. 2025 Jun;46(6):659-669.

doi: 10.15537/smj.2025.46.6.20250205.

Identification of genetic variants in patients with primary and secondary amenorrhea

Flora Bai¹, Renjini Nambiar¹, Chirayu Padhiar¹, Wilson Aruni¹, Chinnadurai Veeramani¹, Mohammed A Alsaif¹, Khalid S Al-Numair¹

Affiliations

Affiliation

¹ From the Department of Biotechnology (Bai), Sathyabama Institute of Science and Technology, Chennai; from the Cytogenetics Department (Bai, Nambiar) and Department of Biologics (Padhiar), LifeCell International Private Ltd, Chennai; from the Department of Biotechnology (Aruni), Amity University, Mumbai, India; from the Department of Community Health Sciences (Veeramani, Alsaif, Al-Numair), College of Applied Medical Sciences, King Saud University, Riyadh, Kingdom of Saudi Arabia; and from the Musculoskeletal Disease Research Centre (Aruni), Loma Linda Veterans Affairs, United States of America.

PMID: 40516947
PMCID: PMC12199654
DOI: 10.15537/smj.2025.46.6.20250205

Identification of genetic variants in patients with primary and secondary amenorrhea

Flora Bai et al. Saudi Med J. 2025 Jun.

. 2025 Jun;46(6):659-669.

doi: 10.15537/smj.2025.46.6.20250205.

Authors

Flora Bai¹, Renjini Nambiar¹, Chirayu Padhiar¹, Wilson Aruni¹, Chinnadurai Veeramani¹, Mohammed A Alsaif¹, Khalid S Al-Numair¹

Affiliation

¹ From the Department of Biotechnology (Bai), Sathyabama Institute of Science and Technology, Chennai; from the Cytogenetics Department (Bai, Nambiar) and Department of Biologics (Padhiar), LifeCell International Private Ltd, Chennai; from the Department of Biotechnology (Aruni), Amity University, Mumbai, India; from the Department of Community Health Sciences (Veeramani, Alsaif, Al-Numair), College of Applied Medical Sciences, King Saud University, Riyadh, Kingdom of Saudi Arabia; and from the Musculoskeletal Disease Research Centre (Aruni), Loma Linda Veterans Affairs, United States of America.

PMID: 40516947
PMCID: PMC12199654
DOI: 10.15537/smj.2025.46.6.20250205

Abstract

Objectives: To identify the cytogenetic and molecular pattern abnormalities and early diagnose the cause of primary and secondary amenorrhea.

Methods: A total of 320 patients in the age group of 14-35 years with clinically confirmed amenorrhea were screened using conventional cytogenetic methods. Patients with a normal karyotype, hypoplastic uterus, and no hormonal imbalance were extensively investigated using molecular cytogenetic platforms such as chromosomal microarrays and clinical exome sequencing (CES).

Results: Of the 266 patients with primary amenorrhea and 54 with secondary amenorrhea, 66.9% and 88.9%, independently, had a normal karyotype. The 20 patients with a normal karyotype, hypoplastic uterus, and no hormonal imbalance were further evaluated for microdeletions of <5 megabases using chromosomal microarray. In 20 cases, 5 samples with no microdeletions were investigated for 150 target genes using CES. A pathogenic variant at chromosome X BMP15, c.661T>C, p.W221R, HET-XL-VUS was observed in one patient (reclassification).

Conclusion: Cytogenetic evaluation of women with amenorrhea was performed in this study. One of the main etiological factors for primary amenorrhea is aberrant karyotypes. Identifying the underlying genetic cause may aid in devising effective treatment strategies. In addition, early diagnosis may enable treatment planning by the family before amenorrhea occurs.

Keywords: amenorrhea; chromosomal abnormalities; chromosomal microarray; clinical exome sequencing; karyotyping.

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Figures

**Figure 1**
- Representative karyotypes of primary amenorrhea patients

**Figure 2**
- Clinical features of pure Turner syndrome with 45,X karyotype

**Figure 3**
- Clinical features of XY (DSD) karyotype. This figure represents the prevalence of secondary sexual characteristics and internal reproductive structures among the study (n=32). The x-axis enumerates 6 assessed features: axillary hair, pubic hair, breast development, right gonad, left gonad, Müllerian structures. For each feature, the blue bar indicates the number of individuals in whom the feature was absent, while the red bar shows the number of individuals in whom the feature was present.

**Figure 4**
- Representative image of clinical exome sequencing with BMP15, c.661T>C, p.W221R, HET-XL-VUS.

See this image and copyright information in PMC

References

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Identification of genetic variants in patients with primary and secondary amenorrhea

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Identification of genetic variants in patients with primary and secondary amenorrhea

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