ライフサイエンスコーパス: Renshaw cell

1 both transmitters on a single post-synaptic Renshaw cell.

2 e close contacts or puncta were observed per Renshaw cell.

3 with the soma and/or dendrites of individual Renshaw cells.

4 synaptic connection between motoneurones and Renshaw cells.

5 motoneurons, Ia inhibitory interneurons, and Renshaw cells.

6 y and organization of motor inputs on mature Renshaw cells.

7 is no reduction in the number of V1-derived Renshaw cells.

8 inhibitory amino acid transporter (VIAAT) in Renshaw cells.

9 nnectivity emerges during the development of Renshaw cells.

10 te the development of inhibitory synapses on Renshaw cells.

11 inhibitory circuit between motor neurons and Renshaw cells.

12 contribute to strengthen inhibitory input on Renshaw cells.

13 al support for the peptidergic modulation of Renshaw cells.

14 tes at both early and late postnatal ages on Renshaw cells.

15 he gephyrin/glycine receptor cluster size on Renshaw cells.

16 owth reached a plateau in 25- and 60-day-old Renshaw cells (0.45 +/- 0.43 microm(2); 0.56 +/- 0.55 mi

17 or expression in gephyrin patches located on Renshaw cells, a type of spinal interneuron that receive

18 Whole-cell recordings in P9-P15 Renshaw cells after P5 TeNT injections showed increases

19 ibitory glycinergic synapses may explain why Renshaw cells, although capable of firing at very high f

20 Group 1 are Renshaw cells and intensely express calbindin and coexpr

21 Early born Renshaw cells and late born Foxp2-V1 interneurons are ti

22 adapted to increase inhibitory efficacy over Renshaw cells and mature postnatally by mechanisms that

23 e cholinergic motoneuronal terminals on both Renshaw cells and motoneurons were enriched in glutamate

24 the formation of inhibitory synapses between Renshaw cells and motor neurons.

25 ter-IR motor axon synapses contact embryonic Renshaw cells and proliferate postnatally matching Rensh

26 oreactivity was used to identify 129 and 171 Renshaw cells and their dendrites in cat and rat lumbar

27 m from the soma in calbindin D28k-identified Renshaw cells and up to 184 microm in gephyrin-identifie

28 e receptor cluster size maturation that sets Renshaw cells apart from other interneurons is discussed

29 Our results suggest that while Renshaw cells are not directly required as an integral p

30 Like other V1 neurons, Renshaw cells are thus competent to receive sensory syna

31 hrna2 was correlated with disconnection from Renshaw cells as well as major structural abnormalities

32 ron inputs were sufficient to depolarize the Renshaw cell beyond threshold for firing.

33 atal day 0 (P0) and this input spread to all Renshaw cells by P10-P15.

34 In neonatal mice motoneurons excite Renshaw cells by releasing both acetylcholine (ACh) and

35 Using two markers for Renshaw cells (calbindin and cholinergic nicotinic recep

36 The responses from single Renshaw cells demonstrate that motoneuron synapses elici

37 roliferation coupled with the enlargement of Renshaw cell dendrites.

38 Concomitantly, Renshaw cells developed with increased excitability and

39 ox gene 6) is necessary for an early step in Renshaw cell development, whereas Engrailed 1 (En1), whi

40 the question of whether they interact during Renshaw cell development.

41 N-related transcription factor genes play in Renshaw cell development.

42 Loss of VIAAT from Chrna2(Cre) -expressing Renshaw cells did not impact any aspect of drug-induced

43 By 10 and 15 days of age, Renshaw cells exhibited gephyrin-immunoreactive clusters

44 ack-coupling loops similar to the well-known Renshaw cells explain the deterioration of synergy due t

45 Adult mammalian Renshaw cells express large and complex postsynaptic gep

46 In neonatal animals, Renshaw cells expressed small punctate gephyrin-immunore

47 ted that this input is functional and evokes Renshaw cell firing.

48 eptors were almost always colocalized inside Renshaw cell gephyrin clusters.

49 ajority (60-75%) of terminals presynaptic to Renshaw cell gephyrin patches contained immunocytochemic

50 ters contained inside boutons presynaptic to Renshaw cell gephyrin patches were also investigated.

51 w cells and proliferate postnatally matching Renshaw cell growth.

52 ht coupling with motor neurons suggests that Renshaw cells have an integral role in movement, a role

53 Renshaw cells, Ia inhibitory interneurons (IaINs), and p

54 ecting, inhibitory interneurons that include Renshaw cells, Ia inhibitory interneurons, and other uni

55 Renshaw cells, identified in human postmortem cervical s

56 The populations of clusters over developing Renshaw cells immunoreactive to gephyrin or glycine rece

57 the plasticity to compensate for loss of the Renshaw cell in adult circuit function.

58 rovide immunohistochemical identification of Renshaw cells in lamina VII of the ventral horn.

59 the recurrent circuitry indicates a role of Renshaw cells in modulating motor outputs that may be co

60 ent work has revealed novel ways to identify Renshaw cells in situ and this in turn has promoted a ra

61 the repercussions for the possible role for Renshaw cells in speed and force control.

62 ent of experimental strategies to manipulate Renshaw cells in spinal circuits and clarify their role

63 tions, the average gephyrin cluster areas on Renshaw cells increased by 18.4% at P15 and 28.4% at P20

64 VGLUT1-IR bouton density on Renshaw cells increased until P15 but thereafter decreas

65 elopment of inhibitory synapse properties on Renshaw cells, influencing recruitment of postsynaptic g

66 n this group receive convergent calbindin-IR Renshaw cell inputs.

67 he number of functional contacts on a single Renshaw cell is more than halved when the nicotinic rece

68 howed that most embryonic (embryonic day 18) Renshaw cells lack dorsal root inputs, but more than hal

69 neurones, and some interneurones, including Renshaw cells, lacked demonstrable Kv2.1-IR.

70 We have recently shown that Renshaw cells mediate powerful shunt inhibition on moton

71 Renshaw cells mediate recurrent inhibition between moton

72 omeric nicotinic receptors at the motoneuron-Renshaw cell (MN-RC) synapse.

73 ings from identified, synaptically connected Renshaw cell-motoneuron pairs in the mouse lumbar spinal

74 Calbindin-positive Renshaw cell number was decreased significantly at 12 we

75 the loss of presynaptic motor axon input on Renshaw cells occurs at early stages of ALS and disconne

76 stimulation was used to evoke currents from Renshaw cells or motoneurons to characterize responses o

77 in close apposition to lateral motoneurons, Renshaw cells, other GFP(+) INs, and unidentified neuron

78 y synapses between identified motoneuron and Renshaw cell pairs.

79 rging inputs from presynaptic motoneuron and Renshaw cell populations.

80 In parallel, Renshaw cell postsynaptic densities apposed to VGLUT1-IR

81 large size of many cholinergic terminals on Renshaw cells presumably correlates with the strong syna

82 increasing the strength of sensory inputs on Renshaw cells prevents their deselection and reduces mot

83 In this review we illustrate how mature Renshaw cell properties and connectivity arise through a

84 Renshaw cell properties have been studied extensively fo

85 to be the avian equivalent of the mammalian Renshaw cell (R-interneurons).

86 circuit formation, and the mature mammalian Renshaw cell raises the possibility that R-interneuronal

87 tudy focuses on the differentiation of adult Renshaw cells (RCs) and Ia inhibitory interneurons (IaIN

88 n 100 mum of the ventral white matter, where Renshaw cells (RCs) are located, (2) interneurons inters

89 Renshaw cells (RCs) are one of the most studied spinal i

90 e Ia inhibitory interneurons (IaINs) and all Renshaw cells (RCs) derive from embryonic V1 interneuron

91 tive afferent input to motoneurons (MNs) and Renshaw cells (RCs) is disrupted by thoracic spinal cord

92 Renshaw cells (RCs) receive excitatory inputs from moton

93 Although Renshaw cells (RCs) were discovered over half a century

94 program that controls the differentiation of Renshaw cells (RCs), an anatomically and functionally di

95 Renshaw cells receive a high density of inhibitory synap

96 INs and other V1-derived interneurons, adult Renshaw cells receive motor axon synapses and lack propr

97 For example, Renshaw cells receive, at least in the neonate, converge

98 neurons from neonatal mice lacking VIAAT in Renshaw cells received spontaneous inhibitory synaptic i

99 Here we examined the Renshaw cell recurrent circuit that exerts inhibitory fe

100 Renshaw cells represent a fundamental component of one o

101 of 4.4 and 2.8 close contacts on cat and rat Renshaw cells, respectively.

102 Thus, Renshaw cells shift from integrating sensory and motor i

103 Our data suggest an integral role for Renshaw cell signaling in shaping the excitability and s

104 Further, Renshaw cell signaling is closely associated with the mo

105 in rat using gephyrin-immunoreactivity, as a Renshaw cell specific marker, in combination with substa

106 Most calbindin-immunoreactive (IR) Renshaw cells survive to end stage but downregulate post

107 Renshaw cell synapses on motor neurons underwent more co

108 glutamatergic and calbindin-labeled putative Renshaw cell synapses on their soma and proximal dendrit

109 okes depolarizing monosynaptic potentials in Renshaw cells that are depressed, but not abolished, by

110 ow that a subset of V1 INs differentiates as Renshaw cells, the interneuronal cell type that mediates

111 generate exclusively cholinergic actions on Renshaw cells, their intraspinal synaptic targets.

112 Renshaw cells (V1(R)) are excitable as soon as they reac

113 VAChT-immunoreactive terminals apposed to Renshaw cells varied in size from 0.6 to 6.9 microm in d

114 s in regard to GABA release sites onto adult Renshaw cells was also found.

115 mine the relationships of these terminals to Renshaw cells, we used dual immunolabelling with antibod

116 s modulate synaptic maturation on developing Renshaw cells, we used three animal models in which affe

117 A total of 50 Renshaw cells were analysed quantitatively using a compu

118 Peptidergic influences on Renshaw cells were assessed in rat using gephyrin-immuno

119 Renshaw cells were identified by their calbindin immunor

120 Renshaw cells were special in that they displayed an abu

121 tion of quadriceps motor neurons mediated by Renshaw cells which had been activated by soleus motor n

122 tor neurons in the spinal cord also activate Renshaw cells, which provide recurrent inhibitory feedba

123 30 cholinergic terminals were observed on 50 Renshaw cells, with a range of 21-138 terminal appositio

124 rved in close contact with the immunolabeled Renshaw cells, with an average of 4.4 and 2.8 close cont