Abstract
BackgroundImmunofluorescence analyses of anterior cruciate ligament (ACL) allografts following remnant-preserving ACL reconstruction using Achilles tendon allografts have provided evidence for the presence of neural elements. In this study, we aimed to examine the expression of neural elements and quantify the presence of neural cells in ACL remnants and Achilles allografts using nerve growth factor (NGF) therapy after remnant-preserving ACL reconstruction.MethodsExperiments were conducted on 5 pairs of rats (approximately 8 weeks old and weighing 320 g at the time of surgery). Longitudinally, split Achilles tendons from the paired rats were freshly frozen and later defrosted with warm saline and allografted onto the right ACL of the other rat that was partially detached at the femoral attachment site. A sham operation was conducted on the left knee to be used as a control. NGF was injected into both knee joints every week for 6 weeks after surgery. The presence of neural cells in the ACL of the sham-operated knee, allografted Achilles tendon, and ACL remnant was examined 6 weeks post-surgery using H and E and immunofluorescent staining.ResultsH and E staining did not reveal neural cells in any of the three groups. However, immunofluorescence analysis showed the presence of nestin-positive neural elements in the normal ACL tissues as well as ACL remnants. Additionally, neural elements were examined in 7 of the 8 (87.5%) allograft tissues. Quantitative analysis showed no difference in the number or area of nuclei among the three groups. However, the number and area of neural cells in the Achilles allografts were significantly lower than those in the other two groups (p = 0.000 and p = 0.001, respectively).ConclusionOur observations indicate that ACL remnants promote the new ingrowth and persistence of neural cells. We suggest that the ingrowth of neural elements can support the persistence and new ingrowth of mechanoreceptors, thereby enhancing the functional stability of knee joints. Moreover, the expression of neural cells in the Achilles allografts was lower than that in normal ACL tissues and ACL remnants in the quantitative evaluation, thereby confirming the essential role of ACL remnants in knee joint functionalization.
Highlights
Immunofluorescence analyses of anterior cruciate ligament (ACL) allografts following remnantpreserving ACL reconstruction using Achilles tendon allografts have provided evidence for the presence of neural elements
Neural cells or mechanoreceptors could not be detected in normal ACL tissues, ACL remnants, or Achilles allograft tissues through H and E staining (Fig. 3)
Nestin was expressed in all normal ACL tissues that were injected with nerve growth factor (NGF)
Summary
Immunofluorescence analyses of anterior cruciate ligament (ACL) allografts following remnantpreserving ACL reconstruction using Achilles tendon allografts have provided evidence for the presence of neural elements. We aimed to examine the expression of neural elements and quantify the presence of neural cells in ACL remnants and Achilles allografts using nerve growth factor (NGF) therapy after remnantpreserving ACL reconstruction. Denti et al reported that mechanoreceptors were present in the bone-patellar tendon autografts in the knees of sheep 3 months after surgery and in human knees with failed autografts at 9 and 10 years after surgery [9]. These findings suggest that ACL remnants are a possible source of re-innervation of the tendon graft. Few studies have quantitatively evaluated neural elements in ACL remnants and ACL allografts
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