Abstract
Anterior cruciate ligament injury occurs when the ligament fibers are stretched, partially torn, or completely torn. The authors propose a new injury mechanism for non-contact anterior cruciate ligament injury of the knee. Accordingly, non-contact anterior cruciate ligament injury could not happen without the acute compression microinjury of the entrapped peripheral proprioceptive sensory axons of the proximal tibia. This would occur under an acute stress response when concomitant microcracks-fractures in the proximal tibia evolve due to the same excessive and repetitive compression forces. The primary damage may occur during eccentric contractions of the acceleration and deceleration moments of strenuous or unaccustomed fatiguing exercise bouts. This primary damage is suggested to be an acute compression/crush axonopathy of the proprioceptive sensory neurons in the proximal tibia. As a result, impaired proprioception could lead to injury of the anterior cruciate ligament as a secondary damage, which is suggested to occur during the deceleration phase. Elevated prostaglandin E2, nitric oxide and glutamate may have a critical neuro-modulatory role in the damage signaling in this dichotomous neuronal injury hypothesis that could lead to mechano-energetic failure, lesion and a cascade of inflammatory events. The presynaptic modulation of the primary sensory axons by the fatigued and microdamaged proprioceptive sensory fibers in the proximal tibia induces the activation of N-methyl-D-aspartate receptors in the dorsal horn of the spinal cord, through a process that could have long term relevance due to its contribution to synaptic plasticity. Luteinizing hormone, through interleukin-1β, stimulates the nerve growth factor-tropomyosin receptor kinase A axis in the ovarian cells and promotes tropomyosin receptor kinase A and nerve growth factor gene expression and prostaglandin E2 release. This luteinizing hormone induced mechanism could further elevate prostaglandin E2 in excess of the levels generated by osteocytes, due to mechanical stress during strenuous athletic moments in the pre-ovulatory phase. This may explain why non-contact anterior cruciate ligament injury is at least three-times more prevalent among female athletes.
Highlights
Anterior cruciate ligament (ACL) injury occurs when the ligament fibers are stretched, partially torn, or completely torn [1]
Life 2021, 11, 443 damage, like in Delayed onset muscle soreness (DOMS) [25,26,27]. They are proposing that the critical damage of the first phase in noncontact ACL (NC-ACL) injury is due to large fiber sensory axonopathy caused by superposition of compression forces
We propose the analog involvement of the mitochondrial electron transport chain-generated free radicals in the acute compression sensory axonopathy of large sensory fibers in the periosteum, like in DOMS
Summary
Anterior cruciate ligament (ACL) injury occurs when the ligament fibers are stretched, partially torn, or completely torn [1]. The authors propose that the initial cause of NC-ACL injury is an acute damaging compression injury of the proprioceptive sensory axons in the proximal tibia. Most NC-ACL injuries happen when “foot strike with the knee close to full extension” [24] This is the provocative position when superposition of damaging compression forces is maximized. The authors of this paper emphasize the importance of the large fiber proprioceptive sensory neurons in the periosteum and in the proximal tibia They believe that the compressive mechano-energetic lesion of these proprioceptive axons could precede the NC-ACL injury. The current authors are proposing that NC-ACL injuries happen under a cognitive demand derived acute stress reaction (ASR) when insufficient force production is unacceptable in unaccustomed and strenuous fatiguing eccentric exercise moments [27,30]
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