Review of RyR1 pathway and associated pathomechanisms

Ryanodine receptor 1-related myopathies (RyR1-RM) comprise the most common non-dystrophic congenital myopathy, with a prevalence of approximately 1/90,000 in the United States [2, 83]. Causative mutations in the gene (RYR1), which encode the major sarcoplasmic reticulum calcium release channel of skeletal muscle (RyR1), have been found in several myopathy subtypes. Although dominantly inherited central core disease (CCD, MIM# 11700) and recessively inherited multi-minicore disease (MmD) are the most commonly associated myopathies caused by mutations in RYR1, mutations have also been identified in cases of centronuclear myopathy (CNM), congenital fiber-type disproportion (CFTD), and King Denborough syndrome [41, 47, 85] These mutations result in constant calcium leak at rest, defective excitation-contraction coupling, and increased mitochondrial oxidative stress [48, 83]. Malignant hyperthermia susceptibility (MHS) trait, a dominantly inherited, severe pharmacogenetic reaction to volatile anesthetics and muscle relaxants, is an allelic condition (MIM# 145600) [85].

The clinical spectrum of RYR1-RM is quite broad. Even within CCD, symptoms may range from very mild to severe. Individuals with CCD typically present with proximal muscle weakness of the hip girdle, hypotonia, mild facial weakness, joint laxity and/or mild contractures, and/or orthopedic complications such as scoliosis [22, 83, 85]. Both hip girdle weakness due to fetal hypotonia and acetabular dysplasia contribute to congenital hip dislocation, which is also observed in CCD [22, 40, 45]. A more severe form of CCD is CCD-associated fetal akinesia. Related symptoms include severe hypotonia, arthrogryposis, skeletal deformities, kyphoscoliosis, and failure to thrive. In some cases, individuals survive birth, and present with strabismus and bilateral ptosis [118]. Individuals with MmD present with moderate to severe symptoms, such as proximal and distal weakness, hypotonia, a combination of contractures and/or laxity, progressive scoliosis, and, in some cases, bulbar weakness and/or external ophthalmoplegia [158]. Individuals with CNM are similar to MmD, but have more severe symptoms initially with improvement overtime. They often present with proximal muscle weakness, ophthalmoplegia, facial weakness, and respiratory impairment [82]. Symptoms associated with CFTD may include skeletal muscle wasting and weakness, hypotonia, ophthalmoplegia, ptosis, respiratory impairment, congenital hip dislocations, joint contractures, foot deformities, and kyphoscoliosis [29, 37]. In rare recessive cases, congenital onset is very severe with respiratory failure requiring ventilation [21, 22, 83, 85, 158]. The phenotype is complicated by several symptoms and may include myalgia, axial weakness, and fatigability [46, 80, 83]. Severity may vary within the family [83] with some individuals presenting with myopathy and MHS and others presenting with only MHS [85].

The defining histopathological feature on muscle biopsy is the presence of a single, central amorphous core extending longitudinally along the muscle fiber in the case of CCD or multiple smaller cores in one fiber (MmD), which in both cases are likely due to reduced mitochondrial oxidative enzyme activity as a result of mitochondrial deficiency or depletion [83, 85]. Fiber type predominance is another histological finding in RYR-RM [81, 158]. Fiber type transformation has been shown to result from mitochondrial activity relative to nitric oxide. As mentioned below in the nitrosylation section of group 5, nitric oxide binds to cytochrome C oxidase of the electron transport chain and inhibits mitochondrial respiration. This phenomenon has been shown in adipose tissue and skeletal muscle and is dependent on peroxisome proliferator-activated receptor gamma coactivator 1-alpha (PGC-1α). PGC-1α regulates muscle fiber type generation, favoring type I fibers. Additionally, PGC-1α overexpression in mouse skeletal muscle results in increased β-oxidation of fatty acids, increased muscle glucose uptake, and overexpression of proteins involved in fat oxidation and glucose transport [134]. We may better understand type I fiber predominance, and possibly uniformity, by studying PGC-1α in RYR1-RM skeletal muscle. PGC-1α levels may be affected greatly due to skeletal muscle fatty infiltration and mitochondrial dysfunction in RYR1-RM.

Type I fiber predominance and hypotrophy are identified in most cases [81, 85, 154, 158] In some cases (namely C-terminal RYR1 mutations), there is also type 1 fiber uniformity without structural changes in over 99 % of the type 1 muscle fibers. This is very similar to congenital neuromuscular disease with uniform type 1 fiber (CNMU1), and, in this disease, ophthalmoplegia is considered to be an important clinical manifestation [125, 126]. This may also be true in RYR1-RM where type 1 fibers are uniform in cases with ophthalmoplegia. On the other hand, cores may be absent in CNM and CFTD, where the predominant features are central nucleation and fiber-type disproportion where type 2 fibers are at least 25 % larger than type 1 fibers [154], as their names suggest. Fatty replacement, fibrosis, and/or nuclear internalization may also be present [22, 83].

In some cases, nemaline rods and cores coexist with myofibrillar disorganization. Patients with rods and cores are considered to have central core/rod disease (CCRD). Interestingly, instead of leaky RyR1 channels as noted in CCD, individuals with CCRD present with excess ryanodine receptors in the central cores [127]. In the recessive form of CCD, MmD, there is a depletion of the RyR1 protein [158].

Although RyR1 is a simple transmembrane protein (homotetrameric), the variation in symptomology in RYR1-RM suggests there is more to this protein and its function, including modifying factors [83, 158]. When scanning the literature, each article unveils small pieces to a bigger puzzle. This review combines several pieces to gain a more complete understanding of RyR1. Understanding RyR1 is critical for treatment development in RYR1-RM, especially given the lack of FDA approved treatment to date. Combined, the literature elucidates RyR1 as a simple protein with a complex pathway due to its tight regulation of ortho- and retrograde calcium flux by several factors including proteins, post-translational modifications, and ligands. Additionally, this paper highlights what is known about RyR1 mutations, the affected interaction sites, possible regulatory functions disrupted, and translation into the diseased state. These compiled results suggest target sites and regulatory complexes for potential therapies.