Infertility and pregnancy outcomes among adults with primary ciliary dyskinesia.

Schreck, Leonie D; Pedersen, Eva S L; Dexter, Katie; Manion, Michele; Massin, Nathalie; Maitre, Bernard; Goutaki, Myrofora; Kuehni, Claudia E (2024). Infertility and pregnancy outcomes among adults with primary ciliary dyskinesia. Human reproduction open, 2024(3), hoae039. Oxford University Press 10.1093/hropen/hoae039

[img]
Preview
Text
hoae039.pdf - Published Version
Available under License Creative Commons: Attribution (CC-BY).

Download (842kB) | Preview

STUDY QUESTION

What is the prevalence of infertility and ectopic pregnancies among individuals with primary ciliary dyskinesia (PCD)?

SUMMARY ANSWER

We found that 39 of 50 men (78%) and 72 of 118 women (61%) with PCD were infertile and that women with PCD had an increased risk of ectopic pregnancies (7.6 per 100 pregnancies, 95% CI 4.7-12.2).

WHAT IS KNOWN ALREADY

PCD is a heterogeneous multiorgan disease caused by mutations in genes required for the function and structure of motile cilia. Previous studies identified a link between PCD and infertility, but original data on prevalence of infertility and risk of ectopic pregnancies, the use and efficacy of medically assisted reproduction (MAR), and the association of fertility with PCD genotype are extremely limited.

STUDY DESIGN SIZE DURATION

We performed a cross-sectional survey about fertility within the Living with PCD study (formerly COVID-PCD). Living with PCD is an international, online, participatory study that collects information directly from people with PCD. People with PCD of any age from anywhere in the world can participate in the study. At the time of the survey, 482 adults with PCD were registered within the Living with PCD study.

PARTICIPANTS/MATERIALS SETTING METHODS

We sent a questionnaire on fertility on 12 July 2022, to all participants older than 18 years enrolled in the Living with PCD study. Responses were collected until 8 March 2023. The fertility questionnaire covered topics related to pregnancy attempts, use of MAR, and pregnancy outcomes. Data were collected via the Research Electronic Data Capture (REDCap) platform. We defined infertility as failure to achieve a clinical pregnancy after 12 months or use of MAR for at least one pregnancy.

MAIN RESULTS AND THE ROLE OF CHANCE

In total, 265 of 482 adult participants (55%) completed the fertility questionnaire. Among 168 adults who had tried to conceive, 39 of 50 men (78%) and 72 of 118 women (61%) were infertile. Of the infertile men, 28 had tried MAR, and 17 of them (61%) fathered a child with the help of MAR. Among infertile women, 59 had used MAR, and 41 of them (69%) became pregnant with the help of MAR. In our population, women with PCD showed a relatively high risk of ectopic pregnancies: 1 in 10 women who became pregnant had at least one ectopic pregnancy and 7.6% of pregnancies were ectopic (95% CI 4.7-12.2). We evaluated the association between fertility and affected PCD genes in 46 individuals (11 men, 35 women) with available genetic and fertility information, and found differences between genotypes, e.g. all five women with a mutation in CCDC40 were infertile and all five with DNAH11 were fertile.

LIMITATIONS REASONS FOR CAUTION

The study has limitations, including potential selection bias as people experiencing problems with fertility might be more likely to fill in the questionnaire, which may have influenced our prevalence estimates. We were unable to validate clinical data obtained from participant self-reports owing to the anonymous study design, which is likely to lead to recall bias.

WIDER IMPLICATIONS OF THE FINDINGS

The study underlines the need for addressing infertility in routine PCD care, with a focus on informing individuals with PCD about their increased risk. It emphasizes the utility and efficacy of MAR in PCD-related infertility. Additionally, women attempting conception should be made aware of the increased risk of ectopic pregnancies and seek systematic early consultation to confirm an intrauterine pregnancy. Fertility, efficacy of MAR, and risk for adverse pregnancy outcomes differ between people with PCD-depending on genotypes-and close monitoring and support might be needed from fertility specialists to increase chances of successful conception.

STUDY FUNDING/COMPETING INTERESTS

Our research was funded by the Swiss National Science Foundation, Switzerland (SNSF 320030B_192804), the Swiss Lung Association, Switzerland (2021-08_Pedersen), and we also received support from the PCD Foundation, USA; the Verein Kartagener Syndrom und Primäre Ciliäre Dyskinesie, Germany; the PCD Support UK, UK; and PCD Australia, Australia. M. Goutaki received funding from the Swiss National Science Foundation, Switzerland (PZ00P3_185923). B. Maitre participates in the RaDiCo-DCP funded by INSERM France. The study authors participate in the BEAT-PCD Clinical Research Collaboration supported by the European Respiratory Society. All authors declare no conflict of interest.

TRIAL REGISTRATION NUMBER

ClinicalTrials.gov ID NCT04602481.

Item Type:

Journal Article (Original Article)

Division/Institute:

04 Faculty of Medicine > Department of Gynaecology, Paediatrics and Endocrinology (DFKE) > Clinic of Paediatric Medicine
04 Faculty of Medicine > Pre-clinic Human Medicine > Institute of Social and Preventive Medicine (ISPM)

Graduate School:

Graduate School for Health Sciences (GHS)

UniBE Contributor:

Schreck, Leonie Daria, Pedersen, Eva Sophie Lunde, Goutaki, Myrofora, Kühni, Claudia

Subjects:

600 Technology > 610 Medicine & health
300 Social sciences, sociology & anthropology > 360 Social problems & social services

ISSN:

2399-3529

Publisher:

Oxford University Press

Funders:

[4] Swiss National Science Foundation ; [204] Swiss Lung Association = Lungenliga Schweiz

Language:

English

Submitter:

Pubmed Import

Date Deposited:

04 Jul 2024 16:28

Last Modified:

10 Jul 2024 16:32

Publisher DOI:

10.1093/hropen/hoae039

PubMed ID:

38962571

Uncontrolled Keywords:

assisted reproduction ectopic pregnancy epidemiology genotype infertility orphan disease primary ciliary dyskinesia

BORIS DOI:

10.48350/198528

URI:

https://boris.unibe.ch/id/eprint/198528

Actions (login required)

Edit item Edit item
Provide Feedback