Comparison of adult, embryonic, and dystrophic myosin heavy chains from chicken muscle by sodium dodecyl sulfate/polyacrylamide gel electrophoresis and peptide mapping.

Rushbrook, Julie Ivory; Stracher, Alfred

doi:10.1073/pnas.76.9.4331

Cited by 104 publications

(51 citation statements)

References 26 publications

(22 reference statements)

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“…These results could also be consistent with the expression of a distinct embryonic isomyosin (1)(2)(3)(4)(5)(6)(7)(8), because our anti-skeletal antibodies cross-react with embryonic as well as adult skeletal myosins. However, our results indicate that these patterns of myosin expression do not apply to the initial developmental program for the myotome.…”

Section: Discussionsupporting

confidence: 77%

“…However, there has been considerable controversy as to the nature of both the heavy-chain and light-chain subunit composition of the myosin isozymes expressed in embryonic muscle. With respect to heavy-chain composition, there are several lines of evidence to suggest that skeletal muscle development is characterized by the expression of a distinct embryonic isomyosin (1)(2)(3)(4)(5)(6)(7)(8). Other evidence has suggested that the developmental program for embryonic skeletal muscle involves either the expression of fast skeletal myosin initially (10), the coexpression offast and slow skeletal isomyosins (7,9), or the expression of cardiac as well as skeletal isomyosins (11,17,18).…”

mentioning

confidence: 99%

“…There is abundant evidence that myosin expression undergoes transitions during the development of both skeletal (1)(2)(3)(4)(5)(6)(7)(8)(9)(10)(11) and cardiac muscle (1,(12)(13)(14)(15)(16) in a number of species. However, there has been considerable controversy as to the nature of both the heavy-chain and light-chain subunit composition of the myosin isozymes expressed in embryonic muscle.…”

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confidence: 99%

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Immunofluorescence analysis of the primordial myosin detectable in embryonic striated muscle.

Sweeney¹,

Clark²,

Umeda³

et al. 1984

Proc. Natl. Acad. Sci. U.S.A.

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Immunofluorescence analysis showed that the earliest myosin detectable in both the embryonic chicken heart and somitic myotome, the precursor to skeletal muscle, was strongly reactive with two different monoclonal antibodies specific for the heavy chain of cardiac ventricular myosin, but it showed no reactivity with affinity-purified polyclonal antibodies specific for the heavy chains of either fast-twitch or slow-tonic skeletal myosins. The heart remained reactive exclusively with the antibodies to cardiac myosin throughout development, while late embryonic (day 20) skeletal muscles were strongly reactive only with their homologous skeletal myosin antibodies. Our findings suggest that the primordial myosin heavy chain detectable in both forms of embryonic chicken striated muscle, the myotome and the heart, is immunologically distinct from myosins expressed in later embryonic as well as adult skeletal muscles, but it contains antigenic determinants similar to those present in cardiac ventricular myosin.There is abundant evidence that myosin expression undergoes transitions during the development of both skeletal (1-11) and cardiac muscle (1,(12)(13)(14)(15)(16)) in a number of species. However, there has been considerable controversy as to the nature of both the heavy-chain and light-chain subunit composition of the myosin isozymes expressed in embryonic muscle. With respect to heavy-chain composition, there are several lines of evidence to suggest that skeletal muscle development is characterized by the expression of a distinct embryonic isomyosin (1-8). Other evidence has suggested that the developmental program for embryonic skeletal muscle involves either the expression of fast skeletal myosin initially (10), the coexpression offast and slow skeletal isomyosins (7, 9), or the expression of cardiac as well as skeletal isomyosins (11,17,18). In the case of cardiac muscle, it is unclear whether the developmental program involves the coexpression of skeletal as well as cardiac isomyosins (17, 18).We examined myosin isozyme expression in the chicken embryo from the earliest demonstrated stages of myogenic differentiation and contractile protein expression in both the developing heart (19, 20) and somitic myotome (21-23), the precursor to skeletal muscle. The antigenic properties of the primordial striated-muscle myosins were analyzed by indirect immunofluorescence with specific monoclonal antibodies produced against the heavy chains of chicken cardiac ventricular (V3) myosin, and with affinity-purified polyclonal antibodies produced against the heavy chains of adult fast and slow skeletal myosins. We found that the earliest myosin heavy chain detectable in both forms of striated muscle was indistinguishable with these antibodies from cardiac ventricular myosin expressed in the adult heart but immunologically distinct from myosins expressed in later embryonic as well as adult skeletal muscles. Myotomal cross-reactivity with the cardiac antibodies was in striking contrast to the absence of reactivity of adu...

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Section: Discussionsupporting

confidence: 77%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Immunofluorescence analysis of the primordial myosin detectable in embryonic striated muscle.

Sweeney¹,

Clark²,

Umeda³

et al. 1984

Proc. Natl. Acad. Sci. U.S.A.

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“…This enzymatic activity is correlated with contractile velocity in skeletal muscle (1) and thus appears to be an important determinant of contractile function. Numerous polymorphic forms of myosin HC exist, not only in different types of muscle-e.g., fast and slow skeletal and cardiac-but also within each muscle type (2)(3)(4)(5)(6)(7)(8)(9)(10)(11)(12). Expression of these forms follows a developmental pattern (12)(13)(14)(15)(16)(17)(18) that may be altered by changes in the physiological (19)(20)(21) and hormonal (10)(11)(12)(13) milieu ofthe cell.…”

mentioning

confidence: 99%

“…The specific activity ofthe probe was 1-5 X 10r' cpm/yg. Hybridization and nuclease S1 digestion were carried.out by the method of Orkin and Goff (38), except that the probe (0.5-1 X 105 cpm, 10-50 ng) was hybridized in a sealed capillary tube with either 5 ,ug of cardiac poly(A)+RNA or 30-50 pg of cardiac total RNA. The digested products were analyzed on 5% sequencing gels (33,38).…”

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confidence: 99%

Molecular cloning of mRNA sequences for cardiac alpha- and beta-form myosin heavy chains: expression in ventricles of normal, hypothyroid, and thyrotoxic rabbits.

Sinha¹,

Umeda²,

Kavinsky³

et al. 1982

Proc. Natl. Acad. Sci. U.S.A.

127

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We have isolated cDNA clones from thyrotoxic (pMHCa) and normal (pMHC(8) adult rabbit hearts. Restriction map analysis and DNA sequence analyses show that, although there is strong homology between overlapping regions of the two clones, they are distinctly different. The two clones exhibited 78483% homology between the derived amino acid sequences and those determined by direct amino acid sequence analysis of rabbit fast skeletal muscle myosin heavy chains. The clones specify a segment of the myosin heavy chain corresponding to subfragment 2 and the COOH-terminal portions of subfragment 1. Nuclease S1 mapping was used to compare transcription of the two clones with expression of the a and (3 forms of myosin heavy chains in the ventricles of thyrotoxic, hypothyroid (propylthiouracil-treated), and normal rabbits. Thyrotoxic ventricles contained only pMHCa transcripts whereas hypothyroid ventricles contained exclusively pMHC(3 transcripts. These data correlate well with the presence of a-and (3-form myosin heavy chains. In the normal young adult rabbit, pMHC(3 transcripts predominate, agreeing with the known (3 form/a form ratio of 4: 1. We therefore conclude that pMHCa and pMHCP contain sequences of the a-and (-form myosin heavy chain genes, respectively.Myosin, a major contractile protein of skeletal and cardiac muscle, is composed of two 200,000-dalton heavy chains (HCs) and two sets oflow molecular weight light chains. The active center of myosin ATPase resides in the globular head of the heavy chain. This enzymatic activity is correlated with contractile velocity in skeletal muscle (1) and thus appears to be an important determinant of contractile function. Numerous polymorphic forms of myosin HC exist, not only in different types of muscle-e.g., fast and slow skeletal and cardiac-but also within each muscle type (2-12). Expression of these forms follows a developmental pattern (12-18) that may be altered by changes in the physiological (19-21) and hormonal (10-13) milieu ofthe cell.Cardiac ventricular muscle contains at least two formsreferred to as a and (3 (9)-of myosin HC. Electrophoresis of myosin under nondenaturing conditions reveals three bands; V1 and V3 are homodimers containing the a and 3 forms, respectively, whereas V2 is a heterodimer (9, 13). The ATPase activity of myosin with a-form HCs has been shown to be considerably higher than that of myosin with (-form .The expression of a-and (3form myosin HCs follows a defined developmental pattern that varies in different animal species. It has been shown that in rabbit the ( form/a form ratio is =3: 1 during the last halfofthe gestational period. After birth, the relative amount of the a form increases so that, during the first 2 wk postnatally, this ratio is 1: 1 (12, 14). Thereafter, the a form decreases and, in the old adult, the 3 form is present almost exclusively (12,14). In the young adult animals used in this study, the ( form/a form ratio was =4:1 (12 (27).Construction and Screening of cDNA Clones. Single-and double-stranded cDNA wa...

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Evolutionary significance of myosin heavy chain heterogeneity in birds

Bandman

Rosser

2000

Microsc. Res. Tech.

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Comparison of adult, embryonic, and dystrophic myosin heavy chains from chicken muscle by sodium dodecyl sulfate/polyacrylamide gel electrophoresis and peptide mapping.

Cited by 104 publications

References 26 publications

Immunofluorescence analysis of the primordial myosin detectable in embryonic striated muscle.

Immunofluorescence analysis of the primordial myosin detectable in embryonic striated muscle.

Molecular cloning of mRNA sequences for cardiac alpha- and beta-form myosin heavy chains: expression in ventricles of normal, hypothyroid, and thyrotoxic rabbits.

Evolutionary significance of myosin heavy chain heterogeneity in birds

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