Melanocortin-4 receptor antagonist TCMCB07 ameliorates cancer- and chronic kidney disease–associated cachexia
Xinxia Zhu, … , Marek Szumowski, Daniel L. Marks
Xinxia Zhu, … , Marek Szumowski, Daniel L. Marks
Published June 16, 2020
Citation Information: J Clin Invest. 2020;130(9):4921-4934. https://doi.org/10.1172/JCI138392.
View: Text | PDF
Research Article Metabolism

Melanocortin-4 receptor antagonist TCMCB07 ameliorates cancer- and chronic kidney disease–associated cachexia

Abstract

Cachexia, a devastating wasting syndrome characterized by severe weight loss with specific losses of muscle and adipose tissue, is driven by reduced food intake, increased energy expenditure, excess catabolism, and inflammation. Cachexia is associated with poor prognosis and high mortality and frequently occurs in patients with cancer, chronic kidney disease, infection, and many other illnesses. There is no effective treatment for this condition. Hypothalamic melanocortins have a potent and long-lasting inhibitory effect on feeding and anabolism, and pathophysiological processes increase melanocortin signaling tone, leading to anorexia, metabolic changes, and eventual cachexia. We used 3 rat models of anorexia and cachexia (LPS, methylcholanthrene sarcoma, and 5/6 subtotal nephrectomy) to evaluate efficacy of TCMCB07, a synthetic antagonist of the melanocortin-4 receptor. Our data show that peripheral treatment using TCMCB07 with intraperitoneal, subcutaneous, and oral administration increased food intake and body weight and preserved fat mass and lean mass during cachexia and LPS-induced anorexia. Furthermore, administration of TCMCB07 diminished hypothalamic inflammatory gene expression in cancer cachexia. These results suggest that peripheral TCMCB07 treatment effectively inhibits central melanocortin signaling and therefore stimulates appetite and enhances anabolism, indicating that TCMCB07 is a promising drug candidate for treating cachexia.

Authors

Xinxia Zhu, Michael F. Callahan, Kenneth A. Gruber, Marek Szumowski, Daniel L. Marks

×

Figure 4

Administration of TCMCB07 s.c. ameliorates anorexia and body weight loss in rats with cancer cachexia.

Options: View larger image (or click on image) Download as PowerPoint
Administration of TCMCB07 s.c. ameliorates anorexia and body weight loss...
(A) Daily food intake in tumor/saline group (n = 8) versus tumor/TCMCB07L (low dose) group (n = 8), tumor/TCMCB07H (high dose) group (n = 8), and sham/saline group (n = 9) after tumor implantation or sham operation. Rats received s.c. injection once (1×) or twice (2×) daily with saline or TCMCB07L (1.5 mg/kg/d) or TCMCB07H (3 mg/kg/d) between day 6 and day 12 after implantation. (B) Cumulative food intake before and after treatment. (C) Body weight gain after treatment (%, tumor-free net gain normalized to baseline of day 6). (D) Tumors were dissected and weighed after animals were euthanized on day 12. (E) Terminal plasma TCMCB07 concentrations were measured by reverse-phase HPLC. All data in A are expressed as mean ± SEM for each group, and all data in BE are expressed with each dot representing 1 sample. Two-way ANOVA in A and for sham/saline group was excluded for 2-way ANOVA analysis in order to clearly show a treatment comparison among 3 tumor groups (tumor/saline, tumor/TCMCB07L, tumor/TCMCB07H) (A). *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001; #P < 0.05; ##P < 0.01; ###P < 0.001, 1-way ANOVA (BD); unpaired Student’s t test (E). Yellow asterisks in A show tumor/TCMCB07L group versus tumor/saline group, and red pound signs in A show tumor/TCMCB07H group versus tumor/saline group.