Single cell RNA-sequencing suggests a novel lipid-associated mast cell population following weight cycling.

Munira Kapadia, Alexa M Betjemann, Matthew A Cottam, Mona Mashayekhi, Heidi J Silver, Alyssa H Hasty, Heather L Caslin
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Abstract

We previously demonstrated that weight cycled mice have increased adipose mast cells compared to obese mice by single cell RNA-sequencing. Here, we aimed to confirm and elucidate these changes. Interestingly, we did not detect an increase in total mast cell numbers in weight cycled mice by Toluidine blue or flow cytometry, however, further subcluster analysis of our dataset showed that our initial mast cell cluster consisted of two unique populations. One population had very high expression of classical mast cell markers and another had elevated lipid handling and antigen presentation genes with a concomitant reduction in classical mast cell genes. This new "lipid-associated" mast cell cluster accounted for most of the mast cells in the weight cycled group. We induced a similar phenotype in vitro using repeated exposure to adipose tissue conditioned media to mimic weight gain and weight regain. Upon repeated exposure to adipose tissue conditioned media, bone marrow-derived mast cells had increased lipid droplets and reduced expression of cKit and FcεR1 compared to control cells. Moreover, we analyzed mast cells in a pilot study of subcutaneous adipose tissue from four obese, prediabetic women. We found two mast cell populations that appear similar to the murine populations detected by sequencing. The population with reduced cKit and FcεR1 was significantly correlated with weight variance. Together, these data suggest that weight cycling may induce a unique population of mast cells similar to lipid- associated macrophages, which have been shown to play a role in diverse diseases from obesity and atherosclerosis to Alzheimer's disease. Future studies will focus on isolation of these cells from mice and humans to better determine their lineage, differentiation, and functional roles.

单细胞rna测序提示体重循环后出现一种新的脂质相关肥大细胞群。
我们最近的研究表明,通过单细胞rna测序,体重循环小鼠的脂肪肥大细胞比肥胖小鼠增加。在这里,我们的目的是确认和阐明这些变化。对我们的数据集的进一步分析表明,我们的初始肥大细胞簇可以亚簇成两个独特的群体:一个具有非常高的经典肥大细胞标记表达,另一个具有升高的脂质处理和抗原呈递基因。这种新的肥大细胞簇占体重循环组肥大细胞的大部分,尽管在小鼠中使用流式细胞术或甲苯胺蓝染色的新研究无法检测到不同的群体,可能是由于经典肥大细胞基因的下调。有趣的是,一项针对人类的初步研究确实表明,肥胖女性皮下脂肪组织中存在两种肥大细胞群,这与通过测序检测到的小鼠群体相似;其中一项与权重方差显著相关。总之,这些数据表明,体重循环可能会诱导一种独特的肥大细胞群,类似于脂质相关巨噬细胞。未来的研究将集中于这些细胞的分离,以更好地确定它们的谱系、分化和功能作用。
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