear then T50 will be 3 months which means that immunosuppressed patients had their reduction in protection twice as fast as the control (healthy) patients.
If we assume the decline in antibody titre is proportional to the antibody titre at any time point, as in a typical exponential decay curve, then the rate of decay in antibody titre for the immunosuppressive group was about 7.8 faster than the control (given they had a lower titre to start with, the decline should be slower than half within the same time frame).

We have three groups of patients (Haematology Patients with no Evusheld, Haematology patients with Evusheld and age and matched controls).
Data will be analysed through 2-way ANOVA and assessing the treatment groups interacting with time remains a valid sample size calculation method. However, to avoid the dropout of cases with missing blood test data, a linear mixed model will be better to analyse and include patients who might have missing blood tests.

If we assume a titre of 600 BAU or more is protective. The mean titre of the control is 540 (90% of the 600 BU/ml), the mean titre for the group: haem + Evusheld is 480 (80% of 600 BU/ml), and the mean titre of the haem group only group is 420 BU/ml, data at three-time points are available, alpha error = 5% and power 95% acceptable, a correlation between measurements are 0.5, then the total sample size is 177 (or 59 per group). If we scale up to allow a 20% lost to follow-up or due to incomplete data, we will need at least 212 patients. If we have 150 patients in each group, we will have confidence in terms of power if our assumptions are valid.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

Actual

24/08/2022

Date of last participant enrolment

Anticipated

1/09/2023

Actual

Date of last data collection

Anticipated

1/09/2024

Actual

Sample size

Target

450

Accrual to date

65

Final

Recruitment in Australia

Recruitment state(s)

WA

Recruitment hospital [1]

Perth Blood Institute - West Perth

Recruitment postcode(s) [1]

6005 - West Perth

Funding & Sponsors

Funding source category [1]

Other Collaborative groups

Name [1]

The Perth Blood Institute

Country [1]

Australia

Primary sponsor type

Other Collaborative groups

Name

The Perth Blood Institute

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Bellberry Human Research Ethics Committee

Ethics committee address [1]

123 Glen Osmond Road Eastwood, South Australia 5063

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

20/05/2022

Approval date [1]

29/06/2022

Ethics approval number [1]

HREC_2022-05-451

Summary

Brief summary

The aim of this study is to assess the immune response to the SARS-CoV-2 vaccines and the prevalence of antibodies (anti-PF4) associated with development of a rare complication of SARS-CoV-2 vaccination, thrombotic thrombocytopaenia syndrome, in patients with blood cancers compared to an elderly control population from primary care.

Who is it for?
You may be eligible for this study if you are aged 18 years or older, have a haematological disorder (including chronic lymphocytic leukaemia, lymphoma, other B cell lymphoproliferative disorders, myeloma, monoclonal gammopathy of undetermined significance, and myeloproliferative disorders) or are immunosuppressed, and are eligible to receive or have received at least 3 doses of an intramuscular SARS-CoV-2 vaccine (including Astra Zeneca (ChAdOx1), Pfizer (BNT162b2) Moderna (mRNA -1273) and Novavax) or the subcutaneous vaccine (Evusheld) as per current Australian Government Vaccine Guidelines. You may also be eligible for this study if you are aged 18 years or older, presenting to primary care without haematological disorders and have received at least 3 doses of SARS-COV-2 vaccination according to Australian Government Vaccine Guidelines.

Study details
All participants will undergo SARS-CoV-2 vaccination in accordance with Australian Government Vaccine Guidelines. For those receiving intramuscular vaccination, a single blood sample for the assessment of immune response and antibody formation will be collected between Days 30 to 120 post 3rd or 4th vaccination, 6 months post 3rd or 4th vaccination (or immediately prior to additional booster vaccination), and between Days 30 to 120 post 4th or 5th vaccination. 
For those receiving subcutaneous vaccination, a single blood sample will be collected up to 7 days prior to vaccination and at Days 20 and 30 post-vaccination. 
At these timepoints, clinical reviews will also be undertaken to determine haematological malignancy diagnosis, baseline characteristics of independent variables (e.g., previous treatments) and blood parameters (e.g., full blood count).

It is hoped that this study may help to determine the immune response to the SARS-CoV-2 vaccination in this vulnerable group of patients, and will inform formulation of guidelines and treatment protocols for SARS-CoV-2 infection in the general population and immunosuppressed haematology patients.

Trial website

Public notes

Contacts

Principal investigator

Name

Prof Ross Baker

Address

Prof. Ross Baker
The Perth Blood Institute
18 Prowse Street,
West Perth-6005
Western Australia

Country

Australia

Phone

+610892005300

Email

[email protected]

Contact person for public queries

Name

Jarod Horobin

Address

Dr. Jarod Horobin
The Perth Blood Institute
18 Prowse Street,
West Perth-6005
Western Australia

Country

Australia

Phone

+610892005300

Email

[email protected]

Contact person for scientific queries

Name

Ross Baker

Address

Prof. Ross Baker
The Perth Blood Institute
18 Prowse Street,
West Perth-6005
Western Australia

Country

Australia

Phone

+610892005300

Email

[email protected]

Trial Review

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