Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes

Yassemine Khawajkie; Nawel Mechtouf; Ngoc Minh Phuong Nguyen; Kurosh Rahimi; Magali Breguet; Jocelyne Arseneau; Brigitte M. Ronnett; Lori Hoffner; Felicia Lazure; Marjolaine Arnaud; Fabrice Peers; Liane Tan; Basam Abu Rafea; Monica Aguinaga; Neil S. Horowitz; Asangla Ao; Seang Lin Tan; Richard Brown; William Buckett; Urvashi Surti; Karine Hovanes; Trilochan Sahoo; Philippe Sauthier; Rima Slim

doi:10.1038/s41379-019-0432-4

Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes

Yassemine Khawajkie, Nawel Mechtouf, Ngoc Minh Phuong Nguyen, Kurosh Rahimi, Magali Breguet, Jocelyne Arseneau, Brigitte M. Ronnett, Lori Hoffner, Felicia Lazure, Marjolaine Arnaud, Fabrice Peers, Liane Tan, Basam Abu Rafea, Monica Aguinaga, Neil S. Horowitz, Asangla Ao, Seang Lin Tan, Richard Brown, William Buckett, Urvashi SurtiKarine Hovanes, Trilochan Sahoo, Philippe Sauthier, Rima Slim

School of Medicine

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

7 Scopus citations

Abstract

Hydatidiform mole (HM) is an aberrant human pregnancy characterized by excessive trophoblastic proliferation and abnormal embryonic development. HM has two morphological types, complete (CHM) and partial (PHM), and non-recurrent ones have three genotypic types, androgenetic monospermic, androgenetic dispermic, and triploid dispermic. Most available studies on risk factors predisposing to different types of HM and their malignant transformation mainly suffer from the lack of comprehensive genotypic analysis of large cohorts of molar tissues combined with accurate postmolar hCG follow-up. Moreover, 10–20% of patients with one HM have at least one non-molar miscarriage, which is higher than the frequency of two pregnancy losses in the general population (2–5%), suggesting a common genetic susceptibility to HM and miscarriages. However, the underlying causes of the miscarriages in these patients are unknown. Here, we comprehensively analyzed 204 HM, mostly from patients referred to the Quebec Registry of Trophoblastic Diseases and for which postmolar hCG monitoring is available, and 30 of their non-molar miscarriages. We revisited the risk of maternal age and neoplastic transformation across the different HM genotypic categories and investigated the presence of chromosomal abnormalities in their non-molar miscarriages. We confirm that androgenetic CHM is more prone to gestational trophoblastic neoplasia (GTN) than triploid dispermic PHM, and androgenetic dispermic CHM is more prone to high-risk GTN and choriocarcinoma (CC) than androgenetic monospermic CHM. We also confirm the association between increased maternal age and androgenetic CHM and their malignancies. Most importantly, we demonstrate for the first time that patients with an HM and miscarriages are at higher risk for aneuploid miscarriages [83.3%, 95% confidence interval (CI): 0.653–0.944] than women with sporadic (51.5%, 95% CI: 50.3–52.7%, p value = 0.0003828) or recurrent miscarriages (43.8%, 95% CI: 40.7–47.0%, p value = 0.00002). Our data suggest common genetic female germline defects predisposing to HM and aneuploid non-molar miscarriages in some patients.

Original language	English (US)
Pages (from-to)	880-892
Number of pages	13
Journal	Modern Pathology
Volume	33
Issue number	5
DOIs	https://doi.org/10.1038/s41379-019-0432-4
State	Published - May 1 2020

ASJC Scopus subject areas

Pathology and Forensic Medicine

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10.1038/s41379-019-0432-4

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Khawajkie, Y., Mechtouf, N., Nguyen, N. M. P., Rahimi, K., Breguet, M., Arseneau, J., Ronnett, B. M., Hoffner, L., Lazure, F., Arnaud, M., Peers, F., Tan, L., Rafea, B. A., Aguinaga, M., Horowitz, N. S., Ao, A., Tan, S. L., Brown, R., Buckett, W., ... Slim, R. (2020). Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes. Modern Pathology, 33(5), 880-892. https://doi.org/10.1038/s41379-019-0432-4

Khawajkie, Y, Mechtouf, N, Nguyen, NMP, Rahimi, K, Breguet, M, Arseneau, J, Ronnett, BM, Hoffner, L, Lazure, F, Arnaud, M, Peers, F, Tan, L, Rafea, BA, Aguinaga, M, Horowitz, NS, Ao, A, Tan, SL, Brown, R, Buckett, W, Surti, U, Hovanes, K, Sahoo, T, Sauthier, P & Slim, R 2020, 'Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes', Modern Pathology, vol. 33, no. 5, pp. 880-892. https://doi.org/10.1038/s41379-019-0432-4

@article{74e453b01fd64efb89fe9b445af5bed5,

title = "Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes",

abstract = "Hydatidiform mole (HM) is an aberrant human pregnancy characterized by excessive trophoblastic proliferation and abnormal embryonic development. HM has two morphological types, complete (CHM) and partial (PHM), and non-recurrent ones have three genotypic types, androgenetic monospermic, androgenetic dispermic, and triploid dispermic. Most available studies on risk factors predisposing to different types of HM and their malignant transformation mainly suffer from the lack of comprehensive genotypic analysis of large cohorts of molar tissues combined with accurate postmolar hCG follow-up. Moreover, 10–20% of patients with one HM have at least one non-molar miscarriage, which is higher than the frequency of two pregnancy losses in the general population (2–5%), suggesting a common genetic susceptibility to HM and miscarriages. However, the underlying causes of the miscarriages in these patients are unknown. Here, we comprehensively analyzed 204 HM, mostly from patients referred to the Quebec Registry of Trophoblastic Diseases and for which postmolar hCG monitoring is available, and 30 of their non-molar miscarriages. We revisited the risk of maternal age and neoplastic transformation across the different HM genotypic categories and investigated the presence of chromosomal abnormalities in their non-molar miscarriages. We confirm that androgenetic CHM is more prone to gestational trophoblastic neoplasia (GTN) than triploid dispermic PHM, and androgenetic dispermic CHM is more prone to high-risk GTN and choriocarcinoma (CC) than androgenetic monospermic CHM. We also confirm the association between increased maternal age and androgenetic CHM and their malignancies. Most importantly, we demonstrate for the first time that patients with an HM and miscarriages are at higher risk for aneuploid miscarriages [83.3%, 95% confidence interval (CI): 0.653–0.944] than women with sporadic (51.5%, 95% CI: 50.3–52.7%, p value = 0.0003828) or recurrent miscarriages (43.8%, 95% CI: 40.7–47.0%, p value = 0.00002). Our data suggest common genetic female germline defects predisposing to HM and aneuploid non-molar miscarriages in some patients.",

author = "Yassemine Khawajkie and Nawel Mechtouf and Nguyen, {Ngoc Minh Phuong} and Kurosh Rahimi and Magali Breguet and Jocelyne Arseneau and Ronnett, {Brigitte M.} and Lori Hoffner and Felicia Lazure and Marjolaine Arnaud and Fabrice Peers and Liane Tan and Rafea, {Basam Abu} and Monica Aguinaga and Horowitz, {Neil S.} and Asangla Ao and Tan, {Seang Lin} and Richard Brown and William Buckett and Urvashi Surti and Karine Hovanes and Trilochan Sahoo and Philippe Sauthier and Rima Slim",

note = "Funding Information: Acknowledgements The authors would like to thank Dr. Olga Basso for her help with the statistical analysis. This study was supported by the Canadian Institutes of Health Research to R.S. (MOP-130364, MOP 102469, and MOP 86546). We also express our gratitude to the Pathology Departments of the following health centers for providing archived products of conception for analyses: McGill University Health Centre, Centre Hospitalier de l{\textquoteright}Universit{\'e} de Montr{\'e}al, Centre Hospitalier Universitaire de Sainte-Justine, Centre de la Sant{\'e} de Laval, H{\^o}pital Pierre Le Gardeur, Centre Hospitalier R{\'e}gional de Rimouski, Centre de Sant{\'e} et de Services Sociaux de Trois Rivi{\`e}res, London Health Science Centre, H{\^o}pital Pierre Boucher, H{\^o}pital Maisonneuve Rosemont, H{\^o}pital Sacr{\'e}-Coeur, H{\^o}pital Anna-Laberge, H{\^o}pital G{\'e}n{\'e}ral du Lakeshore, Jewish General Hospital, H{\^o}pital Honor{\'e} Mercier, Credit Valley Hospital, H{\^o}pital Saint Jean sur Richelieu, H{\^o}pital Regional Saint Jerome, H{\^o}pital Sainte-Mary, and Windsor Regional Hospital. Publisher Copyright: {\textcopyright} 2019, The Author(s), under exclusive licence to United States & Canadian Academy of Pathology.",

year = "2020",

month = may,

day = "1",

doi = "10.1038/s41379-019-0432-4",

language = "English (US)",

volume = "33",

pages = "880--892",

journal = "Modern Pathology",

issn = "0893-3952",

publisher = "Nature Publishing Group",

number = "5",

}

TY - JOUR

T1 - Comprehensive analysis of 204 sporadic hydatidiform moles

T2 - revisiting risk factors and their correlations with the molar genotypes

AU - Khawajkie, Yassemine

AU - Mechtouf, Nawel

AU - Nguyen, Ngoc Minh Phuong

AU - Rahimi, Kurosh

AU - Breguet, Magali

AU - Arseneau, Jocelyne

AU - Ronnett, Brigitte M.

AU - Hoffner, Lori

AU - Lazure, Felicia

AU - Arnaud, Marjolaine

AU - Peers, Fabrice

AU - Tan, Liane

AU - Rafea, Basam Abu

AU - Aguinaga, Monica

AU - Horowitz, Neil S.

AU - Ao, Asangla

AU - Tan, Seang Lin

AU - Brown, Richard

AU - Buckett, William

AU - Surti, Urvashi

AU - Hovanes, Karine

AU - Sahoo, Trilochan

AU - Sauthier, Philippe

AU - Slim, Rima

N1 - Funding Information: Acknowledgements The authors would like to thank Dr. Olga Basso for her help with the statistical analysis. This study was supported by the Canadian Institutes of Health Research to R.S. (MOP-130364, MOP 102469, and MOP 86546). We also express our gratitude to the Pathology Departments of the following health centers for providing archived products of conception for analyses: McGill University Health Centre, Centre Hospitalier de l’Université de Montréal, Centre Hospitalier Universitaire de Sainte-Justine, Centre de la Santé de Laval, Hôpital Pierre Le Gardeur, Centre Hospitalier Régional de Rimouski, Centre de Santé et de Services Sociaux de Trois Rivières, London Health Science Centre, Hôpital Pierre Boucher, Hôpital Maisonneuve Rosemont, Hôpital Sacré-Coeur, Hôpital Anna-Laberge, Hôpital Général du Lakeshore, Jewish General Hospital, Hôpital Honoré Mercier, Credit Valley Hospital, Hôpital Saint Jean sur Richelieu, Hôpital Regional Saint Jerome, Hôpital Sainte-Mary, and Windsor Regional Hospital. Publisher Copyright: © 2019, The Author(s), under exclusive licence to United States & Canadian Academy of Pathology.

PY - 2020/5/1

Y1 - 2020/5/1

N2 - Hydatidiform mole (HM) is an aberrant human pregnancy characterized by excessive trophoblastic proliferation and abnormal embryonic development. HM has two morphological types, complete (CHM) and partial (PHM), and non-recurrent ones have three genotypic types, androgenetic monospermic, androgenetic dispermic, and triploid dispermic. Most available studies on risk factors predisposing to different types of HM and their malignant transformation mainly suffer from the lack of comprehensive genotypic analysis of large cohorts of molar tissues combined with accurate postmolar hCG follow-up. Moreover, 10–20% of patients with one HM have at least one non-molar miscarriage, which is higher than the frequency of two pregnancy losses in the general population (2–5%), suggesting a common genetic susceptibility to HM and miscarriages. However, the underlying causes of the miscarriages in these patients are unknown. Here, we comprehensively analyzed 204 HM, mostly from patients referred to the Quebec Registry of Trophoblastic Diseases and for which postmolar hCG monitoring is available, and 30 of their non-molar miscarriages. We revisited the risk of maternal age and neoplastic transformation across the different HM genotypic categories and investigated the presence of chromosomal abnormalities in their non-molar miscarriages. We confirm that androgenetic CHM is more prone to gestational trophoblastic neoplasia (GTN) than triploid dispermic PHM, and androgenetic dispermic CHM is more prone to high-risk GTN and choriocarcinoma (CC) than androgenetic monospermic CHM. We also confirm the association between increased maternal age and androgenetic CHM and their malignancies. Most importantly, we demonstrate for the first time that patients with an HM and miscarriages are at higher risk for aneuploid miscarriages [83.3%, 95% confidence interval (CI): 0.653–0.944] than women with sporadic (51.5%, 95% CI: 50.3–52.7%, p value = 0.0003828) or recurrent miscarriages (43.8%, 95% CI: 40.7–47.0%, p value = 0.00002). Our data suggest common genetic female germline defects predisposing to HM and aneuploid non-molar miscarriages in some patients.

AB - Hydatidiform mole (HM) is an aberrant human pregnancy characterized by excessive trophoblastic proliferation and abnormal embryonic development. HM has two morphological types, complete (CHM) and partial (PHM), and non-recurrent ones have three genotypic types, androgenetic monospermic, androgenetic dispermic, and triploid dispermic. Most available studies on risk factors predisposing to different types of HM and their malignant transformation mainly suffer from the lack of comprehensive genotypic analysis of large cohorts of molar tissues combined with accurate postmolar hCG follow-up. Moreover, 10–20% of patients with one HM have at least one non-molar miscarriage, which is higher than the frequency of two pregnancy losses in the general population (2–5%), suggesting a common genetic susceptibility to HM and miscarriages. However, the underlying causes of the miscarriages in these patients are unknown. Here, we comprehensively analyzed 204 HM, mostly from patients referred to the Quebec Registry of Trophoblastic Diseases and for which postmolar hCG monitoring is available, and 30 of their non-molar miscarriages. We revisited the risk of maternal age and neoplastic transformation across the different HM genotypic categories and investigated the presence of chromosomal abnormalities in their non-molar miscarriages. We confirm that androgenetic CHM is more prone to gestational trophoblastic neoplasia (GTN) than triploid dispermic PHM, and androgenetic dispermic CHM is more prone to high-risk GTN and choriocarcinoma (CC) than androgenetic monospermic CHM. We also confirm the association between increased maternal age and androgenetic CHM and their malignancies. Most importantly, we demonstrate for the first time that patients with an HM and miscarriages are at higher risk for aneuploid miscarriages [83.3%, 95% confidence interval (CI): 0.653–0.944] than women with sporadic (51.5%, 95% CI: 50.3–52.7%, p value = 0.0003828) or recurrent miscarriages (43.8%, 95% CI: 40.7–47.0%, p value = 0.00002). Our data suggest common genetic female germline defects predisposing to HM and aneuploid non-molar miscarriages in some patients.

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JO - Modern Pathology

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Comprehensive analysis of 204 sporadic hydatidiform moles: revisiting risk factors and their correlations with the molar genotypes

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