ライフサイエンスコーパス: A-fibre

1 A fibre neurones exhibiting SP-LI included seven of eigh

2 A fibre was accepted for study if it gave a stable, all-

3 A fibre was maximally Ca2+-activated in the isometric st

4 A fibre with dual cores, p-type and n-type silicon, is d

5 A fibre with high water holding capacity, extracted from

6 A fibre-based mapping approach, implementing the calcula

7 A fibre-optic hydrophone was integrated into a needle to

8 A fibre-optic probe that integrates a nitrogen-vacancy (

9 A-fibre LTM neurones were divided into Adelta- (D hair u

10 Six of 23 A-fibre nociceptive cells were positive including one Aa

11 Three of 36 A-fibre LTM units exhibited CGRP-LI; all were Aalpha/bet

12 r GABA transporter VGAT and primary afferent A-fibre terminals in neonates.

13 ty occurred in both A and C fibres, although A fibres showed a greater increase in mechano-sensitivit

14 ly categorized as C fibres (nociceptors) and A fibres (non-nociceptive; rapidly and slowly adapting l

15 Na(v)1.9 is expressed selectively in C- and A-fibre nociceptive-type units and is upregulated by G-p

16 btypes of functionally distinct C-fibres and A-fibres.

17 hat both Krause corpuscle afferent types are A-fibre rapid-adapting low-threshold mechanoreceptors, o

18 erived) nociceptive-like fibres include both A-fibres and C-fibres, are insensitive to P2X receptors

19 Repeated stimulation of cutaneous A fibres at 0.5 Hz at twice the threshold level did not

20 Repeated stimulation of cutaneous A fibres at 0.5 Hz at twice the threshold level produced

21 The direct A fibre-evoked activity did not increase, but the backgr

22 d the mean threshold intensity for eliciting A fibre-mediated EPSCs in lamina II neurones.

23 ese tension mechanoreceptors are exclusively A-fibres arising from the nodose ganglion.

24 old mechanoreceptor units or the thirty-five A fibre low threshold units (D-hair and other units) sho

25 imilarly distributed between nodose ganglion A-fibres and C-fibres innervating the lung.

26 ere neurofilament-rich, suggesting they have A-fibres; we therefore focussed on A-fibre neurons to de

27 first pain sensation is mediated by type-II A-fibre nociceptors (II-AMHs).

28 te to the longer AP durations (especially in A-fibre neurons) and larger AP overshoots that are typic

29 l (AP) duration (both rise and fall time) in A-fibre neurons and with AP rise time only in positive C

30 Like A fibre supernormality, these phenomena were explained b

31 Of 52 non-MSA A-fibre neurons including nociceptive and cutaneous low-

32 failed to activate stretch-sensitive nodose A-fibres in the lungs.

33 The data indicate that C-fibres, but not A-fibres, conveyed low-threshold mechanoreceptor inputs

34 after injury reinstated hyperexcitability of A-fibre axons and enhanced mechanosensitivity.

35 etween the mechanical encoding properties of A-fibre nociceptors, which provide the dominant inputs t

36 ed (significant), and was similar to that of A-fibre nociceptive neurones.

37 synapses but did not alter the engulfment of A-fibres.

38 they have A-fibres; we therefore focussed on A-fibre neurons to determine the sensory properties of a

39 possessed little or no immunoreactive orexin A fibres in its core, but had fibres at its periphery.

40 contained a plexus of immunoreactive orexin A fibres throughout its rostro-caudal extent.

41 were found to contain immunoreactive orexin A fibres.

42 Immunoreactive varicose orexin A fibres were found throughout the hypothalamus.

43 h IB4-positive (C-fibre) and NF200-positive (A-fibre) neurons in DRG of CHF rats whereas the immunost

44 to +500 mm Hg) to exposed dentine.Seventeen A-fibres (conduction velocity (CV), 10.6-55.1 m s(-1)) w

45 The mean number of spikes evoked by a single A fibre skin stimulus was remarkably consistent between

46 Ten of sixty-six A fibre neurones exhibited SP-LI, including eight of six

47 This result suggests that A-fibre sprouting arise after peripheral nerve injury, b

48 Latencies of response to A fibre skin stimulation were very long and varied widel

49 and a late subnormal phase (H1), similar to A fibres.

50 ns with respect to being either 'normal' via A-fibres or 'alarm' via TRPV1 expressing C-fibres and, a

51 ade from 25 regenerated nociceptors; 14 were A fibres and the remainder were C fibres.