The diagnostic yield of exome sequencing in liver diseases from a curated gene panel

Xiao Fei Kong; Kelsie Bogyo; Sheena Kapoor; Patrick R. Shea; Emily E. Groopman; Amanda Thomas-Wilson; Enrico Cocchi; Hila Milo Rasouly; Beishi Zheng; Siming Sun; Junying Zhang; Mercedes Martinez; Jennifer M. Vittorio; Lorna M. Dove; Maddalena Marasa; Timothy C. Wang; Elizabeth C. Verna; Howard J. Worman; Ali G. Gharavi; David B. Goldstein; Julia Wattacheril

doi:10.1038/s41598-023-42202-1

The diagnostic yield of exome sequencing in liver diseases from a curated gene panel

Xiao Fei Kong, Kelsie Bogyo, Sheena Kapoor, Patrick R. Shea, Emily E. Groopman, Amanda Thomas-Wilson, Enrico Cocchi, Hila Milo Rasouly, Beishi Zheng, Siming Sun, Junying Zhang, Mercedes Martinez, Jennifer M. Vittorio, Lorna M. Dove, Maddalena Marasa, Timothy C. Wang, Elizabeth C. Verna, Howard J. Worman, Ali G. Gharavi, David B. GoldsteinJulia Wattacheril

Research output: Contribution to journal › Article › peer-review

Abstract

Exome sequencing (ES) has been used in a variety of clinical settings but there are limited data on its utility for diagnosis and/or prediction of monogenic liver diseases. We developed a curated list of 502 genes for monogenic disorders associated with liver phenotypes and analyzed ES data for these genes in 758 patients with chronic liver diseases (CLD). For comparison, we examined ES data in 7856 self-declared healthy controls (HC), and 2187 patients with chronic kidney disease (CKD). Candidate pathogenic (P) or likely pathogenic (LP) variants were initially identified in 19.9% of participants, most of which were attributable to previously reported pathogenic variants with implausibly high allele frequencies. After variant annotation and filtering based on population minor allele frequency (MAF ≤ 10^–4 for dominant disorders and MAF ≤ 10^–3 for recessive disorders), we detected a significant enrichment of P/LP variants in the CLD cohort compared to the HC cohort (X ² test OR 5.00, 95% CI 3.06–8.18, p value = 4.5e−12). A second-level manual annotation was necessary to capture true pathogenic variants that were removed by stringent allele frequency and quality filters. After these sequential steps, the diagnostic rate of monogenic disorders was 5.7% in the CLD cohort, attributable to P/LP variants in 25 genes. We also identified concordant liver disease phenotypes for 15/22 kidney disease patients with P/LP variants in liver genes, mostly associated with cystic liver disease phenotypes. Sequencing results had many implications for clinical management, including familial testing for early diagnosis and management, preventative screening for associated comorbidities, and in some cases for therapy. Exome sequencing provided a 5.7% diagnostic rate in CLD patients and required multiple rounds of review to reduce both false positive and false negative findings. The identification of concordant phenotypes in many patients with P/LP variants and no known liver disease also indicates a potential for predictive testing for selected monogenic liver disorders.

Original language	English (US)
Article number	21540
Journal	Scientific reports
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41598-023-42202-1
State	Published - Dec 2023

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Kong, X. F., Bogyo, K., Kapoor, S., Shea, P. R., Groopman, E. E., Thomas-Wilson, A., Cocchi, E., Milo Rasouly, H., Zheng, B., Sun, S., Zhang, J., Martinez, M., Vittorio, J. M., Dove, L. M., Marasa, M., Wang, T. C., Verna, E. C., Worman, H. J., Gharavi, A. G., ... Wattacheril, J. (2023). The diagnostic yield of exome sequencing in liver diseases from a curated gene panel. Scientific reports, 13(1), Article 21540. https://doi.org/10.1038/s41598-023-42202-1

Kong, XF, Bogyo, K, Kapoor, S, Shea, PR, Groopman, EE, Thomas-Wilson, A, Cocchi, E, Milo Rasouly, H, Zheng, B, Sun, S, Zhang, J, Martinez, M, Vittorio, JM, Dove, LM, Marasa, M, Wang, TC, Verna, EC, Worman, HJ, Gharavi, AG, Goldstein, DB & Wattacheril, J 2023, 'The diagnostic yield of exome sequencing in liver diseases from a curated gene panel', Scientific reports, vol. 13, no. 1, 21540. https://doi.org/10.1038/s41598-023-42202-1

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title = "The diagnostic yield of exome sequencing in liver diseases from a curated gene panel",

abstract = "Exome sequencing (ES) has been used in a variety of clinical settings but there are limited data on its utility for diagnosis and/or prediction of monogenic liver diseases. We developed a curated list of 502 genes for monogenic disorders associated with liver phenotypes and analyzed ES data for these genes in 758 patients with chronic liver diseases (CLD). For comparison, we examined ES data in 7856 self-declared healthy controls (HC), and 2187 patients with chronic kidney disease (CKD). Candidate pathogenic (P) or likely pathogenic (LP) variants were initially identified in 19.9% of participants, most of which were attributable to previously reported pathogenic variants with implausibly high allele frequencies. After variant annotation and filtering based on population minor allele frequency (MAF ≤ 10–4 for dominant disorders and MAF ≤ 10–3 for recessive disorders), we detected a significant enrichment of P/LP variants in the CLD cohort compared to the HC cohort (X 2 test OR 5.00, 95% CI 3.06–8.18, p value = 4.5e−12). A second-level manual annotation was necessary to capture true pathogenic variants that were removed by stringent allele frequency and quality filters. After these sequential steps, the diagnostic rate of monogenic disorders was 5.7% in the CLD cohort, attributable to P/LP variants in 25 genes. We also identified concordant liver disease phenotypes for 15/22 kidney disease patients with P/LP variants in liver genes, mostly associated with cystic liver disease phenotypes. Sequencing results had many implications for clinical management, including familial testing for early diagnosis and management, preventative screening for associated comorbidities, and in some cases for therapy. Exome sequencing provided a 5.7% diagnostic rate in CLD patients and required multiple rounds of review to reduce both false positive and false negative findings. The identification of concordant phenotypes in many patients with P/LP variants and no known liver disease also indicates a potential for predictive testing for selected monogenic liver disorders.",

author = "Kong, {Xiao Fei} and Kelsie Bogyo and Sheena Kapoor and Shea, {Patrick R.} and Groopman, {Emily E.} and Amanda Thomas-Wilson and Enrico Cocchi and {Milo Rasouly}, Hila and Beishi Zheng and Siming Sun and Junying Zhang and Mercedes Martinez and Vittorio, {Jennifer M.} and Dove, {Lorna M.} and Maddalena Marasa and Wang, {Timothy C.} and Verna, {Elizabeth C.} and Worman, {Howard J.} and Gharavi, {Ali G.} and Goldstein, {David B.} and Julia Wattacheril",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

doi = "10.1038/s41598-023-42202-1",

language = "English (US)",

volume = "13",

journal = "Scientific reports",

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T1 - The diagnostic yield of exome sequencing in liver diseases from a curated gene panel

AU - Kong, Xiao Fei

AU - Bogyo, Kelsie

AU - Kapoor, Sheena

AU - Shea, Patrick R.

AU - Groopman, Emily E.

AU - Thomas-Wilson, Amanda

AU - Cocchi, Enrico

AU - Milo Rasouly, Hila

AU - Zheng, Beishi

AU - Sun, Siming

AU - Zhang, Junying

AU - Martinez, Mercedes

AU - Vittorio, Jennifer M.

AU - Dove, Lorna M.

AU - Marasa, Maddalena

AU - Wang, Timothy C.

AU - Verna, Elizabeth C.

AU - Worman, Howard J.

AU - Gharavi, Ali G.

AU - Goldstein, David B.

AU - Wattacheril, Julia

PY - 2023/12

Y1 - 2023/12

N2 - Exome sequencing (ES) has been used in a variety of clinical settings but there are limited data on its utility for diagnosis and/or prediction of monogenic liver diseases. We developed a curated list of 502 genes for monogenic disorders associated with liver phenotypes and analyzed ES data for these genes in 758 patients with chronic liver diseases (CLD). For comparison, we examined ES data in 7856 self-declared healthy controls (HC), and 2187 patients with chronic kidney disease (CKD). Candidate pathogenic (P) or likely pathogenic (LP) variants were initially identified in 19.9% of participants, most of which were attributable to previously reported pathogenic variants with implausibly high allele frequencies. After variant annotation and filtering based on population minor allele frequency (MAF ≤ 10–4 for dominant disorders and MAF ≤ 10–3 for recessive disorders), we detected a significant enrichment of P/LP variants in the CLD cohort compared to the HC cohort (X 2 test OR 5.00, 95% CI 3.06–8.18, p value = 4.5e−12). A second-level manual annotation was necessary to capture true pathogenic variants that were removed by stringent allele frequency and quality filters. After these sequential steps, the diagnostic rate of monogenic disorders was 5.7% in the CLD cohort, attributable to P/LP variants in 25 genes. We also identified concordant liver disease phenotypes for 15/22 kidney disease patients with P/LP variants in liver genes, mostly associated with cystic liver disease phenotypes. Sequencing results had many implications for clinical management, including familial testing for early diagnosis and management, preventative screening for associated comorbidities, and in some cases for therapy. Exome sequencing provided a 5.7% diagnostic rate in CLD patients and required multiple rounds of review to reduce both false positive and false negative findings. The identification of concordant phenotypes in many patients with P/LP variants and no known liver disease also indicates a potential for predictive testing for selected monogenic liver disorders.

AB - Exome sequencing (ES) has been used in a variety of clinical settings but there are limited data on its utility for diagnosis and/or prediction of monogenic liver diseases. We developed a curated list of 502 genes for monogenic disorders associated with liver phenotypes and analyzed ES data for these genes in 758 patients with chronic liver diseases (CLD). For comparison, we examined ES data in 7856 self-declared healthy controls (HC), and 2187 patients with chronic kidney disease (CKD). Candidate pathogenic (P) or likely pathogenic (LP) variants were initially identified in 19.9% of participants, most of which were attributable to previously reported pathogenic variants with implausibly high allele frequencies. After variant annotation and filtering based on population minor allele frequency (MAF ≤ 10–4 for dominant disorders and MAF ≤ 10–3 for recessive disorders), we detected a significant enrichment of P/LP variants in the CLD cohort compared to the HC cohort (X 2 test OR 5.00, 95% CI 3.06–8.18, p value = 4.5e−12). A second-level manual annotation was necessary to capture true pathogenic variants that were removed by stringent allele frequency and quality filters. After these sequential steps, the diagnostic rate of monogenic disorders was 5.7% in the CLD cohort, attributable to P/LP variants in 25 genes. We also identified concordant liver disease phenotypes for 15/22 kidney disease patients with P/LP variants in liver genes, mostly associated with cystic liver disease phenotypes. Sequencing results had many implications for clinical management, including familial testing for early diagnosis and management, preventative screening for associated comorbidities, and in some cases for therapy. Exome sequencing provided a 5.7% diagnostic rate in CLD patients and required multiple rounds of review to reduce both false positive and false negative findings. The identification of concordant phenotypes in many patients with P/LP variants and no known liver disease also indicates a potential for predictive testing for selected monogenic liver disorders.

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The diagnostic yield of exome sequencing in liver diseases from a curated gene panel

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