W Cameron’s research while affiliated with Tufts Medical Center and other places

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Publications (3)


Histamine type I (H1) receptor radioligand binding studies on normal T cell subsets, B cells, and monocytes
  • Article

April 1986

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5 Reads

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55 Citations

The Journal of Immunology

W Cameron

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We have documented a single, specific binding site for [3H]pyrilamine on normal human T helper, T suppressor, B cells, and monocytes. The binding of the radioligand to its receptor is reversible with cold H1 antagonist, saturates at 40 to 60 nM, and binding equilibrium is achieved in 2 to 4 min. Using a computer program (Ligand), we calculated the dissociation constants, binding capacities, and numbers of receptors per cell for each of the different cell types. Monocytes were found to have the highest affinity (mean KD +/- SD; 3.8 +/- 4.8 nM) for [3H]pyrilamine, followed by T helper cells (KD = 5.0 +/- 6.6 nM), B cells (KD = 14.2 +/- 2.0 nM), and T suppressor cells (KD = 44.6 +/- 49.4 nM). T suppressor cells were found to express the higher number of H1 receptors per cell (35,697 +/- 15,468), followed by B cells (10,732 +/- 9060), T helper cells (6838 +/- 8167), and monocytes (5589 +/- 2266). The kinetics of binding for this radioligand was carried out in resting and mitogen-stimulated T cells over a 48-hr period. We found that the binding affinity for [3H]pyrilamine increased over the 48-hr period, whereas the number of receptors per T cell was essentially unchanged. In contrast, T cells stimulated with Con A or PHA were shown to have a greater than fourfold increase in the number of receptors per cell, whereas the binding affinity for [3H]pyrilamine decreased over the 48-hr period. Preincubation of T cells with unlabeled histamine before carrying out the radioligand binding assay resulted in a decrease in the binding affinity of the receptors to [3H]pyrilamine, but the number of receptors per cell did not change significantly. Although the function of H1 receptors on T cells, B cells, and monocytes has not been completely defined, this receptor has the potential of playing an important role in modulating the immune response.



Citations (2)


... In addition, it inhibits IFN-, TNF-, and IL-12 and enhances IL-10 synthesis in LPS-or mitogen-activated, peripheral blood mononuclear cells [374,376], and increases IL-1 stimulated synthesis of IL-6 by monocytes [377]. These complex impacts of histamine were found to be mediated through the activation of H1R [378], H2R [374], and H3R on immune cell cytokine synthesis [330]. Recently, cloned H4R has been characterized as functionally active to modulate cytokines [274,284,285]. ...

Reference:

Histamine, Histamine Receptors, and their Role in Immunomodulation: An Updated Systematic Review
Histamine type I (H1) receptor radioligand binding studies on normal T cell subsets, B cells, and monocytes
  • Citing Article
  • April 1986

The Journal of Immunology

... Any reintroduction of a drug in a patient who has experienced a hypersensitivity reaction has an inherent risk that the same reaction might occur again. Although rarely experienced and described in the literature, more severe symptoms or more extensive manifestations may be elicited (40,41). In HIV patients with exanthems to sulfonamides, the develop- The protocol is analogously used for other antibiotics (total of 192 procedures on 42 patients between 2004 and 2008). ...

A complicated case of penicillin allergy
  • Citing Article
  • January 1985

Annals of Allergy