4.7 Article

Unique Deep Radiomic Signature Shows NMN Treatment Reverses Morphology of Oocytes from Aged Mice

Journal

BIOMEDICINES
Volume 10, Issue 7, Pages -

Publisher

MDPI
DOI: 10.3390/biomedicines10071544

Keywords

oocyte; aging; morphology; machine learning; NMN

Funding

  1. Australian Research Council [CE140100003, DP170101863]
  2. National Health and Medical Research Council [APP1139763, APP1117538, APP1127821, APP1122484, APP1103689, APP1093643]
  3. NSW cancer Institute [ECF1291]
  4. Jumpstart Fertility

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The purpose of this study is to develop a deep radiomic signature based on an artificial intelligence model, which can accurately identify oocyte morphological changes associated with reproductive aging. By employing deep learning, swarm intelligence, and discriminative analysis, a highly informative signature was obtained and applied to distinguish oocytes from different age groups. The results showed that the signature could successfully differentiate morphological changes in oocytes, reflecting the decline in oocyte quality.
The purpose of this study is to develop a deep radiomic signature based on an artificial intelligence (AI) model. This radiomic signature identifies oocyte morphological changes corresponding to reproductive aging in bright field images captured by optical light microscopy. Oocytes were collected from three mice groups: young (4- to 5-week-old) C57BL/6J female mice, aged (12-month-old) mice, and aged mice treated with the NAD+ precursor nicotinamide mononucleotide (NMN), a treatment recently shown to rejuvenate aspects of fertility in aged mice. We applied deep learning, swarm intelligence, and discriminative analysis to images of mouse oocytes taken by bright field microscopy to identify a highly informative deep radiomic signature (DRS) of oocyte morphology. Predictive DRS accuracy was determined by evaluating sensitivity, specificity, and cross-validation, and was visualized using scatter plots of the data associated with three groups: Young, old and Old + NMN. DRS could successfully distinguish morphological changes in oocytes associated with maternal age with 92% accuracy (AUC similar to 1), reflecting this decline in oocyte quality. We then employed the DRS to evaluate the impact of the treatment of reproductively aged mice with NMN. The DRS signature classified 60% of oocytes from NMN-treated aged mice as having a 'young' morphology. In conclusion, the DRS signature developed in this study was successfully able to detect aging-related oocyte morphological changes. The significance of our approach is that DRS applied to bright field oocyte images will allow us to distinguish and select oocytes originally affected by reproductive aging and whose quality has been successfully restored by the NMN therapy.

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