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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03010228
Other study ID # VLA15-101
Secondary ID C4601005
Status Completed
Phase Phase 1
First received
Last updated
Start date January 31, 2017
Est. completion date January 16, 2019

Study information

Verified date March 2023
Source Pfizer
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Observer-blind, partially randomized, multi-center dose escalation Phase I study in healthy adults below 40 years of age. 180 subjects will be enrolled in 6 treatment groups (different doses; different formulation: with/without adjuvant); vaccinations will be given I.M.(intramuscular) into the deltoid region on Days 0, 28 and 56. Study participants will be followed up until one year after first vaccination. Booster Extension: Subjects in the 48µg and 90µg Treatment groups who received a complete Primary immunization schedule will be included into a Booster Extension 13 months after the first immunization.


Description:

This is an observer-blind, partially randomized, multi-center dose escalation Phase I study which aims to assess the safety, immunogenicity and dose response of VLA15 in healthy adults aged below 40 years. Overall 180 subjects will be enrolled in 6 treatment groups: VLA15 12µg with and w/o (without) Alum, VLA15 48µg with and w/o Alum, VLA15 90µg with and w/o Alum. For the first 24 subjects, the study will be open-label and subjects will not be randomized but included into a staggered dose escalation scheme for safety precaution. Thereafter, the study will be conducted observer-blind in respect to the investigators and site staff involved in clinical evaluation of subjects, subjects will be blinded as well. Remaining 156 subjects will be randomized into the 6 treatment groups. I.M. vaccinations are administered on Days 0, 28 and 56 into deltoid region of the non-dominant arm. The study will investigate the safety and tolerability as well as immunogenicity of VLA15. The primary objective addresses safety and tolerability of the vaccine up to three months after enrollment, i.e. 84 days after first vaccination. The study includes 1 screening visit and 8 outpatient visits from day 0 through day 365. In addition, safety phone calls will be performed. Booster Extension: Subjects in the 48µg and 90µg dose Groups at the Belgian site, who received a complete primary immunization schedule (three vaccinations), will be included into a Booster Extension to investigate the safety and immunogenicity of a booster dose of VLA15 administered 13 months after the first immunization. An extension analysis on safety and immunogenicity will be performed after the last subject has completed the last study visit at Month 19. Additionally a M14 interim analysis on immunogenicity data will be performed, when all subjects completed Month 14. For inclusion in the Booster Extension of this study only subjects are eligible, who were enrolled in Belgium, completed the primary immunization schedule (three vaccinations) and were randomized into 48µg or 90µg dose groups with or without alum. Subjects included in the staggered dose escalation phase will not be asked to participate in the Booster Extension for operational reasons.


Recruitment information / eligibility

Status Completed
Enrollment 179
Est. completion date January 16, 2019
Est. primary completion date September 28, 2017
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years to 39 Years
Eligibility Inclusion Criteria: - Healthy adults =18 to <40 years of age (for US healthy adults = 19 years to <40 years) at the time of screening. Health status is assessed by investigator at time of screening based on medical history, physical examination, and laboratory parameters. - Written informed consent obtained from the subject prior to any study related procedures. - BMI =18.5 and <30 at Visit 0 (Screening Visit). - Men or women; women require a negative pregnancy test at screening. Women with childbearing potential must agree to use an adequate contraception during the entire study. Booster Extension: - Completed Primary immunization schedule (three vaccinations) - Randomization into 48µg or 90µg group with or without Alum - Written informed consent for Booster Extension obtained from the subject prior to any study related procedures. - Enrolled at study site in Belgium - Men or women; women require a negative pregnancy test before booster vaccination. Women of childbearing potential must agree to use an adequate contraception during the entire study. Exclusion Criteria: - Pathological findings in any of the investigations (i.e. medical history, physical examination) as deemed clinically relevant by the investigator or any abnormal laboratory parameter of hematology, clinical chemistry, coagulation, RF (Rheumatoid Factor) or ACPA (Anti-citrullinated protein antibodies) at the Screening Visit. - Medical history of severe cardiovascular, respiratory (including asthma), metabolic, neurological, hepatic, rheumatic, hematological, gastrointestinal, renal disorders. - Medical history of or current musculoskeletal disorders as deemed clinically relevant by the investigator, arthritis or chronic musculoskeletal pain. - Previous vaccination against Lyme borreliosis with any (investigational) vaccine. - Use of any other investigational or non-registered medicinal product within 30 days prior to VLA15 vaccination at Visit 1 (Day 0) and throughout the entire study period. - Chronic illness related to Lyme borreliosis (LB), a history of or active symptomatic LB as suspected or diagnosed by a physician. Subjects with a positive serology test result for Borrelia burgdorferi sensu lato (s.l.) antibodies at screening are excluded. - Tick bite within 3 weeks prior to screening, or tick bite during vaccination period (i.e. Day 0 to Day 56). - Known active infection with Babesia microti (babesiosis) or Anaplasma phagocytophilum (ehrlichiosis). - Active or passive immunization four weeks before first vaccination at Visit 1 and up to Day 84 (i.e. 4 weeks after the last VLA15 immunization). Afterwards, vaccinations should be avoided, except for influenza (seasonal or pandemic) vaccines which may be administered after Day 84 (i.e. 4 weeks after the last VLA15 immunization). Subjects susceptible to require a vaccine during the study period (e.g. due to planned travel) should be excluded at screening. - Known congenital, hereditary or acquired immunodeficiency, including infection with human immunodeficiency virus (HIV), status post organ transplantation or immuno-suppressive therapy within 30 days prior to Day 0 and up to Day 84. Immuno-suppressive therapy is defined as administration of chronic (longer than 14 days) prednisone or equivalent = 0.05 mg/kg/day. Topical and inhaled steroids are allowed. - Planned intake of NSAID (Nonsteroidal anti-inflammatory drug) within three days prior and within seven days after any VLA15 vaccination. - History of severe hypersensitivity reactions and anaphylaxis. - History of allergic bronchial asthma and severe allergic rhinoconjunctivitis. - Known hypersensitivity or allergic reactions to one of the components of the vaccine. - History of autoimmune disease, including Type I Diabetes mellitus. Subjects with vitiligo or thyroid disease taking thyroid hormone replacement are not excluded. - Any malignancy in the past 5 years. If treatment for cancer was successfully completed more than 5 years ago and the malignancy is considered to be cured, the subject may be enrolled. - Acute febrile infections within 4 weeks prior to first vaccination and body temperature >37.8 C (oral) prior to each vaccination. - Known or suspected alcohol abuse, alcohol dependence, i.e. an average of more than approximately 60 g alcohol (approximately 1 liter of beer or 0.5 liter of wine) per day] or illicit drug use within the last year; - Inability or unwillingness to avoid more than the usual intake of alcohol (i.e. not more than 60 g alcohol (approximately 1 liter of beer or 0.5 liter of wine) per day) during the 48 hours after vaccination. - Pregnancy (positive pregnancy test), lactation or inadequate contraception in women with childbearing potential - Inability or unwillingness to provide informed consent or not able to understand and comply with protocol requirements, instructions and protocol-stated restrictions. - Donation of blood or blood-derived products (e.g. plasma) within 4 weeks prior to Visit 0 (Screening Visit) and during the entire study. - Receipt of blood or blood-derived products in the past 3 months prior to Visit 0 (Screening Visit) or anticipation of such products during the entire study. - Mental disorder as deemed clinically relevant by the investigator. - History of Guillain-Barré-Syndrome (GBS). - Any condition which might interfere with study objectives or that would limit the subject's ability to complete the study in the opinion of the investigator. - Persons who are committed to an institution (by virtue of an order issued either by the judicial or the administrative authorities). - Persons who are in a dependent relationship with the sponsor, an investigator or other study team members, or the study center. Dependent relationships include close relatives and household members (i.e. children, partner/spouse, siblings, parents) as well as employees of the investigator or study center personnel. Booster Extension: - Individual stopping rule was met during the Initial Study. - Subject has a known thrombocytopenia, bleeding disorder, or receipt of anticoagulants in the 3 weeks prior to booster vaccination contraindicating I.M. vaccination as judged by the investigator. - Pathological findings in the symptom driven physical examination as deemed clinically relevant by the investigator or any clinically significant abnormal laboratory parameter of hematology, clinical chemistry based on investigator judgement at Visit 8. Subjects with a positive test result for RF and ACPA at Visit 8 are excluded. - Use of any other investigational or non-registered medicinal product within 30 days prior to VLA15 booster vaccination at Visit 9 and throughout the entire Booster Extension period. - Tick bite within 3 weeks prior to booster vaccination (i.e. Visit 9). - Known active infection with Babesia microti (babesiosis) or Anaplasma phagocytophilum (ehrlichiosis). - Active or passive immunization four weeks before and within 7 days after booster vaccination at Visit 9. - Known congenital, hereditary or acquired immunodeficiency, including infection with human immunodeficiency virus (HIV), status post organ transplantation or immuno-suppressive therapy within 30 days prior to booster vaccination and up to 28 days after. Immuno-suppressive therapy is defined as administration of chronic (longer than 14 days) prednisone or equivalent = 0.05 mg/kg/day. Topical and inhaled steroids are allowed. - Developed any of the following conditions since enrolment into Initial Study: 1. Chronic illness related to Lyme borreliosis (LB), a history of or active symptomatic LB as suspected or diagnosed by a physician. 2. Severe cardiovascular, respiratory (including asthma), metabolic, neurological, hepatic, rheumatic, hematological, gastrointestinal, renal disorders. 3. Musculoskeletal disorders as deemed clinically relevant by the investigator, arthritis or chronic musculoskeletal pain. 4. Severe hypersensitivity reactions and anaphylaxis. 5. Allergic bronchial asthma and severe allergic rhinoconjunctivitis. 6. Hypersensitivity or allergic reactions to one of the components of the vaccine. 7. Autoimmune disease, including Type I Diabetes mellitus. Subjects with vitiligo or thyroid disease taking thyroid hormone replacement are not excluded. 8. Mental disorder as deemed clinically relevant by the investigator. 9. Guillain-Barré-Syndrome (GBS) 10. Malignancy - Known or suspected alcohol abuse alcohol dependence, i.e. an average of more than approximately 60 g alcohol (approximately 1 liter of beer or 0.5 liter of wine per day) or illicit drug use within the last year. - Inability or unwillingness to avoid more than the usual intake of alcohol (i.e. not more than 60 g alcohol (approximately 1 liter of beer or 0.5 liter of wine) per day) during the 48 hours after vaccination. - Pregnancy (positive pregnancy test), lactation or inadequate contraception in women of childbearing potential. - Inability or unwillingness to provide informed consent or not able to understand and comply with protocol requirements, instructions and protocol-stated restrictions. - Any condition which might interfere with study objectives or that would limit the subject's ability to complete the study in the opinion of the investigator. - Persons who are committed to an institution (by virtue of an order issued either by the judicial or the administrative authorities). - Persons who are in a dependent relationship with the sponsor, an investigator or other study team members, or the study center. Dependent relationships include close relatives and household members (i.e. children, partner/spouse, siblings, parents) as well as employees of the investigator or study center personnel.

Study Design


Intervention

Biological:
VLA15 with Alum
I.M. vaccination with a multivalent outer surface protein A (OspA) based vaccine candidate on days 0, 28 and 56; three different doses
VLA15 without Alum
I.M. vaccination with a multivalent outer surface protein A (OspA) based vaccine candidate on days 0, 28 and 56; three different doses

Locations

Country Name City State
Belgium University Hospital Ghent Ghent
United States eStudy Site La Mesa California
United States eStudySite La Mesa California
United States Celerion Inc. Lincoln Nebraska
United States Celerion, Inc Lincoln Nebraska

Sponsors (2)

Lead Sponsor Collaborator
Pfizer Valneva Austria GmbH

Countries where clinical trial is conducted

United States,  Belgium, 

Outcome

Type Measure Description Time frame Safety issue
Primary Rate of SAEs to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of related SAEs to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of any solicited or unsolicited Grade 3 or Grade 4 events up to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of any solicited or related unsolicited Grade 3 or Grade 4 events up to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of solicited local AEs within 7 days after each and after any vaccination up to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of solicited systemic AEs within 7 days after each and after any vaccination up to Day 84 up to Day 84 (Month 3) after first vaccination
Primary Rate of unsolicited AEs to Day 84, including clinically significant laboratory parameter changes up to Day 84 (Month 3) after first vaccination
Primary Rate of related unsolicited AEs to Day 84, including clinically significant laboratory parameter changes up to Day 84 (Month 3) after first vaccination
Secondary Rate of SAEs during the entire study period up to Day 365 (Month 12)
Secondary Rate of related SAEs during the entire study period up to Day 365 (Month 12)
Secondary Rate of any solicited or unsolicited Grade 3 or Grade 4 AEs during the entire study period up to Day 365 (Month 12)
Secondary Rate of any solicited or related unsolicited Grade 3 or Grade 4 AEs during the entire study period up to Day 365 (Month 12)
Secondary Rate of unsolicited AEs during the entire study period up to Day 365 (Month 12)
Secondary Rate of related unsolicited AEs during the entire study period up to Day 365 (Month 12)
Secondary Changes in laboratory parameters and rate of subjects with abnormal laboratory parameter up to Day 365 (Month 12)
Secondary GMTs (Geometric Mean Titre) for IgG against each OspA serotype ST1 to ST6, determined by ELISA Day 0, 28, 56, 84, 180, 236 and 365
Secondary SCRs (Seroconversion Rate, defined based on fold increase of each OspA serotype specific IgG (ST1 to ST6) as compared to baseline) Day 28, 56, 84, 180, 236 and 365
Secondary GMFR (Geometric Mean of the fold rise as compared to baseline) for IgG against each OspA serotype ST1 to ST6, determined by ELISA Day 28, 56, 84, 180, 236 and 365
See also
  Status Clinical Trial Phase
Recruiting NCT05641116 - Effectiveness of an Intervention Combining Adapted Physical Activity and Therapeutic Education in Patients With Chronic Symptoms Attributed to Lyme Borreliosis. N/A