ライフサイエンスコーパス: antagonist muscle

1 nd repetitive co-contractions of agonist and antagonist muscles.

2 n insect legs with different arrangements of antagonist muscles.

3 stronger where they assist the weaker of two antagonist muscles.

4 ibraries from sensory neurons that innervate antagonist muscles.

5 p Ia excitatory reflexes between agonist and antagonist muscles.

6 ons to occur without increased resistance to antagonist muscles.

7 nchronous or asynchronous neuronal firing in antagonist muscles.

8 with feedback delay and tonically controlled antagonist muscles.

9 e spinal neurons mediating co-contraction of antagonist muscles.

10 nus and striking coactivation of agonist and antagonist muscles.

11 red activation of the agonist, synergist and antagonist muscles.

12 he phase difference between neural drives to antagonist muscles, a long-standing observation yet unex

13 es complement the balance of strength of the antagonist muscles acting on the joint.

14 ociated with large 5-15 Hz coherence between antagonist muscle activities.

15 ctromyography from task-relevant agonist and antagonist muscles, alongside transcranial magnetic stim

16 imb swing velocity.(6) In stance, minimizing antagonist muscle and joint passive forces could save en

17 ved botulinum type A toxin injections in the antagonist muscle at the same treatment session.

18 Continuous contraction of agonist and antagonist muscles caused by involuntary motor-unit firi

19 t at age 10-12 years there is little agonist-antagonist muscle co-contraction around the time of foot

20 s resulting from coactivation of agonist and antagonist muscles driving the joints toward equilibrium

21 y there was less coactivation of agonist and antagonist muscles during the AAN paradigm.

22 in the predominant co-contraction of agonist/antagonist muscles during voluntary movement observed in

23 By preserving agonist-antagonist muscle dynamics, the AMI allows proprioceptiv

24 EMG with no significant coupling between the antagonist muscle EMGs.

25 is stimulated by an agonist neuron, while an antagonist muscle fiber is unstimulated by a pause and s

26 ts of applying vibration to the tendon of an antagonist muscle (flexor carpi radialis) during the cou

27 les until an equilibrium between agonist and antagonist muscle force is achieved.

28 wing that, at the rest postures, agonist and antagonist muscles generated equal forces indicated that

29 Coactivation of agonist-antagonist muscle groups was observed both at rest and d

30 ed contractions, including cocontractions of antagonist muscle groups, during voluntary movements.

31 ity so that reciprocally acting, agonist and antagonist muscles have a stable platform from which to

32 tive finger movements, stretch of the loaded antagonist muscle (i.e., extensor) was accompanied by in

33 gether with botulinum toxin injection in the antagonist muscle improves eye alignment in comitant hor

34 consisting of surgically connected, agonist-antagonist muscles including muscle-sensing electrodes.

35 Co-contraction of antagonist muscles is characteristic of spasticity arisi

36 he phase difference between neural drives to antagonist muscles is determined by the relative strengt

37 o, CA) suggested that changes in agonist and antagonist muscle lengths were responsible for the endur

38 burst was not preceded by an increase in the antagonist muscle MEP:IEMG ratio.

39 o-contraction, the inhibitory input from the antagonist muscle overcomes the additional excitatory an

40 ndex related to the co-activation of agonist-antagonist muscle pairs (C-index) was modulated with tou

41 inhibitory Group Ia reflexes linking agonist/antagonist muscle pairs acting at the shoulder and elbow

42 mplified hexapedal leg geometry with agonist-antagonist muscle pairs actuating each leg joint.

43 which surgically preserve and couple agonist-antagonist muscle pairs for the subtalar and ankle joint

44 cy inhibition and excitation between agonist/antagonist muscle pairs; inhibition was significantly mo

45 Antagonist muscle passive torques alone can thus control

46 ase in corticospinal excitability related to antagonist muscle recruitment could compensate for a pot

47 The timing of such antagonist muscle recruitment relative to the stop signa

48 During locomotion, functional antagonist muscles, TA and Sol, were coactivated both in

49 sected muscle and in the passively stretched antagonist muscle, there was a dramatic increase in the

50 Subjects (n = 20) predictively co-activated antagonist muscles to adjust one component of the impeda

51 on alters the control signals to agonist and antagonist muscles to change movement speed.

52 t may occur due to the co-contraction of the antagonist muscle, which constrains PIC behaviour.