Official Title
Minimal Residual Disease as a Possible Predictive Factor for Relapse in Patients With AL Amyloidosis
Brief Title
Minimal Residual Disease as a Possible Predictive Factor for Relapse in Patients With AL Amyloidosis
Protocol ID
NCT02555969
Lead Sponsor
Tufts Medical Center
Brief Summary
This protocol will assess patients with AL amyloidosis who achieve a complete response
(CR) or very good partial response (VGPR) to therapy for minimal residual disease (MRD).
Three approaches to MRD testing will be used since there is no established method. The
investigators will clone and sequence each patient's light chain (LC) gene and design
patient-specific primers to evaluate genomic DNA from future marrow specimens. Whole
genome sequencing (WGS) will be used to test baseline and follow-up marrow cell DNA,
seeking copy number variations in chromosomes 1 and 2 or 22, and structural variations in
chromosomes 11 and 14, consistent with the known genetic abnormalities in AL and with
clonal LC gene use. Plasma protein analysis by mass spectrometry will also be used to
look for fragmentary protein sequences associated with the culprit LC gene of each
subject. The feasibility and predictive value of these three approaches in patients
achieving CR or VGPR will be evaluated. This protocol will help provide insight into the
ways that the disease changes and progresses. MRD testing is likely an important next
step in AL management.
Detailed Description
This protocol will assess AL amyloidosis patients who achieve a CR or VGPR to first-line
therapy for evidence of MRD by Q-PCR, NGS, and plasma protein analysis by mass
spectrometry using marrow cells obtained annually at times of standard clinical
evaluations.
A bone marrow aspirate sample from diagnosis will be used to create a baseline profile of
each patient's disease. This sample will allow the investigators to create the
primer-probe sets required for MRD testing by Q-PCR, which will be conducted after the
patient has achieved a CR or VGPR. A baseline bone marrow biopsy sample will either be
taken at the time of consent or can be taken from storage if the patient has previously
consented to have their marrow cells banked for research purposes. An extra 15 mL of
aspirate will be taken from their diagnostic bone marrow biopsy, which is routinely
conducted on newly diagnosed patients for clinical purposes. Annual bone marrow aspirates
will not be taken for research purposes until after the patient has responded. Patients
will remain on protocol, but only begin MRD testing after achieving a CR or VGPR to
first-line therapy at which point annual marrow collections for MRD testing will begin.
In the event the patient does not reach a CR or VGPR to first-line therapy, the baseline
bone marrow aspirate from diagnosis will be discarded.
Patients who choose to allow their marrow to be used in this study will sign a consent
form specifically for this study. At the time of consent, three green top tubes of
peripheral blood will be obtained for WGS of non-tumor cells. No further blood samples
will be required for this study. After achieving a CR or VGPR, patients will be
completely re-staged as is standard of care at annual intervals. Samples to test for the
presence of MRD in their marrows will be obtained at these times of clinical re-staging
for up to 3 years after their response to therapy. Both blood and bone marrow samples for
this study will be immediately taken to an on-site laboratory where they will be briefly
stored before testing. This will ensure no study samples interfere with routine clinical
care.
In order to test for the presence of MRD, three techniques will be used: Q-PCR, WGS, and
plasma protein analysis by mass spectrometry. Both Q-PCR and WGS will use genomic DNA
from marrow aspirate samples. To make primer-probe sets for Q-PCR, bone marrow samples
from baseline will be used to create individualized primer-probe sets that can recognize
the genetically unique LC gene that causes each patient's disease. To perform WGS,
genomic DNA will be supplied to the core genetics laboratory for creation of a library
and multiplex next generation sequencing. To perform plasma protein analysis, plasma will
be isolated from a portion of each subject's peripheral blood and bone marrow aspirate
samples in an on-site laboratory. Each subject's de-identified LC gene sequence and their
de-identified plasma samples will then be sent to Memorial Sloan-Kettering Cancer Center
(MSKCC) for mass spectrometry to look for fragmentary protein sequences associated with
the culprit LC gene of each subject.
After reaching a CR or VGPR, at annual evaluations for up to 3 years, the genomic DNA
from the research sample of bone marrow collected during standard of care clinical
procedures will be used to confirm maintenance of response by testing for the presence of
MRD with each of the 3 methods (Q-PCR, WGS, and plasma protein analysis) noted above.
Marrow material collected for the purposes of this study will not be stored after
analysis, and primer-probe set design will be conducted entirely within Tufts Medical
Center. Any marrow samples not fully consumed during analysis will be destroyed.
By using these three methods this protocol will determine whether one method is superior
to the others and whether the three methods produce results that correlate with each
other. The decision to discontinue participation in MRD testing will be made by the
patient and the physician on an individual basis. Patients who have relapse or
hematologic progression of disease during the three year period by standard blood and
urine tests will no longer have testing for MRD.
Enrollment Count
56 participants
Eligibility Criteria
Inclusion Criteria:
- Patients with AL amyloidosis at Tufts Medical Center who have baseline bone marrow
samples available and achieve a CR or VGPR to treatment. Patients may consent and
register at diagnosis and have a baseline marrow collected at the time of consent;
or patients may consent during therapy prior to achieving a response, if they have
previously banked marrow cells for research.
Exclusion Criteria:
- Patients who do not have available baseline bone marrow samples.
Filters
Amyloidosis
Primary Amyloidosis
COMPLETED
CHILD
ADULT
OLDER_ADULT