Publications by authors named "Seldin M"

Unlabelled: Polycystic ovary syndrome (PCOS) is a complex condition with clear genetic susceptibilities that impact the heterogeneous clinical presentation of symptoms and severity through unknown mechanisms. Chronic inflammation is linked to PCOS, but a clear cause-and-effect relationship has yet to be established. This study used an in depth systems immunology approach and a letrozole-induced PCOS mouse model to identify changes in inflammatory factors associated with PCOS symptoms.

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Importance: African Americans have a higher prevalence of Type 2 Diabetes (T2D) compared to White groups. T2D is a health disparity clinically characterized by dysregulation of lipids and chronic inflammation. However, how the relationships among biological and sociological predictors of T2D drive this disparity remains to be addressed.

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  • Peripancreatic adipose tissue (PAT), which accumulates with obesity, negatively affects metabolic health and beta cell function, highlighting its significance compared to subcutaneous adipose tissue (SAT).
  • PAT secretes higher levels of inflammatory substances and certain adipokines linked to poor metabolic outcomes, with variations in islet insulin secretion observed between male and female donors.
  • RNA sequencing reveals that PAT influences gene transcription and lipid metabolism in islets in a sex-dependent manner, suggesting different metabolic impacts compared to SAT.
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  • Chronic stress disrupts circadian rhythms, which can lead to mental and metabolic health issues; this study investigates how chronic social stress affects the circadian regulation of brain and liver functions in mice.
  • Male mice underwent chronic social defeat stress, and their behaviors were analyzed to identify stress resilience and susceptibility, with tissue samples collected for further study every 4 hours.
  • Findings suggest that resilient mice exhibit improved circadian transcription patterns and metabolic rhythms across different tissues, indicating better coordination between brain and liver functions compared to those susceptible to stress.
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Cellular heterogeneity of human adipose tissue, is linked to the pathophysiology of obesity and may impact the response to energy restriction and changes in fat mass. Here, we provide an optimized pipeline to estimate cellular composition in human abdominal subcutaneous adipose tissue (ASAT) from publicly available bulk RNA-Seq using signature profiles from our previously published full-length single nuclei (sn)RNA-Seq of the same depot. Individuals with obesity had greater proportions of macrophages and lower proportions of adipocyte sub-populations and vascular cells compared with lean individuals.

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  • White adipose tissue (WAT) plays a crucial role in storing lipids and maintaining energy balance, making adipocyte formation and stability important for addressing obesity and metabolic disorders.
  • Researchers identified PATZ1 as a significant adipogenic transcription factor involved in the development of adipocytes, as it promotes adipogenesis through specific protein interactions and DNA binding.
  • Experiments revealed that removing PATZ1 in mice resulted in decreased adipocyte precursor cells and fat mass, highlighting its essential regulatory role in adipocyte differentiation and overall fat tissue development.
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Diet is a robust entrainment cue that regulates diurnal rhythms of the gut microbiome. We and others have shown that disruption of the circadian clock drives the progression of colorectal cancer (CRC). While certain bacterial species have been suggested to play driver roles in CRC, it is unknown whether the intestinal clock impinges on the microbiome to accelerate CRC pathogenesis.

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Background: Physical activity has been associated with preventing the development of type 2 diabetes and atherosclerotic cardiovascular disease. However, our understanding of the precise molecular mechanisms underlying these effects remains incomplete and good biomarkers to objectively assess physical activity are lacking.

Methods: We analyzed 3072 serum proteins in 26 men, normal weight or overweight, undergoing 12 weeks of a combined strength and endurance exercise intervention.

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Activation-induced cytidine deaminase (AID) is a B cell-specific mutator required for antibody diversification. However, it is also implicated in the etiology of several B cell malignancies. Evaluating the AID-induced mutation load in patients at-risk for certain blood cancers is critical in assessing disease severity and treatment options.

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  • - The circadian clock plays a crucial role in regulating the immune system and is important for both disease defense and cancer detection.
  • - Research using single-cell RNA sequencing reveals that certain immune cells, particularly PD-L1-expressing myeloid-derived suppressor cells (MDSCs), oscillate in numbers based on the time of day and suppress the activity of CD8 T cells.
  • - Timing the administration of anti-PD-L1 treatment to coincide with the peak levels of MDSCs enhances its effectiveness, highlighting the importance of circadian rhythms in cancer immunotherapy.
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Several classification systems have been developed to define tumor subtypes in colorectal cancer (CRC). One system proposes that tumor heterogeneity derives in part from distinct cancer stem cell populations that co-exist as admixtures of varying proportions. However, the lack of single cell resolution has prohibited a definitive identification of these types of stem cells and therefore any understanding of how each influence tumor phenotypes.

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Introduction: Female reproductive function depends on a choreographed sequence of hormonal secretion and action, where specific stresses such as inflammation exert profound disruptions. Specifically, acute LPS-induced inflammation inhibits gonadotropin production and secretion from the pituitary, thereby impacting the downstream production of sex hormones. These outcomes have only been observed in acute inflammatory stress and little is known about the mechanisms by which chronic inflammation affects reproduction.

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  • Inter-organ communication is essential for maintaining physiological balance, and disruptions in this process can lead to various diseases, making serum bioactive factors significant targets for treatment and biomarker discovery.
  • Recent studies utilize RNA sequencing to identify secreted proteins involved in inter-tissue signaling, allowing researchers to analyze gene variations that affect signaling across metabolic tissues.
  • A new web resource, GD-CAT, allows users to easily explore gene correlations across multiple tissues, revealing important connections in metabolic pathways and tissue-specific variations related to health and disease.
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  • Colorectal cancer is a leading cause of cancer deaths, and resistance to oxaliplatin, a key chemotherapy drug, leads to tumor recurrence.
  • Researchers developed oxaliplatin-resistant LoVo cell lines and found that miR-29a-3p levels were significantly higher in these resistant cells and in tumor tissues compared to normal tissues.
  • Overexpression of miR-29a-3p causes oxaliplatin resistance by downregulating FEM1B, which leads to higher levels of the oncogene Gli1, resulting in reduced sensitivity to the drug and decreased DNA damage in resistant cells.
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Endogenous retroviruses (ERVs) are remnants of ancient parasitic infections and comprise sizable portions of most genomes. Although epigenetic mechanisms silence most ERVs by generating a repressive environment that prevents their expression (heterochromatin), little is known about mechanisms silencing ERVs residing in open regions of the genome (euchromatin). This is particularly important during embryonic development, where induction and repression of distinct classes of ERVs occur in short temporal windows.

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Quantitative traits are often complex because of the contribution of many loci, with further complexity added by environmental factors. In medical research, systems genetics is a powerful approach for the study of complex traits, as it integrates intermediate phenotypes, such as RNA, protein, and metabolite levels, to understand molecular and physiological phenotypes linking discrete DNA sequence variation to complex clinical and physiological traits. The primary purpose of this review is to describe some of the resources and tools of systems genetics in humans and rodent models, so that researchers in many areas of biology and medicine can make use of the data.

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Obesity is a major risk factor for type 2 diabetes, dyslipidemia, cardiovascular disease, and hypertension. Intriguingly, there is a subset of metabolically healthy obese (MHO) individuals who are seemingly able to maintain a healthy metabolic profile free of metabolic syndrome. The molecular underpinnings of MHO, however, are not well understood.

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Objective: Tissue crosstalk mediated by secreted hormones underlies the integrative control of metabolism. We previously showed that CTRP13/C1QL3, a secreted protein of the C1q family, can improve glucose metabolism and insulin action in vitro and reduce food intake and body weight in mice when centrally delivered. A role for CTRP13 in regulating insulin secretion in isolated islets has also been demonstrated.

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Balance between metabolic and reproductive processes is important for survival, particularly in mammals that gestate their young. How the nervous system coordinates this balance is an active area of study. Herein, we demonstrate that somatostatin (SST) neurons of the tuberal hypothalamus alter feeding in a manner sensitive to metabolic and reproductive states in mice.

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Activation-induced cytidine deaminase (AID) is a B cell-specific base editor required during class switch recombination and somatic hypermutation for B cell maturation and antibody diversification. However, it has also been implicated as a factor in the etiology of several B cell malignancies. Evaluating the AID-induced mutation load in patients at-risk for certain types of blood cancers is critical in assessing disease severity and treatment options.

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