TY - JOUR
T1 - Current clinical practices and challenges in molecular testing
T2 - a GOAL Consortium Hematopathology Working Group report
AU - Lee, Thomas D.
AU - Aisner, Dara L.
AU - David, Marjorie P.
AU - Eno, Celeste C.
AU - Gagan, Jeffrey
AU - Gocke, Christopher D.
AU - Guseva, Natalya V.
AU - Haley, Lisa
AU - Jajosky, Audrey N.
AU - Jones, Daniel
AU - Mansukhani, Mahesh M.
AU - Mroz, Pawel
AU - Murray, Sarah S.
AU - Newsom, Kimberly J.
AU - Paulson, Vera
AU - Roy, Somak
AU - Rushton, Chase
AU - Segal, Jeremy P.
AU - Senaratne, T. Niroshini
AU - Siddon, Alexa J.
AU - Starostik, Petr
AU - Van Ziffle, Jessica A.G.
AU - Wu, David
AU - Xian, Rena R.
AU - Yohe, Sophia
AU - Kim, Annette S.
N1 - Publisher Copyright:
© 2023 by The American Society of Hematology.
PY - 2023/8/16
Y1 - 2023/8/16
N2 - While molecular testing of hematologic malignancies is now standard of care, there is variability in practice and testing capabilities between different academic laboratories, with common questions arising on how to best meet clinical expectations. A survey was sent to hematopathology subgroup members of the Genomics Organization for Academic Laboratories consortium to assess current and future practice and potentially establish a reference for peer institutions. Responses were received from 18 academic tertiary-care laboratories regarding next-generation sequencing (NGS) panel design, sequencing protocols and metrics, assay characteristics, laboratory operations, case reimbursement, and development plans. Differences in NGS panel size, use, and gene content were reported. Gene content for myeloid processes was reported to be generally excellent, while genes for lymphoid processes were less well covered. The turnaround time (TAT) for acute cases, including acute myeloid leukemia, was reported to range from 2 to 7 calendar days to 15 to 21 calendar days, with different approaches to achieving rapid TAT described. To help guide NGS panel design and standardize gene content, consensus gene lists based on current and future NGS panels in development were generated. Most survey respondents expected molecular testing at academic laboratories to continue to be viable in the future, with rapid TAT for acute cases likely to remain an important factor. Molecular testing reimbursement was reported to be a major concern. The results of this survey and subsequent discussions improve the shared understanding of differences in testing practices for hematologic malignancies between institutions and will help provide a more consistent level of patient care.
AB - While molecular testing of hematologic malignancies is now standard of care, there is variability in practice and testing capabilities between different academic laboratories, with common questions arising on how to best meet clinical expectations. A survey was sent to hematopathology subgroup members of the Genomics Organization for Academic Laboratories consortium to assess current and future practice and potentially establish a reference for peer institutions. Responses were received from 18 academic tertiary-care laboratories regarding next-generation sequencing (NGS) panel design, sequencing protocols and metrics, assay characteristics, laboratory operations, case reimbursement, and development plans. Differences in NGS panel size, use, and gene content were reported. Gene content for myeloid processes was reported to be generally excellent, while genes for lymphoid processes were less well covered. The turnaround time (TAT) for acute cases, including acute myeloid leukemia, was reported to range from 2 to 7 calendar days to 15 to 21 calendar days, with different approaches to achieving rapid TAT described. To help guide NGS panel design and standardize gene content, consensus gene lists based on current and future NGS panels in development were generated. Most survey respondents expected molecular testing at academic laboratories to continue to be viable in the future, with rapid TAT for acute cases likely to remain an important factor. Molecular testing reimbursement was reported to be a major concern. The results of this survey and subsequent discussions improve the shared understanding of differences in testing practices for hematologic malignancies between institutions and will help provide a more consistent level of patient care.
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U2 - 10.1182/bloodadvances.2023010149
DO - 10.1182/bloodadvances.2023010149
M3 - Article
C2 - 37236162
AN - SCOPUS:85169321370
SN - 2473-9529
VL - 7
SP - 4599
EP - 4607
JO - Blood Advances
JF - Blood Advances
IS - 16
ER -