Delineating muscarinic receptor functions.
نویسندگان
چکیده
A as the first chemical molecule to be established as a neurotransmitter, has attracted enduring interest from researchers over several decades. However, deciphering all of the physiological manifestations associated with actions of this molecule has been difficult, and many mysteries of cholinergic neurotransmission still remain to be resolved. Like many other neurotransmitters, the actions of acetylcholine are mediated by both ionotropic and metabotropic receptors. Within these two classes of receptors, a large amount of heterogeneity has been discovered that further complicates the assignment of specific physiological functions (1, 2). Five different subtypes (M1–M5) of G proteincoupled muscarinic receptors have been identified and characterized. The M1, M3, and M5 subtypes couple to the GqyG11 family of G-proteins whereas M2 and M4 preferentially interact with the GiyGo family (2, 8). Aside from being involved in the control of many peripheral cholinergic responses, muscarinic receptors significantly contribute to a variety of centrally mediated functions, such as locomotion, learning and memory, regulation of circadian rhythm, antinociception, generation of epileptic seizures, and thermoregulation (1, 2). The involvement of muscarinic transmission in a variety of physiological responses has accelerated the pace for the development of muscarinic drugs as the pharmacotherapeutic strategies for treatment of several disorders, such as Parkinson’s and Alzheimer’s diseases (1). However, most common muscarinic pharmacological agents have significant drawbacks because of their high degree of unwanted side effects. These limitations are mainly attributable to a lack of subtype selectivity of the available agents for the individual muscarinic receptors, and this is compounded by the lack of information about the functional specificity of these receptor subtypes as well as their overlapping pattern of expression in the many tissues of the body. The study by Gomeza et al. (5), which uses the approach of inactivating an individual gene in the mouse by homologous recombination, should greatly help in resolving not only the issue of receptor subtype specificity but also the complex issue of neuronal circuit interaction. It was convincingly demonstrated that M4 muscarinic receptor deficient mice do not show altered responses to muscarinic agonist-induced receptor activation such as analgesia, tremor, hypothermia, and salivation. Surprisingly, though, these mice showed an increase in basal locomotor activity and greatly enhanced locomotor responses after activation of D1 dopamine receptors. Thus, to date, genetic deletion of the M1 (6), M2 (4), and M4 (5) receptor genes have been reported. The muscarinic receptor functions found to be affected in the mutants are summarized in Table 1. Although information from the genetic deletion approach is not yet available for the M3 and M5 muscarinic receptor subtypes, interesting generalizations can already be made about the physiological actions of various subtypes. Particularly, the classic central responses to muscarinic agonists, such as tremor, analgesia, a major part of hypothermic responses, as well as cardiac responses can be decisively attributed to M2 subtype stimulation. Muscarinic agonist-induced seizures and Mcurrents in sympathetic ganglion neurons have been associated with the M1 subtype; however, studies on other receptor subtype knockout mice will be required to confirm an exclusive role for this subtype in these functions. Pharmacological investigations have connected the M3 receptor with salivation responses (1, 2), and, indeed, muscarinic agonist-induced salivation was found to be preserved in M1, M2, and M4 receptor knockout mice (4–6). Although this connection may also need direct confirmation from a similar approach with the M3 receptor subtype, the current map of muscarinic receptor function has already provided invaluable information, which will undoubtedly facilitate the development and characterization of more specific pharmacological agents. Besides clarifying the specific role of the receptor proteins in the whole animal, knockout models are increasingly valuable in assessing neuronal circuitry and neurotransmitter interactions. An important observation presented by Gomeza et al. in mice lacking M4 muscarinic receptors is supersensitivity of dopamine receptors, particularly the D1 subtype (5). This supersensitivity was accompanied by a mild locomotor hyperactivity. From multiple pharmacological, anatomical, and electrophysiological studies, it has become evident that muscarinic cholinergic and dopaminergic functions might interact (3, 7, 9). There are several potential levels of these interactions, determined by both preand postsynaptic localization of muscarinic receptors and an important role of intrastriatal cholinergic interneurons in striatal neuronal organization (3). A cellular colocalization of the dopaminergic and muscarinic receptors on striatal medium spiny g-aminobutyric acid neurons and cholinergic interneurons has been well established. In clinical practice, anticholinergic drugs are commonly used as a therapy to treat Parkinson’s disease symptoms and extrapyramidal side effects associated with chronic neuroleptic treatment (1, 3). However, despite decades of research, the precise mechanism that underlies this cholinergic-dopaminergic interaction is still unknown. The paper by Gomeza et al. (5) sheds light on this relatively poorly understood phenomenon. The authors suggest that, in normal animals, M4 muscarinic receptors located on striatonigral projection neurons can counteract the increase in neuronal activity after D1 receptor activation (5). Thus, in these mice, the observed hyperactivity and D1 receptor supersensitivity may be caused by increased activity of the striatonigral pathway because of the lack of inhibitory striatal M4 receptors. These findings highlight a putative interaction between these two neurotransmitter systems. Although the molecular events underlying this interaction are not obviously apparent, many possibilities exist. First, colocalization of the receptors on the same cellular components in the striatum suggests the possibility of a direct interaction between muscarinic and dopaminergic receptors at the level of Gproteins andyor intracellular signaling. Another possibility might involve the well established role of cholinergic interneurons in the striatum, the major locomotor
منابع مشابه
MUSCARINIC RECEPTOR SUBTYPES IN SMOOTH MUSCLE FROM THE BODY OF HUMAN STOMACH
Up to date, there are four pharmacologically characterized subtypes of muscarinic receptors (M1, M2, M3 and M4). In our study we have investigated muscarinic receptor subtypes in smooth muscle layers of human stomach. Isolated preparations of longitudinal and circular muscle layers from human stomach were used. Acetylcholine, bethanechol, carbachol, pilocarpine and AHR -602 produced concen...
متن کاملBiological behaviors of muscarinic receptors in mesenchymal stem cells derived from human placenta and bone marrow
Objective(s): Cells perform their functional activities by communicating with each other through endogenous substances and receptors. Post-translation, stem cells function properly in new host tissue by carrying specific cell surface receptors. We aimed to characterize muscarinic receptor subtypes in mesenchymal stem cells (MSCs) together with osteogenic and adipogenic...
متن کاملImportance and prospects for design of selective muscarinic agonists.
There are five subtypes of muscarinic receptors that serve various important physiological functions in the central nervous system and the periphery. Mental functions like attention, learning, and memory are attributed to the muscarinic M1 subtype. These functions decline during natural aging and an early deficit is typical for Alzheimer s disease. In addition, stimulation of the M1 receptor in...
متن کاملInvolvement of Dorsal Hippocampal Muscarinic Cholinergic Receptors of CA1 Area on Anxiety Induced by Iron Oxide Nanoparticles in Adult Male Rats
Introduction: Recent findings revealed the biological effects of iron oxide nanoparticles on the central nervous system. Moreover, the brain cholinergic system plays a role in the modulation of anxiety behaviors. Therefore, this study aimed to evaluate the role of dorsal hippocampal muscarinic cholinergic receptors of the CA1 area on anxiety induced by iron oxide nanoparticles in adult male rat...
متن کاملAcetylcholine modifies neuronal acoustic rate-level functions in guinea pig auditory cortex by an action at muscarinic receptors.
Cholinergic modification of neuronal responsiveness in auditory cortex includes alteration of spontaneous and tone-evoked neuronal discharge. Previously it was suggested that the effects of acetylcholine (ACh) and muscarinic agonists on neuronal discharge resembled those due to increases in the intensity of acoustic stimuli (Ashe et al. 1989). To determine the relationship between neuronal modi...
متن کاملذخیره در منابع من
با ذخیره ی این منبع در منابع من، دسترسی به آن را برای استفاده های بعدی آسان تر کنید
برای دانلود متن کامل این مقاله و بیش از 32 میلیون مقاله دیگر ابتدا ثبت نام کنید
ثبت ناماگر عضو سایت هستید لطفا وارد حساب کاربری خود شوید
ورودعنوان ژورنال:
- Proceedings of the National Academy of Sciences of the United States of America
دوره 96 22 شماره
صفحات -
تاریخ انتشار 1999