TY - JOUR
T1 - PMS2CL interference leading to erroneous identification of a pathogenic PMS2 variant in Black patients
AU - Penn Medicine BioBank, Regeneron Genetics Center
AU - Cappadocia, Jacqueline
AU - Aiello, Lisa B.
AU - Kelley, Michael J.
AU - Katona, Bryson W.
AU - Maxwell, Kara N.
AU - Verma, Anurag
AU - Verma, Shefali S.
AU - Bradford, Yuki
AU - Brock, Ashlei
AU - DerOhannessian, Stephanie
AU - Dudek, Scott
AU - Dunn, Joseph
AU - Drivas, Theodore
AU - Haubein, Ned
AU - Hu-Sain, Khadijah
AU - Judy, Renae
AU - Kloter, Ashley
AU - Ko, Yi An
AU - Livingstone, Meghan
AU - Morrel, Linda
AU - Morse, Colleen
AU - Poindexter, Afiya
AU - Risman, Marjorie
AU - Tran, Teo
AU - Vadivieso, Fred
AU - Weaver, Jo Ellen
AU - Rader, Daniel J.
AU - Ritchie, Marylyn D.
AU - Feldman, Michael D.
AU - Beechert, Christina
AU - Forsythe, Caitlin
AU - Fuller, Erin D.
AU - Gu, Zhenhua
AU - Lattari, Michael
AU - Lopez, Alexander
AU - Overton, John D.
AU - Padilla, Maria Sotiropoulos
AU - Pradhan, Manasi
AU - Manoochehri, Kia
AU - Schleicher, Thomas D.
AU - Widom, Louis
AU - Wolf, Sarah E.
AU - Ulloa, Ricardo H.
AU - Averitt, Amelia
AU - Banerjee, Nilanjana
AU - Cantor, Michael
AU - Li, Dadong
AU - Malhotra, Sameer
AU - Sharma, Deepika
AU - Staples, Jeffrey
N1 - Publisher Copyright:
© 2024
PY - 2024/1
Y1 - 2024/1
N2 - This study investigates the frequency of a clinically reported variant in PMS2, NM_000535.7:c.2523G>A p.(W841∗), from next-generation sequencing studies in 2 racially diverse cohorts. We identified clinical reports of the PMS2 c.2523G>A p.(W841∗) variant in the National Precision Oncology Program's somatic testing database (n = 25,168). We determined frequency of the variant in germline exome sequencing from the Penn Medicine BioBank (n = 44,256) and in gnomAD. The PMS2 c.2523G>A p.(W841∗) was identified as a homozygous variant on tumor testing in an adult patient of self-identified Black race/ethnicity with no evidence of constitutional mismatch repair deficiency. The variant was clinically reported on 35 total tumor and liquid biopsy tests (0.1%), and all individuals with the variant were of self-identified Black race/ethnicity (0.6% of n = 5787). In individuals of African genetic ancestry (AFR), the variant's germline frequency was reported to be 0.2% and 1.3% in the Penn Medicine BioBank (PMBB) and gnomAD, respectively. The variant cannot be found in any individuals of European genetic ancestry (EUR) from either of the databases. The variant is found in a region of PMS2 with 100% homology to the PMS2CL pseudogene. PMS2 c.2523G>A p.(W841∗), when identified, is typically an African-ancestry-specific PMS2CL pseudogene variant, which should be recognized to prevent misdiagnosis of Lynch syndrome in Blacks.
AB - This study investigates the frequency of a clinically reported variant in PMS2, NM_000535.7:c.2523G>A p.(W841∗), from next-generation sequencing studies in 2 racially diverse cohorts. We identified clinical reports of the PMS2 c.2523G>A p.(W841∗) variant in the National Precision Oncology Program's somatic testing database (n = 25,168). We determined frequency of the variant in germline exome sequencing from the Penn Medicine BioBank (n = 44,256) and in gnomAD. The PMS2 c.2523G>A p.(W841∗) was identified as a homozygous variant on tumor testing in an adult patient of self-identified Black race/ethnicity with no evidence of constitutional mismatch repair deficiency. The variant was clinically reported on 35 total tumor and liquid biopsy tests (0.1%), and all individuals with the variant were of self-identified Black race/ethnicity (0.6% of n = 5787). In individuals of African genetic ancestry (AFR), the variant's germline frequency was reported to be 0.2% and 1.3% in the Penn Medicine BioBank (PMBB) and gnomAD, respectively. The variant cannot be found in any individuals of European genetic ancestry (EUR) from either of the databases. The variant is found in a region of PMS2 with 100% homology to the PMS2CL pseudogene. PMS2 c.2523G>A p.(W841∗), when identified, is typically an African-ancestry-specific PMS2CL pseudogene variant, which should be recognized to prevent misdiagnosis of Lynch syndrome in Blacks.
KW - Lynch syndrome
KW - PMS2
KW - PMS2CL
KW - germline genetic testing
KW - pseudogene interference
UR - http://www.scopus.com/inward/record.url?scp=85208459662&partnerID=8YFLogxK
U2 - 10.1016/j.gimo.2024.101858
DO - 10.1016/j.gimo.2024.101858
M3 - Article
AN - SCOPUS:85208459662
SN - 2949-7744
VL - 2
JO - Genetics in Medicine Open
JF - Genetics in Medicine Open
M1 - 101858
ER -