Acylation-stimulating Protein (ASP)/Complement C3adesArg Deficiency Results in Increased Energy Expenditure in Mice

Xia, Zhunan; Stanhope, Kimber L.; Digitale, Erin; Simion, Oana Maria; Chen, Lan‐Ying; Havel, Peter J.; Cianflone, Katherine

doi:10.1074/jbc.m311319200

Cited by 70 publications

(79 citation statements)

References 56 publications

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“…Based on a number of studies in mice and adipocytes, ASP enhances adipose fat storage through increased fatty acid esterification (for review see Kalant et al 2 and Cianflone et al 7 ). ASP deficiency (C3 knockout mice) results in decreased adipose tissue and delayed postprandial TG clearance, [17][18][19][20][21] while acute administration of ASP increases postprandial TG clearance. [15][16][17]19 Related to glucose metabolism, ASP increases glucose transport in adipocytes and myotubes through translocation of GLUT1, GLUT3 and GLUT4.…”

Section: Discussionmentioning

confidence: 99%

“…ASP deficiency (C3 knockout mice) results in decreased adipose tissue and delayed postprandial TG clearance, [17][18][19][20][21] while acute administration of ASP increases postprandial TG clearance. [15][16][17]19 Related to glucose metabolism, ASP increases glucose transport in adipocytes and myotubes through translocation of GLUT1, GLUT3 and GLUT4. [61][62][63] As well, ASP has recently been demonstrated to stimulate insulin secretion from islet cells both ex vivo and in vivo.…”

Section: Discussionmentioning

confidence: 99%

“…[11][12][13] While no direct role for C3 has been proposed, ASP appears to be an important determinant of postprandial lipemia in both human 14 and mouse models. [15][16][17][18][19] In complement C3(À/À) ASP-deficient mice, the lack of ASP results in delayed postprandial triglyceride clearance, which is normalized acutely through ASP injection. The mice are characterized by reduced adipose tissue with a compensatory upregulation of energy expenditure.…”

Section: Introductionmentioning

confidence: 99%

“…The mice are characterized by reduced adipose tissue with a compensatory upregulation of energy expenditure. [17][18][19][20][21] Adiponectin is a hormone secreted exclusively from adipose tissue. It is thought to enhance insulin sensitivity by stimulating hepatic glucose utilization and reducing plasma nonesterified fatty acid levels (NEFA) (for a review, see Ukkola and Santaniem 22 ).…”

Section: Introductionmentioning

confidence: 99%

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Relationships among acylation stimulating protein, adiponectin and complement C3 in lean vs obese type 2 diabetes

et al. 2005

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Objective: The purpose of this study was to determine the relationships between adipocyte hormones acylation stimulating protein (ASP), adiponectin, complement C3 (C3) (ASP precursor) and insulin, C-reactive protein (CRP), lipid profiles and insulin resistance in lean vs obese type 2 diabetes subjects. Subjects: Lean type 2 diabetes subjects (DL n ¼ 27) vs obese type 2 diabetes subjects (DO n ¼ 55) were compared to agematched nondiabetic groups (Obese, OB n ¼ 55 and control, CTL n ¼ 50).Results: The DO group demonstrated significant increases in plasma ASP and C3 with decreases in plasma adiponectin as compared to CTL. Interestingly, these increases in ASP and C3 were as high, or greater, in the DL group in spite of normal weight. By contrast adiponectin in the DL group was comparable to CTL, in spite of marked insulin resistance. C3 correlated with insulin, glucose and homeostasis model assessment of insulin resistance (HOMA-IR); ASP correlated with body mass index (BMI), glucose, insulin and plasma lipid parameters (non-esterified fatty acids (NEFA), triglyceride, cholesterol and apolipoprotein B). Adiponectin correlated with BMI, glucose, NEFA, triglyceride, high-density lipoprotein cholesterol and apolipoprotein A1 but not HOMA-IR, ASP or C3. CRP correlated only with HOMA-IR. Conclusion: Increased ASP and C3 are both associated with diabetes and related lipid factors but are not regulated coordinately. Adiponectin appears to be more closely related to body size (decreased in obese subjects) than insulin resistance in these subjects.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Relationships among acylation stimulating protein, adiponectin and complement C3 in lean vs obese type 2 diabetes

et al. 2005

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“…Mice with C3 and ASP deficiencies show resistance to weight gain despite increased food intake [14]. These animals also have increased energy expenditure [30]. However, it is unclear to what extent circulating C3 reflects the concentrations in the adipose tissue.…”

Section: Discussionmentioning

confidence: 99%

Weight gain in relation to plasma levels of complement factor 3: results from a population-based cohort study

et al. 2005

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Aims/hypothesis: Mice that are deficient for complement factor 3 (C3) have shown resistance to weight gain, despite increased food intake. Cross-sectional studies of humans have reported correlations between C3 and obesity. This longitudinal study explored whether C3 predicts a large weight gain in middle-aged men. Methods: Plasma concentrations of C3 and complement factor 4 (C4) were measured in 2,706 non-diabetic healthy men aged between 38 and 50 years, who were re-examined after a mean period of 6.1 years. Results: After adjustments for initial weight, age, height and follow-up time, the odds of incurring large weight gain (75th percentile, ≥3.8 kg) were 1.00 (reference), 0.96 (95% CI:0.7-1.2), 1.1 (CI:0.9-1.5) and 1.4 (CI: 1.1-1.8), respectively, among men with C3 levels in the first, second, third and fourth quartiles (p for trend= 0.01) respectively. This relationship remained significant after further adjustments for lifestyle factors (physical inactivity, alcohol, smoking), metabolic factors (glucose or homeostasis model assessment values, cholesterol, triglycerides), inflammatory markers (fibrinogen, haptoglobin, ceruloplasmin, orosomucoid, α1-antitrypsin) and for C4. C4 was associated with weight gain after adjustments for initial weight, height, follow-up time and lifestyle factors, but not after adjustments for C3. Conclusions/interpretation: C3 is a risk factor for incurring large weight gain in middleaged men.

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Adipose Organ Development and Remodeling

Cinti

2018

Comprehensive Physiology

142

121

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During the last decades, research on adipose tissues has spread in parallel with the extension of obesity. Several observations converged on the idea that adipose tissues are organized in a large organ with endocrine and plastic properties. Two parenchymal components: white (WATs) and brown adipose tissues (BATs) are contained in subcutaneous and visceral compartments. Although both have endocrine properties, their function differs: WAT store lipids to allow intervals between meals, BAT burns lipids for thermogenesis. In spite of these opposite functions, they share the ability for reciprocal reversible transdifferentiation to tackle special physiologic needs. Thus, chronic need for thermogenesis induces browning and chronic positive energy balance induce whitening. Lineage tracing and data from explant studies strongly suggest other remodeling properties of this organ. During pregnancy and lactation breast WAT transdifferentiates into milk-secreting glands, composed by cells with abundant cytoplasmic lipids (pink adipocytes) and in the postlactation period pink adipocytes transdifferentiate back into WAT and BAT. The plastic properties of mature adipocytes are supported also by a liposecretion process in vitro where adult cell in culture transdifferentiate to differentiated fibroblast-like elements able to give rise to different phenotypes (rainbow adipocytes). In addition, the inflammasome system is activated in stressed adipocytes from obese adipose tissue. These adipocytes die and debris are reabsorbed by macrophages inducing a chronic low-grade inflammation, potentially contributing to insulin resistance and T2 diabetes. Thus, the plastic properties of this organ could open new therapeutic perspectives in the obesity-related metabolic disease and in breast pathologies. © 2018 American Physiological Society. Compr Physiol 8:1357-1431, 2018.

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Acylation-stimulating Protein (ASP)/Complement C3adesArg Deficiency Results in Increased Energy Expenditure in Mice

Cited by 70 publications

References 56 publications

Relationships among acylation stimulating protein, adiponectin and complement C3 in lean vs obese type 2 diabetes

Relationships among acylation stimulating protein, adiponectin and complement C3 in lean vs obese type 2 diabetes

Weight gain in relation to plasma levels of complement factor 3: results from a population-based cohort study

Adipose Organ Development and Remodeling

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