Momb Brent A, Kent Jane A, Chipkin Stuart R, Miller Mark S
bioRxiv. 2025 Sep 3:2025.08.28.672942. doi: 10.1101/2025.08.28.672942.
Intracellular accumulation of hydrogen ions (H ) and inorganic phosphate (P ) have temperature-dependent effects on single fiber contractile function between 10-30°C. , human skeletal muscle temperatures range between 35-38°C, and although contractile function is highly dependent on temperature, the effects of fatigue-inducing [H ] and [P ] on contractile mechanics at 37°C is unknown. Using sinusoidal analysis, the independent and combined effects of these metabolites on cellular and molecular contractile function were determined at 37°C in slow-contracting myosin heavy chain (MHC) I and fast-contracting MHC IIA fibers from vastus lateralis muscle of 13 older adults (8 females), under four conditions: maximal calcium activation ("control"; 5 mM P , pH 7.0), high P (30 mM), low pH (6.2), and fatigue (30 mM P and pH 6.2). Specific tension (force/cross-sectional area, mN/mm ) in both fiber types was reduced only under fatigue conditions (20-26%). MHC I fibers had slower cross-bridge kinetics with fewer or less stiff strongly-bound myosin-actin cross-bridges in high P , low pH, and fatigue. In contrast, fatigued MHC IIA fibers had faster cross-bridge kinetics with increased myofilament and/or cross-bridge viscosity. Single fiber oscillatory work was reduced in both fiber types when P or pH alone was altered. However, fatigue conditions returned oscillatory work values toward control through alterations to cross-bridge kinetics in MHC I fibers and changes to work absorption and production processes in MHC IIA fibers. These findings quantify fiber-type specific mechanical and kinetic mechanisms of fatigue in human skeletal muscle at 37°C, thus advancing our understanding of metabolite-based muscle fatigue .
Working skeletal muscle increases intracellular concentrations of hydrogen ion and inorganic phosphate, leading to fatigue, or loss of force-generating capacityTemperature plays a well-established role in the muscle response to hydrogen ion and/or inorganic phosphate accumulation, but has not previously been studied at human body temperature (37°C)At 37°C, reduced force generation only occurs when high phosphate and hydrogen ions are combined, not when changed individuallyIn slow-contracting fibers, fatigue slowed myosin-actin cross-bridge kinetics and reduced the number or stiffness of strongly-bound cross-bridges. In fast-contracting fibers, fatigue increased myosin-actin cross-bridge kinetics and increased myofilament viscosity.The distinct responses by fiber type to fatigue provides new insight into its mechanisms and advances our understanding of the whole muscle and body responses to fatigue.
氢离子(H⁺)和无机磷酸盐(Pi)在细胞内的积累对10 - 30°C之间的单纤维收缩功能具有温度依赖性影响。然而,人体骨骼肌温度在35 - 38°C之间,尽管收缩功能高度依赖于温度,但疲劳诱导的[H⁺]和[Pi]对37°C时收缩力学的影响尚不清楚。使用正弦分析,在四种条件下,测定了这些代谢物对13名老年人(8名女性)股外侧肌慢收缩肌球蛋白重链(MHC)I型和快收缩MHC IIA型纤维在37°C时细胞和分子收缩功能的独立及联合影响:最大钙激活(“对照”;5 mM Pi,pH 7.0)、高Pi(30 mM)、低pH(6.2)和疲劳(30 mM Pi和pH 6.2)。两种纤维类型的比张力(力/横截面积,mN/mm²)仅在疲劳条件下降低(20 - 26%)。在高Pi、低pH和疲劳状态下,MHC I型纤维的横桥动力学较慢,强结合的肌球蛋白 - 肌动蛋白横桥数量减少或刚性降低。相比之下,疲劳的MHC IIA型纤维具有较快的横桥动力学,肌丝和/或横桥粘度增加。当单独改变Pi或pH时,两种纤维类型的单纤维振荡功均降低。然而,疲劳条件通过改变MHC I型纤维的横桥动力学以及MHC IIA型纤维的功吸收和产生过程,使振荡功值恢复到对照水平。这些发现量化了37°C时人体骨骼肌疲劳的纤维类型特异性机械和动力学机制,从而增进了我们对基于代谢物的肌肉疲劳的理解。
工作中的骨骼肌会增加细胞内氢离子和无机磷酸盐的浓度,导致疲劳,即产生力的能力丧失。温度在肌肉对氢离子和/或无机磷酸盐积累的反应中起着既定作用,但此前尚未在人体温度(37°C)下进行研究。在37°C时,只有当高磷酸盐和氢离子同时存在时才会出现力产生减少,单独改变时则不会。在慢收缩纤维中,疲劳会减慢肌球蛋白 - 肌动蛋白横桥动力学,并减少强结合横桥的数量或刚性。在快收缩纤维中,疲劳会增加肌球蛋白 - 肌动蛋白横桥动力学并增加肌丝粘度。纤维类型对疲劳的不同反应为其机制提供了新的见解,并增进了我们对整个肌肉和身体对疲劳反应的理解。
