First custom next-generation sequencing infertility panel in Latin America: design and first results

Lorenzi, Daniela; Fernández, Carolina; Bilinski, Melina; Fabbro, Mónica; Galain, Micaela; Menazzi, Sebastián; Miguens, Mariana; Perassi, Pamela Nicotra; Fulco, María Florencia; Kopelman, Susana; Fiszbajn, G.; Nodar, F.; Papier, S.

doi:10.5935/1518-0557.20190065

Cited by 9 publications

(9 citation statements)

References 49 publications

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“…The elevated number of candidate genes makes it hard to find a genetic cause of infertility in the majority of the cases (22)(23)(24). Anyway, a multi-disease gene panel can improve the identification of the etiology of male infertility (3,25,26). In several cases, idiopathic infertility has a genetic origin, therefore a correct phenotyping and medical history of the infertile patient may represent an initial basis for the genetic interpretation of the disorder (27), especially for the genetic variants of uncertain Severe oligozoospermia was defined for total sperm count <1.0 million; mild oligozoospermia was defined for total sperm count enclosed between 1.0 and 5.0 million; oligozoospermia for total sperm count enclosed between 5.0 and 39.0 million (21).…”

Section: Discussionmentioning

confidence: 99%

Male Infertility Diagnosis: Improvement of Genetic Analysis Performance by the Introduction of Pre-Diagnostic Genes in a Next-Generation Sequencing Custom-Made Panel

Precone¹,

Cannarella

Paolacci

et al. 2021

Front. Endocrinol.

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BackgroundInfertility affects about 7% of the general male population. The underlying cause of male infertility is undefined in about 50% of cases (idiopathic infertility). The number of genes involved in human spermatogenesis is over two thousand. Therefore, it is essential to analyze a large number of genes that may be involved in male infertility. This study aimed to test idiopathic male infertile patients negative for a validated panel of “diagnostic” genes, for a wide panel of genes that we have defined as “pre-diagnostic.”MethodsWe developed a next-generation sequencing (NGS) gene panel including 65 pre-diagnostic genes that were used in 12 patients who were negative to a diagnostic genetic test for male infertility disorders, including primary spermatogenic failure and central hypogonadism, consisting of 110 genes.ResultsAfter NGS sequencing, variants in pre-diagnostic genes were identified in 10/12 patients who were negative to a diagnostic test for primary spermatogenic failure (n = 9) or central hypogonadism (n = 1) due to mutations of single genes. Two pathogenic variants of DNAH5 and CFTR genes and three uncertain significance variants of DNAI1, DNAH11, and CCDC40 genes were found. Moreover, three variants with high impact were found in AMELY, CATSPER 2, and ADCY10 genes.ConclusionThis study suggests that searching for pre-diagnostic genes may be of relevance to find the cause of infertility in patients with apparently idiopathic primary spermatogenic failure due to mutations of single genes and central hypogonadism.

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Section: Discussionmentioning

confidence: 99%

Male Infertility Diagnosis: Improvement of Genetic Analysis Performance by the Introduction of Pre-Diagnostic Genes in a Next-Generation Sequencing Custom-Made Panel

Precone¹,

Cannarella

Paolacci

et al. 2021

Front. Endocrinol.

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“…Some examples also have been illustrated in the development of infertility NGS panel for targeted exons and their flanking regions in 75 infertility related genes, including FSHR as one of the diagnostic genes which have proven associations with infertility, in order to assess the genetic variations of infertile patients with a custom bioinformatic pipeline for data analysis. By applying the MiSeq platform of Illumina, investigators revealed the underlying genetic cause of infertility in their 25 samples properly [ 56 ]. França et al also reviewed the ability of NGS methods in the discovery of heterogeneity of some FSHR and other infertility gene-related disorders and concluded the widespread usage of such technologies in the near future for the detection of new players in female reproduction diseases would be recommended [ 57 ].…”

Section: Advanced Genetic Screening Methods For Fshr Profilingmentioning

confidence: 99%

Pharmacogenomic Biomarkers of Follicle-Stimulating Hormone Receptor Malfunction in Females with Impaired Ovarian Response—A Genetic Survey

Tafazoli

Wołczyński

Wawrusiewicz‐Kurylonek

et al. 2021

JCM

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Follicle-stimulating hormone receptor (FSHR) plays an essential role as one of the most important molecules in response to some of infertility related medications. Impaired ovarian reserve and poor response to such treatments are partially dependent on the FSHR molecule itself. However, the function and drug sensitivity for this receptor may change due to various allele and polymorphisms in the FSHR gene. Studies indicated some of the FSHR-mediated treatments utilized in clinical centers display different outcomes in specific populations, which may arise from FSHR altered genotypes in certain patients. To support the increased demands for reaching the personalized drug and hormone therapy in clinics, focusing on actionable variants through Pharmacogenomic analysis of this receptor may be necessary. The current study tries to display a perspective view on genetic assessments for Pharmacogenomic profiling of the FSHR gene via providing a systematic and critical overview on the genetics of FSHR and its diverse responses to ligands for infertility treatment in females with impaired ovarian responses and show the potential effects of the patient genetic make-up on related binding substances efficacy. All identified functional drug-related alleles were selected through a comprehensive literature search and analyzed. Advanced technologies for the genetic evaluation of them are also discussed properly.

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“…To investigate if rare variants potentially involved in the development of OHSS were present, variants called in the 12 cases with OHSS were filtered using a predefined in silico gene panel including 76 genes predisposing to OHSS (Online Resource 2). The genes included in the gene panel were selected based on an extensive literature search in PubMed and Online Mendelian Inheritance in Man (OMIM) and were implicated in controlled ovarian stimulation response, associated with OHSS or regulation of gonadotropin action and/or ovarian angiogenesis [3,14,[16][17][18][19][20][21][22][23][24]. The gene panel included both known disease-associated genes related to OHSS and candidate genes which association with OHSS needs further study.…”

Section: Analysis I: In Silico Gene Panelmentioning

confidence: 99%

Rare genetic variants suggest dysregulation of signaling pathways in low- and high-risk patients developing severe ovarian hyperstimulation syndrome

Borgwardt

Olsen

Rossing

et al. 2020

J Assist Reprod Genet

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Purpose To investigate if rare gene variants in women with severe ovarian hyperstimulation syndrome (OHSS) provide clues to the mechanisms involved in the syndrome. Methods Among participants in a prospective randomized study (Toftager et al. 2016), six women with predicted low and six women with predicted high risk of OHSS developing severe OHSS (grades 4 and 5, Golan classification) were selected. In the same cohort, six plus six matched controls developing no signs of OHSS (Golan grade 0) were selected. Whole-exome sequencing was performed. Analysis using a predefined in silico OHSS gene panel, variant filtering, and pathway analyses was done. Results We found no convincing monogenetic association with the development of OHSS using the in silico gene panel. Pathway analysis of OHSS variant lists showed substantial overlap in highly enriched top pathways (p value range p < 0.0001 and p > 9.8E-17) between the low-and high-risk group developing severe OHSS, i.e., "the integrin-linked kinase (ILK) signaling pathway" and the "axonal guidance signaling pathway," both being connected to vasoactive endothelial growth factor (VEGF) and endothelial function. Conclusion Rare variants in OHSS cases with two distinct risk profiles enrich the same signaling pathways linked to VEGF and endothelial function. Clarification of the mechanism as well as potentially defining genetic predisposition of the high vascular permeability is important for future targeted treatment and prevention of OHSS; the potential roles of ILK signaling and the axonal guidance signaling need to be validated by functional studies.

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First custom next-generation sequencing infertility panel in Latin America: design and first results

Cited by 9 publications

References 49 publications

Male Infertility Diagnosis: Improvement of Genetic Analysis Performance by the Introduction of Pre-Diagnostic Genes in a Next-Generation Sequencing Custom-Made Panel

Male Infertility Diagnosis: Improvement of Genetic Analysis Performance by the Introduction of Pre-Diagnostic Genes in a Next-Generation Sequencing Custom-Made Panel

Pharmacogenomic Biomarkers of Follicle-Stimulating Hormone Receptor Malfunction in Females with Impaired Ovarian Response—A Genetic Survey

Rare genetic variants suggest dysregulation of signaling pathways in low- and high-risk patients developing severe ovarian hyperstimulation syndrome

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