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SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences

Disclosure: R. Santos: None. G. Parodi: None. G. Leite: None. W. Morales: None. S.R. Weitsman: None. G. Barlow: None. I. Rivera: None. M. Sanchez: None. D. Flor: None. L. Choi: None. S.L. Gonzales: None. F. Faria: None. M. Villanueva-Millan: None. M. Pimentel: None. R. Mathur: None. Polycystic ovary...

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Autores principales: Santos, Roberta, Parodi, Gonzalo, Leite, Gabriela, Morales, Walter, Weitsman, Stacy R, Barlow, Gillian, Rivera, Ignacio, Sanchez, Maritza, Flor, Dilara, Choi, Linette, Gonzales, Sophia L, Faria, Flavio, Villanueva-Millan, Maria Jesus, Pimentel, Mark, Mathur, Ruchi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10555233/
http://dx.doi.org/10.1210/jendso/bvad114.1676
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author Santos, Roberta
Parodi, Gonzalo
Leite, Gabriela
Morales, Walter
Weitsman, Stacy R
Barlow, Gillian
Rivera, Ignacio
Sanchez, Maritza
Flor, Dilara
Choi, Linette
Gonzales, Sophia L
Faria, Flavio
Villanueva-Millan, Maria Jesus
Pimentel, Mark
Mathur, Ruchi
author_facet Santos, Roberta
Parodi, Gonzalo
Leite, Gabriela
Morales, Walter
Weitsman, Stacy R
Barlow, Gillian
Rivera, Ignacio
Sanchez, Maritza
Flor, Dilara
Choi, Linette
Gonzales, Sophia L
Faria, Flavio
Villanueva-Millan, Maria Jesus
Pimentel, Mark
Mathur, Ruchi
author_sort Santos, Roberta
collection PubMed
description Disclosure: R. Santos: None. G. Parodi: None. G. Leite: None. W. Morales: None. S.R. Weitsman: None. G. Barlow: None. I. Rivera: None. M. Sanchez: None. D. Flor: None. L. Choi: None. S.L. Gonzales: None. F. Faria: None. M. Villanueva-Millan: None. M. Pimentel: None. R. Mathur: None. Polycystic ovary syndrome (PCOS) is a major endocrine disorder affecting ∼12% of reproductive age women. It has diverse clinical manifestations, including hyperandrogenism, ovarian dysfunction and enlargement, infertility, insulin resistance, and others. The role of the gut microbiome in PCOS is poorly understood. We previously found higher testosterone (T) levels in PCOS stool samples vs. controls and identified bacterial candidates that correlated with testosterone levels. Here, we further investigate the role of one candidate microbe, Rothia sp., in the development of PCOS-like phenotypes. Methods: The presence of androgen biosynthesis associated genes in Rothia sp. was confirmed by RT-PCR. Rothia sp. was cultured in M9 minimal medium plus cholesterol. T production in the supernatant was measured by LC-MS/MS. Next, reproductive-age female rats were gavaged with 10(6) CFU/mL Rothia or with PBS (controls) daily for 2 weeks. H&E stained slides from daily vaginal lavages were used to assess estrous cycles. Serum T and progesterone (P) levels were measured by LC-MS/MS, and insulin levels by ELISA. Ovaries, uteri, and cardiac blood were harvested. Results: Genes encoding proteins associated with T biosynthesis (cytochrome P450, 3-beta hydroxysteroid dehydrogenase/isomerase family protein and NAD(P)H steroid dehydrogenase-like protein) were detected in Rothia sp. T production in Rothia sp. cultures was confirmed, with levels from 3.2±0.01 pg/mL after 48 hrs to 8.9±0.02 pg/mL after 6 days. T was not detected in negative controls (P<0.001). In gavaged rats, analysis of vaginal slides (controls n=10; Rothia n=10) revealed a disruption of estrous cycles in Rothia rats, with 68% of days in luteal phase (metestrus & diestrus) vs. 46% in controls (P=0.001). The predominance of luteal phase days in Rothia rats was driven by longer time in diestrus (1.96 vs 1.67 days in controls, P=0.04), and shorter time in estrus (1.24 vs 1.91 days in controls, P=0.001). Peak P and T levels occurred in diestrus in both groups. Rothia rats spent more days in diestrus, and the cumulative exposure times to P (P=0.046) and T (P=0.036) in the diestrus phase were significantly higher in Rothia rats vs controls. Final serum insulin levels were higher in Rothia rats (1.8±0.5 ng/dL) vs controls (1.0±0.1 ng/dL; P=0.07). Rothia rats also had heavier ovaries vs controls (0.128±0.007g vs 0.097±0.01g; P=0.07), and higher uterus weights (0.48±0.04g vs. 0.36±0.04g; P=0.04). Conclusion: Here we show that a specific Rothia sp. can produce testosterone in vitro. Gavaging female rats with this microbe results in PCOS-like phenotypes, including higher insulin levels, enlarged ovaries, significant disruption of reproductive cycles and longer exposure to peak progesterone and testosterone. This longer exposure to peak progesterone and testosterone may result in reproductive and metabolic sequelae that warrant further investigation. Presentation Date: Saturday, June 17, 2023
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spelling pubmed-105552332023-10-06 SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences Santos, Roberta Parodi, Gonzalo Leite, Gabriela Morales, Walter Weitsman, Stacy R Barlow, Gillian Rivera, Ignacio Sanchez, Maritza Flor, Dilara Choi, Linette Gonzales, Sophia L Faria, Flavio Villanueva-Millan, Maria Jesus Pimentel, Mark Mathur, Ruchi J Endocr Soc Reproductive Endocrinology Disclosure: R. Santos: None. G. Parodi: None. G. Leite: None. W. Morales: None. S.R. Weitsman: None. G. Barlow: None. I. Rivera: None. M. Sanchez: None. D. Flor: None. L. Choi: None. S.L. Gonzales: None. F. Faria: None. M. Villanueva-Millan: None. M. Pimentel: None. R. Mathur: None. Polycystic ovary syndrome (PCOS) is a major endocrine disorder affecting ∼12% of reproductive age women. It has diverse clinical manifestations, including hyperandrogenism, ovarian dysfunction and enlargement, infertility, insulin resistance, and others. The role of the gut microbiome in PCOS is poorly understood. We previously found higher testosterone (T) levels in PCOS stool samples vs. controls and identified bacterial candidates that correlated with testosterone levels. Here, we further investigate the role of one candidate microbe, Rothia sp., in the development of PCOS-like phenotypes. Methods: The presence of androgen biosynthesis associated genes in Rothia sp. was confirmed by RT-PCR. Rothia sp. was cultured in M9 minimal medium plus cholesterol. T production in the supernatant was measured by LC-MS/MS. Next, reproductive-age female rats were gavaged with 10(6) CFU/mL Rothia or with PBS (controls) daily for 2 weeks. H&E stained slides from daily vaginal lavages were used to assess estrous cycles. Serum T and progesterone (P) levels were measured by LC-MS/MS, and insulin levels by ELISA. Ovaries, uteri, and cardiac blood were harvested. Results: Genes encoding proteins associated with T biosynthesis (cytochrome P450, 3-beta hydroxysteroid dehydrogenase/isomerase family protein and NAD(P)H steroid dehydrogenase-like protein) were detected in Rothia sp. T production in Rothia sp. cultures was confirmed, with levels from 3.2±0.01 pg/mL after 48 hrs to 8.9±0.02 pg/mL after 6 days. T was not detected in negative controls (P<0.001). In gavaged rats, analysis of vaginal slides (controls n=10; Rothia n=10) revealed a disruption of estrous cycles in Rothia rats, with 68% of days in luteal phase (metestrus & diestrus) vs. 46% in controls (P=0.001). The predominance of luteal phase days in Rothia rats was driven by longer time in diestrus (1.96 vs 1.67 days in controls, P=0.04), and shorter time in estrus (1.24 vs 1.91 days in controls, P=0.001). Peak P and T levels occurred in diestrus in both groups. Rothia rats spent more days in diestrus, and the cumulative exposure times to P (P=0.046) and T (P=0.036) in the diestrus phase were significantly higher in Rothia rats vs controls. Final serum insulin levels were higher in Rothia rats (1.8±0.5 ng/dL) vs controls (1.0±0.1 ng/dL; P=0.07). Rothia rats also had heavier ovaries vs controls (0.128±0.007g vs 0.097±0.01g; P=0.07), and higher uterus weights (0.48±0.04g vs. 0.36±0.04g; P=0.04). Conclusion: Here we show that a specific Rothia sp. can produce testosterone in vitro. Gavaging female rats with this microbe results in PCOS-like phenotypes, including higher insulin levels, enlarged ovaries, significant disruption of reproductive cycles and longer exposure to peak progesterone and testosterone. This longer exposure to peak progesterone and testosterone may result in reproductive and metabolic sequelae that warrant further investigation. Presentation Date: Saturday, June 17, 2023 Oxford University Press 2023-10-05 /pmc/articles/PMC10555233/ http://dx.doi.org/10.1210/jendso/bvad114.1676 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of the Endocrine Society. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (https://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Reproductive Endocrinology
Santos, Roberta
Parodi, Gonzalo
Leite, Gabriela
Morales, Walter
Weitsman, Stacy R
Barlow, Gillian
Rivera, Ignacio
Sanchez, Maritza
Flor, Dilara
Choi, Linette
Gonzales, Sophia L
Faria, Flavio
Villanueva-Millan, Maria Jesus
Pimentel, Mark
Mathur, Ruchi
SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title_full SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title_fullStr SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title_full_unstemmed SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title_short SAT371 Gavaging Adult Female Rats with Rothia sp. Leads to Profound Disruption of the Estrous Cycles and Metabolic Consequences
title_sort sat371 gavaging adult female rats with rothia sp. leads to profound disruption of the estrous cycles and metabolic consequences
topic Reproductive Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10555233/
http://dx.doi.org/10.1210/jendso/bvad114.1676
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