Genetic and Epigenetic Profiling of the Infertile Male

Evaluation of the reproductive quality of the male gamete by standard semen analysis is often inadequate to predict ART outcome. Men may be prone to meiotic error and have a higher proportion of spermatozoa with fragmented chromatin that is capable of affecting the conceptus' health. In men with unexplained infertility, supplementary tests may be pivotal to gain insight into the paternal contribution to the zygotic genome.A total of 113 consenting men were included in the study with an additional 5 donor specimens used as a control. Among the study participants, 87 were screened for sperm aneuploidy by fluorescent in situ hybridization (FISH) and ranked according to their increasing age. A total of 18 men were assessed by whole exome sequencing and categorized according to their reproductive outcome as either fertile or infertile. Another set of men (n=10) had their gene expression analyzed by RNA-seq and were profiled according to their reproductive capacity in comparison to three couples utilizing a proven fertile donor specimen.FISH revealed that the average aneuploidy rate was highest for men in the over-55 age group (9.6%), while men over 55 had the highest average disomy for chromosomes 17 (1.2%) and 18 (1.3%). ART results for the entire cohort comprised of 157 cycles, stratified by paternal age. The youngest age group (25-30 years old) had a fertilization rate of 87.7% which decreased to 46.0% in the over-55 age group. Clinical pregnancy rate was highest in the 25-30 age group (80.0%) while no pregnancies were attained in the over-55 age groups. Pregnancy loss was characterized by a steadily increasing trend, highest in the 51-55 age group (50.0%).NGS was performed on a cohort of patients classified as having recurrent pregnancy loss. This cohort was classified as the infertile group (n=10) and was compared to a control group (n=8) consisting of patients successfully treated by ART. Eight couples in 17 ICSI cycles achieved a clinical pregnancy rate of 82.4% while 10 infertile couples treated in 21 cycles achieved a pregnancy rate of only 23.8%, all resulting in pregnancy loss. DNA sequencing on the spermatozoa from these patients yielded an overall aneuploidy of 4.0% for the fertile and 8.6% for the infertile group (PRNA sequencing was performed on a group of patients (n=10) with normal semen analyses. Five men unable to attain a pregnancy after ART were categorized as the infertile group, while 5 men who successfully sustained a pregnancy were categorized as the fertile group. Analysis was performed in comparison to a control group (n=3) and resulted in 86 differentially expressed genes (PSperm aneuploidy assessment supported by information on specific gene mutations may indicate the subtle dysfunctions of the spermatozoon. Furthermore, by querying non-coding RNA we may gather knowledge on the embryo developmental competence of the male gamete, providing crucial information on the etiology of unexplained infertility of the infertile male.