Abstract
Simple SummaryPancreatic cancer (PDAC) is a deadly disease, exacerbated by obesity, which lacks effective therapeutic interventions. Most PDAC has a limited response to immune- and chemotherapy. Treating PDAC is made additionally challenging by the rapid emergence of muscle wasting and cachexia, which predict poor response to several therapies. We have found that dietary supplementation with β-hydroxy-β-methylbutyrate promotes immunosurveillance in PDAC tumors and protects muscle. This dietary supplement has the potential to be an important adjuvant in PDAC therapy, opening the doors to immunotherapy response.Pancreatic ductal adenocarcinoma (PDAC) is the fourth leading cause of cancer-related deaths in the United States, and effective therapies for PDAC are currently lacking. Moreover, PDAC is promoted and exacerbated by obesity, while cachexia and sarcopenia are exceptionally common comorbidities that predict both poor survival and treatment response. Managing PDAC with immunotherapies has thus far proven ineffective, partly due to the metabolically hostile tumor microenvironment. β-hydroxy-β-methylbutyrate (HMB), a metabolite of leucine commonly used as a dietary supplement to boost muscle growth and immune function, may be an attractive candidate to augment PDAC therapy. We therefore sought to test the hypothesis that HMB would enhance antitumor immunity while protecting mouse muscle mass. Control and diet-induced obese C57BL/6 male mice bearing subcutaneously injected Panc02 tumors were supplemented with 1% HMB and treated with or without 50 mg/kg gemcitabine (n = 15/group). HMB was associated with reduced muscle inflammation and increased muscle fiber size. HMB also reduced tumor growth and promoted antitumor immunity in obese, but not lean, mice, independent of the gemcitabine treatment. Separately, in lean tumor-bearing mice, HMB supplementation promoted an anti-PD1 immunotherapy response (n = 15/group). Digital cytometry implicated the decreased abundance of M2-like macrophages in PDAC tumors, an effect that was enhanced by anti-PD1 immunotherapy. We confirmed that HMB augments M1-like macrophage (antitumor) polarization. These preclinical findings suggest that HMB has muscle-sparing and antitumor activities against PDAC in the context of obesity, and that it may sensitize otherwise nonresponsive PDAC to immunotherapy.
Highlights
Pancreatic ductal adenocarcinoma (PDAC) is the fourth leading cause of cancerrelated deaths in the United States
A growing proportion of patients with pancreatic cancer are obese at the start of therapy, and many of these individuals have sarcopenic obesity, a condition characterized by the presence of a high fat mass but a low muscle mass
Obesity in the presence of sarcopenia is predictive of morbidity and mortality in patients with pancreatic cancer [9], at least in part because sarcopenic obesity increases the risk of developing cancer cachexia [10]
Summary
Pancreatic ductal adenocarcinoma (PDAC) is the fourth leading cause of cancerrelated deaths in the United States. This high mortality rate is exacerbated by the limited efficacy of chemotherapies and immunotherapies [1]. Cancer-associated cachexia, defined by involuntary weight loss and breakdown of adipose and muscle tissue, is present in about 80% of patients with pancreatic cancer and contributes significantly to PDAC mortality [4,5]. Obesity in the presence of sarcopenia is predictive of morbidity and mortality in patients with pancreatic cancer [9], at least in part because sarcopenic obesity increases the risk of developing cancer cachexia [10]
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