Flushing Clinical Trial
Official title:
Exploring the Role of Prostaglandin D2 and the DP1 Receptor on Nicotinic Acid Induced Flushing
This study will focus on investigating the nicotinic acid stimulated release of prostaglandin D2 in normal controls. In subsequent studies, the investigators would like to further explore this pathway in people with type 2 diabetes. Enhanced blood flow (or flushing) may be compromised or exaggerated in type 2 diabetes particularly in those with impairment of autonomic function measured as the respiratory heart rate variability (HRV) of different frequencies reflecting the balance between the sympathetic and parasympathetic nervous systems. The investigators hypothesize that the vasodilatory effects induced by nicotinic acid will be different in glabrous and hairy skin and that autonomic imbalance may alter the response.
The investigators propose that nicotinic acid (NA) stimulates release of prostaglandin D2
(PGD2). To fully understand this mechanism, the investigators will examine the systemic
release of PGD2 and skin blood flow using laser Doppler (LDF) on the upper and lower limbs
of healthy control subjects. The investigators will quantify and establish the effects of
oral nicotinic acid (Niaspan®) given alone and in combination with aspirin on:
1. skin blood flow using laser Doppler (LDF) of glabrous and hairy skin of the forearm of
healthy subjects
2. the severity and intensity of flushing using a visual analog scale, FAST tool, and
whether aspirin is able to block the flushing response
3. the impact on sympathetic/parasympathetic balance using the various frequencies of
heart rate variability (HRV) which reflect the contribution of the different divisions
of the autonomic nervous system (ANS)
4. circulating levels of PGD2 and other neuropeptides to determine other mediators of the
flushing response. This will allow us to conclude whether this pathway is intact and
explore other non-DP1 vasodilatory mechanisms.
5. Langerhans cell density in epidermis and microvasculature using immunohistochemistry of
Langerin (measured as CD1a) in 3 mm skin biopsies of volar and hairy surfaces of the
forearm and hairy surface of the lateral aspect of proximal lower limb. To date, there
is very little known about the density or distribution of Langerhans cells. The PGD2
receptor DP1 will be examined for its content in the epidermis using
immunohistochemistry or RTPCR.
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