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The Wenner-Gren Institute, The Arrhenius Laboratories F3, Stockholm University, S-106 91 Stockholm, Sweden
To examine
the significance of brown adipose tissue for the thermogenic response
to glucagon, we injected glucagon intraperitoneally into rats (that
have glucagon-sensitive brown fat cells) and into hamsters (that have
glucagon-insensitive brown fat cells). Although a thermogenic response
to glucagon injection was apparently observed in rats, this response
was not augmented by cold acclimation and was not dose dependent.
Similar observations were made in hamsters. The thermogenic response
could be fully blocked by prior injection of the
-adrenergic blocker
propranolol. Thus no direct thermogenic response to injected glucagon
could be demonstrated, and the thermogenic response observed was fully
due to vehicle injection. However, glucagon injection was able to
unmask mitochondrial
[3H]GDP binding. As
expected, isolated brown fat cells from rats and mice responded
thermogenically to glucagon but brown fat cells from hamsters were
unresponsive. The EC50 of the rat
brown fat cells was high (5 nM); these cells also responded to
secretin, with an EC50 of 22 nM.
It was concluded that, in contrast to earlier observations, no
thermogenic response to injected glucagon could be observed; this may
be related to differences in glucagon preparations. Brown fat cells
from certain species are, however, glucagon sensitive. It is uncertain
whether glucagon is the endogenous agonist for these receptors, but the
presence of the glucagon-responsive receptor indicates alternative
means to norepinephrine for stimulation of brown adipose tissue
thermogenesis and, probably, of recruitment.
nonshivering thermogenesis; cold acclimation; guanosine diphosphate binding capacity; propranolol; secretin
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