Insulin Resistance, Hyperinsulinemia, and Mitochondria Dysfunction in Nonobese Girls With Polycystic Ovarian Syndrome

Cree-Green, Melanie; Rahat, Haseeb; Newcomer, Bradley R.; Bergman, Bryan C.; Brown, Mark S.; Coe, Gregory; Newnes, Lindsey; Garcia‐Reyes, Yesenia; Bacon, Samantha; Thurston, Jessica; Pyle, Laura; Scherzinger, Ann; Nadeau, Kristen J.

doi:10.1210/js.2017-00192

Cited by 70 publications

(66 citation statements)

References 51 publications

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“…One proposed mechanism that could disrupt this balance is through mitochondrial dysfunction, characterized by mitochondrial DNA (mtDNA) depletion. It has been associated with the pathogenesis of PCOS, including hyperglycemia, insulin resistance, hyperandrogenism, and anovulation . mtDNA depletion downregulates adiponectin expression, while it stabilizes CTRP6 mRNA, inhibiting its decay .…”

Section: Discussionmentioning

confidence: 99%

Circulating levels of C1q/TNF‐α‐related protein 6 (CTRP6) in polycystic ovary syndrome

et al. 2020

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Polycystic ovary syndrome (PCOS) is one of the most common endocrine disorders affecting females of reproductive age. It has been associated with cardiometabolic disorders including diabetes mellitus and cardiovascular disorders, and increases the risk of developing fecundity pathologies including recurrent pregnancy loss (RPL) and infertility. C1q/tumor necrosis factor‐α‐related protein‐6 (CTRP6) is a novel adipokine involved in glucose and lipid metabolism, host inflammation, and organogenesis. In the present study, we aimed to determine the association of serum CTRP6 levels with some components of metabolic syndrome in PCOS patients (infertile PCOS [inf‐PCOS] and PCOS‐RPL). This case–control study included 120 PCOS patients (60 inf‐PCOS and 60 PCOS‐RPL) and 60 healthy controls. Serum high‐sensitivity C‐reactive protein (hs‐CRP) and homocysteine were measured using commercial kits, while adiponectin and CTRP6 levels were assessed using ELISA technique. Inf‐PCOS and PCOS‐RPL individuals had higher levels of serum CTRP6 than controls (546.15 ± 125.02 ng/ml and 534.04 ± 144.19 ng/ml vs. 440.16 ± 159.24 ng/ml; both p < .001). Moreover, serum adiponectin levels were significantly reduced, while fasting insulin, homeostasis model assessment of insulin resistance, free testosterone, and hs‐CRP levels were significantly elevated in PCOS group, when compared with controls. Furthermore, serum CTRP6 positively associated with body mass index in all subjects. It showed an inverse correlation with adiponectin in PCOS group and subgroups. However, it had a direct association with hs‐CRP in PCOS group and inf‐PCOS subgroup, but not PCOS‐RPL subgroup. These findings unravel a probable role of CTRP6 in PCOS pathogenesis, which poses a possibility to be a good diagnostic target. However, further investigation is needed.

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Section: Discussionmentioning

confidence: 99%

Circulating levels of C1q/TNF‐α‐related protein 6 (CTRP6) in polycystic ovary syndrome

et al. 2020

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“…Furthermore, it stands to reason that the propagation of these mitochondria from a fertilized egg to a blastocyst and ultimately a live-born offspring should result in abnormal mitochondrial function throughout the body. Recent studies in a rat PCOS model have noted mitochondrial dysfunction in the pancreas (57) and kidney (58), and human studies have now reported altered mitochondrial function in skeletal muscle (59) as well as follicular fluid and cumulus cells of PCOS patients (46).…”

Section: Figurementioning

confidence: 99%

Prenatal androgen induced lean PCOS impairs mitochondria and mRNA profiles in oocytes

Chappell

Zhou

Schutt

et al. 2020

Endocrine Connections

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Polycystic ovary syndrome (PCOS) is the most common ovulatory defect in women. Although most PCOS patients are obese, a subset of PCOS women are lean but show similar risks for adverse fertility outcomes. A lean PCOS mouse model was created using prenatal androgen administration. This developmentally programmed mouse model was used for this study. Our objective was to investigate if mitochondrial structure and functions were compromised in oocytes obtained from lean PCOS mouse. The lean PCOS mouse model was validated by performing glucose tolerance test, HbA1c levels, body weight and estrous cycle analyses. Oocytes were isolated and were used to investigate inner mitochondrial membrane potential, oxidative stress, lipid peroxidation, ATP production, mtDNA copy number, transcript abundance and electron microscopy. Our results demonstrate that lean PCOS mice have similar weight to that of the controls but exhibit glucose intolerance and hyperinsulinemia along with dysregulated estrus cycle. Analysis of their oocytes show impaired inner mitochondrial membrane function, elevated reactive oxygen species (ROS) and increased RNA transcript abundance. Electron microscopy of the oocytes showed impaired mitochondrial ultrastructure. In conclusion, the lean PCOS mouse model shows a decreased oocyte quality related to impaired mitochondrial ultrastructure and function.

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“…Data from youth aged 12 to 21 years recruited from the RESistance to InSulin in Type 1 ANd Type 2 diabetes (RESISTANT) study and the Androgens and Insulin Resistance Study (AIRS) cohorts (studies performed prior to ClinicalTrials.gov identifier requirements) were used for this secondary data analysis. Inclusion criteria were BMI ≥ 95th percentile specific for sex and age for the group with obesity, BMI = 10th to 84th percentile for the normal‐weight participants in the control group, and sedentary status, to minimize impacts of varying physical activity on IS (< 3 hours of regular exercise per week, validated with both a 3‐day activity recall and 7 days of accelerometer use).…”

Section: Methodsmentioning

confidence: 99%

“…Informed consent was obtained from all participants ≥ 18 years of age, and parental consent and participant assent were obtained from all participants < 18 years of age. The two groups included in this secondary analysis were originally enrolled as the normal‐weight control group to match those with type 1 diabetes and lean PCOS participants and the control group with obesity to match those with PCOS and T2D participants with obesity. The comparison of the two different weight control groups has not been performed.…”

Section: Methodsmentioning

confidence: 99%

Muscle Insulin Resistance in Youth with Obesity and Normoglycemia is Associated with Altered Fat Metabolism

Cree‐Green

Wiromrat

Stuppy

et al. 2019

Obesity

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Objective This study aimed to phenotype and compare adipose, hepatic, and muscle insulin sensitivity (IS) in a diet‐ and physical activity–controlled cohort of normoglycemic youth with obesity with that of participants without obesity (controls) to distinguish early metabolic abnormalities in pediatric obesity. Methods Thirty‐eight participants (17 in the control group [BMI < 85th percentile] and 21 youth with obesity [BMI ≥ 95th percentile]; age: 12‐21 years; 76% female; Tanner stage 4‐5; sedentary) were enrolled. Tissue‐specific IS was measured using a four‐phase hyperinsulinemic‐euglycemic clamp with glucose and glycerol isotope tracers to assess suppression of endogenous glucose release and lipolysis by insulin. Intramyocellular lipid content was assessed by 1H–magnetic resonance spectroscopy, and hepatic fat fraction (HFF) and visceral fat were assessed by magnetic resonance imaging. Calf‐muscle mitochondrial activity was measured with exercise‐stimulated 31P–magnetic resonance spectroscopy. Results Youth with obesity had higher HFF (P < 0.001), visceral fat (P = 0.024), and intramyocellular lipid content (P = 0.017) and lower muscle (glucose clearance rate [P < 0.001]), adipose (P < 0.0001), and hepatic IS (P < 0.003). Mitochondria postexercise response was not different. In participants with obesity, muscle IS inversely correlated with HFF (r = 0.700, P = 0.002) and suppressed free fatty acid concentrations (r = −0.65, P = 0.003). Conclusions Inactive normoglycemic youth with obesity had decreased muscle, adipose, and hepatic IS. Free fatty acids and liver fat were inversely associated with muscle IS, which argues for lipid‐targeted interventions.

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Insulin Resistance, Hyperinsulinemia, and Mitochondria Dysfunction in Nonobese Girls With Polycystic Ovarian Syndrome

Cited by 70 publications

References 51 publications

Circulating levels of C1q/TNF‐α‐related protein 6 (CTRP6) in polycystic ovary syndrome

Circulating levels of C1q/TNF‐α‐related protein 6 (CTRP6) in polycystic ovary syndrome

Prenatal androgen induced lean PCOS impairs mitochondria and mRNA profiles in oocytes

Muscle Insulin Resistance in Youth with Obesity and Normoglycemia is Associated with Altered Fat Metabolism

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