Among numerous mechanisms implicated in the regulation of orofacial movements, dopamine-containing neurons have received the most extensive study. Here we review the effects of a) constitutive knockout of D
1–5 dopamine receptors and b) conditional mutations with progressive ablation of D
1 receptor–expressing cells, on the topography of spontaneous and D
1-like agonist–induced orofacial movements. In constitutive knockouts, D
1 and D
2 exert primary roles in regulating horizontal and vertical jaw movements, respectively, in opposite directions; in contrast, both D
1 and D
2 receptors regulate tongue protrusions and incisor chattering, in the same direction. D
3 and D
5 receptors play more subtle roles in regulating orofacial movements, while D
4 receptors do not play any material role. Progressive loss of forebrain D
1 receptor–expressing cells in CamKIIa/Cre D
1Tox mutants is associated primarily with decreases in head and vibrissae movements, while progressive loss of striatal D
1 receptor–expressing cells in DARPP-32/Cre D
1Tox mutants is associated primarily with reductions in jaw movements and tongue protrusions but increases in head and vibrissae movements. Further application of constitutive and particularly conditional mutants may clarify further not only dopaminergic regulation of orofacial movements but also the pathophysiology of orofacial dysfunction in Huntington’s disease and Parkinson’s disease.
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