A Safety and Immunology Study of a Modified Vaccinia Vaccine for HER-2(+) Breast Cancer After Adjuvant Therapy
| Status: | Completed |
|---|---|
| Conditions: | Breast Cancer, Cancer |
| Therapuetic Areas: | Oncology |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 3/16/2019 |
| Start Date: | June 2010 |
| End Date: | September 2012 |
A Phase I Safety and Immunogenicity Trial of MVA-BN®-HER2 Vaccine in HER-2-Positive Breast Cancer Patients Following Adjuvant Therapy
The current trial, BNIT-BR-003, will evaluate the safety and biological activity of a fixed
dose of MVA-BN®-HER2 following adjuvant chemotherapy in patients with HER-2-positive breast
cancer.
The intent of vaccination is to induce a combined antibody and T-cell anti-HER-2 immune
response, which is intended to target HER-2-expressing tumor cells, and may induce tumor
regression or slow progression of disease.
dose of MVA-BN®-HER2 following adjuvant chemotherapy in patients with HER-2-positive breast
cancer.
The intent of vaccination is to induce a combined antibody and T-cell anti-HER-2 immune
response, which is intended to target HER-2-expressing tumor cells, and may induce tumor
regression or slow progression of disease.
MVA-BN®-HER2 is a candidate breast cancer immunotherapy product comprised of a highly
attenuated non-replicating vaccinia virus, MVA-BN®, engineered to encode a modified form of
the HER-2 protein.
MVA-BN® is a well-characterized, clonal strain of modified vaccinia virus Ankara (MVA) being
developed as a smallpox vaccine, suitable for use in high-risk (e.g., immunocompromised)
individuals. MVA-BN®-derived vectors encoding heterologous antigens are being developed for
use as vaccines for infectious diseases such as HIV, and for the treatment of cancer. A large
database exists from safety evaluations in animals and in humans for MVA-BN®, and
MVA-BN®-derived vectors.
HER-2 is overexpressed in 20-30% of human breast cancers. It is an oncogene/growth factor
receptor critical for the malignant phenotype of HER-2- expressing tumors. It is an
immunogenic target, and immune responses to this protein have been shown to mediate potent
anti-tumor activity in multiple animal models. Means to stimulate anti-HER-2 reactivity are
now being studied clinically. Sponsor, collaborators, and others have used both Protein and
DNA vaccine forms of HER-2, and a safety database is developed and no significant adverse
events have resulted from HER-2 directed vaccination.
MVA-BN®-HER2 encodes a modified form of the HER-2 protein, hereinafter referred to as HER2.
HER2 contains the extracellular domain of HER-2 but lacks the intracellular, cell signaling
domain. In addition, HER2 includes two universal T-cell epitopes from tetanus toxin to
facilitate the stimulation of an immune response to HER-2, a self-protein.
The current trial, BNIT-BR-003, will evaluate the safety and biological activity of a fixed
dose of MVA-BN®-HER2 following adjuvant chemotherapy in patients with breast cancers which
overexpress HER-2.
Patients will receive 6 subcutaneous vaccinations at 4-week intervals and will have blood
drawn for immune function analysis.
attenuated non-replicating vaccinia virus, MVA-BN®, engineered to encode a modified form of
the HER-2 protein.
MVA-BN® is a well-characterized, clonal strain of modified vaccinia virus Ankara (MVA) being
developed as a smallpox vaccine, suitable for use in high-risk (e.g., immunocompromised)
individuals. MVA-BN®-derived vectors encoding heterologous antigens are being developed for
use as vaccines for infectious diseases such as HIV, and for the treatment of cancer. A large
database exists from safety evaluations in animals and in humans for MVA-BN®, and
MVA-BN®-derived vectors.
HER-2 is overexpressed in 20-30% of human breast cancers. It is an oncogene/growth factor
receptor critical for the malignant phenotype of HER-2- expressing tumors. It is an
immunogenic target, and immune responses to this protein have been shown to mediate potent
anti-tumor activity in multiple animal models. Means to stimulate anti-HER-2 reactivity are
now being studied clinically. Sponsor, collaborators, and others have used both Protein and
DNA vaccine forms of HER-2, and a safety database is developed and no significant adverse
events have resulted from HER-2 directed vaccination.
MVA-BN®-HER2 encodes a modified form of the HER-2 protein, hereinafter referred to as HER2.
HER2 contains the extracellular domain of HER-2 but lacks the intracellular, cell signaling
domain. In addition, HER2 includes two universal T-cell epitopes from tetanus toxin to
facilitate the stimulation of an immune response to HER-2, a self-protein.
The current trial, BNIT-BR-003, will evaluate the safety and biological activity of a fixed
dose of MVA-BN®-HER2 following adjuvant chemotherapy in patients with breast cancers which
overexpress HER-2.
Patients will receive 6 subcutaneous vaccinations at 4-week intervals and will have blood
drawn for immune function analysis.
Inclusion Criteria:
- Signed Informed Consent
- Women, ≥ 18 years of age
- Histologically documented, HER-2-positive breast cancer without metastatic disease.
Hormone receptor (ER/PR) status may be either positive or negative. HER-2 (+) status
may be determined by one of the following measurements:
- Immunohistochemistry 3+ or FISH/CISH+ (HER-2 gene signal to centromere 17 signal > 2).
NOTE: HER-2 assessment may have been on initial diagnosis and need not be repeated.
- Patients should be assessed as having no evidence of disease (NED) at the end of
adjuvant chemotherapy. In addition, these patients must have a clinical evaluation and
lab work as standard of care disease assessment without evidence of recurrence within
28 days of the first planned dose of MVA-BN®-HER2.
- Completed adjuvant and/or neoadjuvant chemotherapy for breast cancer at least 3 months
previously (measured from the date of the last dose of chemotherapy) and prior to the
first planned dose of MVA-BN®-HER2).
- ECOG Performance Score of 0, 1.
- Predicted life expectancy ≥ 12 months
- Left ventricular ejection fraction (LVEF) by ECHO ≥ LLN as defined by institutional
standards
- Women of childbearing potential must:
- have a negative serum or urine pregnancy test, and
- must agree to use a medically acceptable barrier and/or chemical method of
contraception throughout the study treatment period and for 28 days after the
last dose of MVA-BN®-HER2.
- No significant cardiac, bone marrow dysfunction, or coagulopathy (defined as no Grade
3 or greater AE according to NCI CTCAE v 3.0). No significant hepatic or renal
dysfunction (defined as no Grade 2 or greater AE according to NCI CTCAE v 3.0.
Patients with a known history of a CLINICALLY NON-SIGNIFICANT laboratory parameter may
be eligible for inclusion provided an exemption is granted by the study Medical
Monitor prior to enrollment.
- A negative virology screen for HIV, HBsAg, and HCV
Exclusion Criteria:
- Congestive heart failure (NYHA Class III or IV), unstable angina, or cardiovascular
disease such as stroke or myocardial infarction (current or within the past 6 months)
- History of cardiac toxicity secondary to chemotherapy or Herceptin immunotherapy (LVEF
decline of 15% or greater from baseline)
- History of prior malignancies other than breast cancer within the past 5 years,
excluding basal or squamous cell carcinoma of the skin or carcinoma in situ of the
cervix
- Any breast cancer metastases beyond the lymph nodes
- Known allergy to eggs, egg products, or aminoglycoside antibiotics, e.g., gentamicin
or tobramycin
- Chronic administration (defined as 6 or more consecutive days of use) of systemic
corticosteroids within 14 days of the first planned dose of MVA-BN®-HER2. Limited use
of inhaled steroids, nasal sprays, eye drops, and topical creams for small body areas
is allowed.
- History of or active autoimmune disease. Persons with vitiligo or thyroid disease
taking thyroid replacement hormones are not excluded.
- Prior solid organ or hematopoietic allogenic transplant(s)
- Prior use of hematopoietic growth factors (e.g., GM-CSF) within 14 days of the first
planned dose of MVA-BN®-HER2
- Receipt of an investigational agent within 28 days of the first planned dose of
MVA-BN®-HER2
- Prior "vaccine" therapy for breast cancer at any time
- Vaccination:
Live (attenuated) vaccine (e.g., FluMist®) Vaccination with a live vaccine within 28 days
of the first planned dose of MVA-BN®-HER2, or plans to receive a live vaccine within 28
days after the last dose of MVA-BN®-HER2 is not allowed Killed (inactivated) vaccine
(e.g.,PneumoVax®) Vaccination with a killed vaccine within 14 days of the first planned
dose of MVA-BN®-HER2, or plans to receive a killed vaccine within 14 ' days after the last
dose of MVA-BN®-HER2 is not allowed
- A maximum cumulative dose of prior doxorubicin > 360 mg/m2 or epirubicn > 720 mg/m2
- Radiation therapy within 14 days of the first planned dose of MVA-BN®-HER2 or plans
for radiation therapy after enrollment. Prior to initiating palliative radiation
during the treatment phase of the study, the Sponsor's medical monitor or designee
must be contacted.
- Pregnant, lactating, or nursing
- Any condition which, in the opinion of the investigator, would prevent full
participation in this trial or the long-term follow-up study, or would interfere with
the evaluation of the trial endpoints
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