Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study

Herdiantri Sufriyana; Yu Wei Wu; Emily Chia Yu Su

doi:10.1142/9789811286421_0042

Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study

Herdiantri Sufriyana, Yu Wei Wu, Emily Chia Yu Su^*

^*Corresponding author for this work

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution › peer-review

2 Scopus citations

Abstract

Background. Existing proposed pathogenesis for preeclampsia (PE) was only applied for early onset subtype and did not consider pre-pregnancy and competing risks. We aimed to decipher PE subtypes by identifying related transcriptome that represents endometrial maturation and histologic chorioamnionitis. Methods. We utilized eight arrays of mRNA expression for discovery (n=289), and other eight arrays for validation (n=352). Differentially expressed genes (DEGs) were overlapped between those of: (1) healthy samples from endometrium, decidua, and placenta, and placenta samples under histologic chorioamnionitis; and (2) placenta samples for each of the subtypes. They were all possible combinations based on four axes: (1) pregnancy-induced hypertension; (2) placental dysfunction-related diseases (e.g., fetal growth restriction [FGR]); (3) onset; and (4) severity. Results. The DEGs of endometrium at late-secretory phase, but none of decidua, significantly overlapped with those of any subtypes with: (1) early onset (p-values ≤0.008); (2) severe hypertension and proteinuria (p-values ≤0.042); or (3) chronic hypertension and/or severe PE with FGR (p-values ≤0.042). Although sharing the same subtypes whose DEGs with which significantly overlap, the gene regulation was mostly counter-expressed in placenta under chorioamnionitis (n=13/18, 72.22%; odds ratio [OR] upper bounds ≤0.21) but co-expressed in late-secretory endometrium (n=3/9, 66.67%; OR lower bounds ≥1.17). Neither the placental DEGs at first-nor second-Trimester under normotensive pregnancy significantly overlapped with those under late-onset, severe PE without FGR. Conclusions. We identified the transcriptome of endometrial maturation in placental dysfunction that distinguished early-and late-onset PE, and indicated chorioamnionitis as a PE competing risk. This study implied a feasibility to develop and validate the pathogenesis models that include pre-pregnancy and competing risks to decide if it is needed to collect prospective data for PE starting from pre-pregnancy including chorioamnionitis information.

Original language	English
Title of host publication	Pacific Symposium on Biocomputing 2024, PSB 2024
Editors	Russ B. Altman, Lawrence Hunter, Marylyn D. Ritchie, Tiffany Murray, Teri E. Klein
Publisher	World Scientific
Pages	549-563
Number of pages	15
Edition	2024
ISBN (Electronic)	9789811286414
DOIs	https://doi.org/10.1142/9789811286421_0042
State	Published - 2024
Event	29th Pacific Symposium on Biocomputing, PSB 2024 - Kohala Coast, United States Duration: 3 Jan 2024 → 7 Jan 2024

Conference

Conference	29th Pacific Symposium on Biocomputing, PSB 2024
Country/Territory	United States
City	Kohala Coast
Period	3/01/24 → 7/01/24

Keywords

Chorioamnionitis
Endometrial maturation
Gene regulation
Microarray analysis
Preeclampsia

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10.1142/9789811286421_0042

Cite this

Sufriyana, H., Wu, Y. W., & Su, E. C. Y. (2024). Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study. In R. B. Altman, L. Hunter, M. D. Ritchie, T. Murray, & T. E. Klein (Eds.), Pacific Symposium on Biocomputing 2024, PSB 2024 (2024 ed., pp. 549-563). World Scientific. https://doi.org/10.1142/9789811286421_0042

Sufriyana, Herdiantri ; Wu, Yu Wei ; Su, Emily Chia Yu. / Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes : A preliminary study. Pacific Symposium on Biocomputing 2024, PSB 2024. editor / Russ B. Altman ; Lawrence Hunter ; Marylyn D. Ritchie ; Tiffany Murray ; Teri E. Klein. 2024. ed. World Scientific, 2024. pp. 549-563

@inproceedings{d1e06eb19fcc44c296e999ef19517b7e,

title = "Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study",

abstract = "Background. Existing proposed pathogenesis for preeclampsia (PE) was only applied for early onset subtype and did not consider pre-pregnancy and competing risks. We aimed to decipher PE subtypes by identifying related transcriptome that represents endometrial maturation and histologic chorioamnionitis. Methods. We utilized eight arrays of mRNA expression for discovery (n=289), and other eight arrays for validation (n=352). Differentially expressed genes (DEGs) were overlapped between those of: (1) healthy samples from endometrium, decidua, and placenta, and placenta samples under histologic chorioamnionitis; and (2) placenta samples for each of the subtypes. They were all possible combinations based on four axes: (1) pregnancy-induced hypertension; (2) placental dysfunction-related diseases (e.g., fetal growth restriction [FGR]); (3) onset; and (4) severity. Results. The DEGs of endometrium at late-secretory phase, but none of decidua, significantly overlapped with those of any subtypes with: (1) early onset (p-values ≤0.008); (2) severe hypertension and proteinuria (p-values ≤0.042); or (3) chronic hypertension and/or severe PE with FGR (p-values ≤0.042). Although sharing the same subtypes whose DEGs with which significantly overlap, the gene regulation was mostly counter-expressed in placenta under chorioamnionitis (n=13/18, 72.22%; odds ratio [OR] upper bounds ≤0.21) but co-expressed in late-secretory endometrium (n=3/9, 66.67%; OR lower bounds ≥1.17). Neither the placental DEGs at first-nor second-Trimester under normotensive pregnancy significantly overlapped with those under late-onset, severe PE without FGR. Conclusions. We identified the transcriptome of endometrial maturation in placental dysfunction that distinguished early-and late-onset PE, and indicated chorioamnionitis as a PE competing risk. This study implied a feasibility to develop and validate the pathogenesis models that include pre-pregnancy and competing risks to decide if it is needed to collect prospective data for PE starting from pre-pregnancy including chorioamnionitis information.",

keywords = "Chorioamnionitis, Endometrial maturation, Gene regulation, Microarray analysis, Preeclampsia",

author = "Herdiantri Sufriyana and Wu, {Yu Wei} and Su, {Emily Chia Yu}",

note = "Publisher Copyright: {\textcopyright} 2023 The Authors.; 29th Pacific Symposium on Biocomputing, PSB 2024 ; Conference date: 03-01-2024 Through 07-01-2024",

year = "2024",

doi = "10.1142/9789811286421_0042",

language = "English",

pages = "549--563",

editor = "Altman, {Russ B.} and Lawrence Hunter and Ritchie, {Marylyn D.} and Tiffany Murray and Klein, {Teri E.}",

booktitle = "Pacific Symposium on Biocomputing 2024, PSB 2024",

publisher = "World Scientific",

address = "新加坡",

edition = "2024",

}

Sufriyana, H, Wu, YW & Su, ECY 2024, Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study. in RB Altman, L Hunter, MD Ritchie, T Murray & TE Klein (eds), Pacific Symposium on Biocomputing 2024, PSB 2024. 2024 edn, World Scientific, pp. 549-563, 29th Pacific Symposium on Biocomputing, PSB 2024, Kohala Coast, United States, 3/01/24. https://doi.org/10.1142/9789811286421_0042

Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study. / Sufriyana, Herdiantri; Wu, Yu Wei; Su, Emily Chia Yu.
Pacific Symposium on Biocomputing 2024, PSB 2024. ed. / Russ B. Altman; Lawrence Hunter; Marylyn D. Ritchie; Tiffany Murray; Teri E. Klein. 2024. ed. World Scientific, 2024. p. 549-563.

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution › peer-review

TY - GEN

T1 - Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes

T2 - 29th Pacific Symposium on Biocomputing, PSB 2024

AU - Sufriyana, Herdiantri

AU - Wu, Yu Wei

AU - Su, Emily Chia Yu

PY - 2024

Y1 - 2024

N2 - Background. Existing proposed pathogenesis for preeclampsia (PE) was only applied for early onset subtype and did not consider pre-pregnancy and competing risks. We aimed to decipher PE subtypes by identifying related transcriptome that represents endometrial maturation and histologic chorioamnionitis. Methods. We utilized eight arrays of mRNA expression for discovery (n=289), and other eight arrays for validation (n=352). Differentially expressed genes (DEGs) were overlapped between those of: (1) healthy samples from endometrium, decidua, and placenta, and placenta samples under histologic chorioamnionitis; and (2) placenta samples for each of the subtypes. They were all possible combinations based on four axes: (1) pregnancy-induced hypertension; (2) placental dysfunction-related diseases (e.g., fetal growth restriction [FGR]); (3) onset; and (4) severity. Results. The DEGs of endometrium at late-secretory phase, but none of decidua, significantly overlapped with those of any subtypes with: (1) early onset (p-values ≤0.008); (2) severe hypertension and proteinuria (p-values ≤0.042); or (3) chronic hypertension and/or severe PE with FGR (p-values ≤0.042). Although sharing the same subtypes whose DEGs with which significantly overlap, the gene regulation was mostly counter-expressed in placenta under chorioamnionitis (n=13/18, 72.22%; odds ratio [OR] upper bounds ≤0.21) but co-expressed in late-secretory endometrium (n=3/9, 66.67%; OR lower bounds ≥1.17). Neither the placental DEGs at first-nor second-Trimester under normotensive pregnancy significantly overlapped with those under late-onset, severe PE without FGR. Conclusions. We identified the transcriptome of endometrial maturation in placental dysfunction that distinguished early-and late-onset PE, and indicated chorioamnionitis as a PE competing risk. This study implied a feasibility to develop and validate the pathogenesis models that include pre-pregnancy and competing risks to decide if it is needed to collect prospective data for PE starting from pre-pregnancy including chorioamnionitis information.

AB - Background. Existing proposed pathogenesis for preeclampsia (PE) was only applied for early onset subtype and did not consider pre-pregnancy and competing risks. We aimed to decipher PE subtypes by identifying related transcriptome that represents endometrial maturation and histologic chorioamnionitis. Methods. We utilized eight arrays of mRNA expression for discovery (n=289), and other eight arrays for validation (n=352). Differentially expressed genes (DEGs) were overlapped between those of: (1) healthy samples from endometrium, decidua, and placenta, and placenta samples under histologic chorioamnionitis; and (2) placenta samples for each of the subtypes. They were all possible combinations based on four axes: (1) pregnancy-induced hypertension; (2) placental dysfunction-related diseases (e.g., fetal growth restriction [FGR]); (3) onset; and (4) severity. Results. The DEGs of endometrium at late-secretory phase, but none of decidua, significantly overlapped with those of any subtypes with: (1) early onset (p-values ≤0.008); (2) severe hypertension and proteinuria (p-values ≤0.042); or (3) chronic hypertension and/or severe PE with FGR (p-values ≤0.042). Although sharing the same subtypes whose DEGs with which significantly overlap, the gene regulation was mostly counter-expressed in placenta under chorioamnionitis (n=13/18, 72.22%; odds ratio [OR] upper bounds ≤0.21) but co-expressed in late-secretory endometrium (n=3/9, 66.67%; OR lower bounds ≥1.17). Neither the placental DEGs at first-nor second-Trimester under normotensive pregnancy significantly overlapped with those under late-onset, severe PE without FGR. Conclusions. We identified the transcriptome of endometrial maturation in placental dysfunction that distinguished early-and late-onset PE, and indicated chorioamnionitis as a PE competing risk. This study implied a feasibility to develop and validate the pathogenesis models that include pre-pregnancy and competing risks to decide if it is needed to collect prospective data for PE starting from pre-pregnancy including chorioamnionitis information.

KW - Chorioamnionitis

KW - Endometrial maturation

KW - Gene regulation

KW - Microarray analysis

KW - Preeclampsia

UR - http://www.scopus.com/inward/record.url?scp=85181416885&partnerID=8YFLogxK

U2 - 10.1142/9789811286421_0042

DO - 10.1142/9789811286421_0042

M3 - Conference contribution

C2 - 38160306

AN - SCOPUS:85181416885

SP - 549

EP - 563

BT - Pacific Symposium on Biocomputing 2024, PSB 2024

A2 - Altman, Russ B.

A2 - Hunter, Lawrence

A2 - Ritchie, Marylyn D.

A2 - Murray, Tiffany

A2 - Klein, Teri E.

PB - World Scientific

Y2 - 3 January 2024 through 7 January 2024

ER -

Low-and high-level information analyses of transcriptome connecting endometrial-deciduaplacental origin of preeclampsia subtypes: A preliminary study

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