Association of myostatin on early calf mortality, growth, and carcass composition traits in crossbred cattle

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ANIMAL GENETICS

Association of myostatin on early calf mortality, growth, and carcass composition traits in crossbred cattle¹^,2

E. Casas³, G. L. Bennett, T. P. L. Smith and L. V. Cundiff

U.S. Meat Animal Research Center, USDA, ARS, Clay Center, NE 68933-0166

³ Correspondence: P.O. Box 166 (phone: 402-762-4168; fax: 402-762-4173; e-mail: casas{at}email.marc.usda.gov).

The objective of this study was to investigate a potential associationof an inactive myostatin allele with early calf mortality, andevaluate its effect on growth and carcass traits in a crossbredpopulation. Animals were obtained by mating F₁ cows to F₁ (BelgianBlue x British Breed) or Charolais sires. Cows were obtainedfrom mating Hereford, Angus, and MARC III ( $1/4$ Hereford, $1/4$ Angus, $1/4$ Pinzgauer, and $1/4$ Red Poll) dams to Hereford, Angus, Tuli, Boran,Brahman, or Belgian Blue sires. Belgian Blue was the sourceof the inactive myostatin allele. Myostatin genotypes were determinedfor all animals including those that died before weaning. Earlycalf mortality was examined in the F₂ subpopulation (n = 154),derived from the F₁ sires mated to F₁ cows from Belgian Bluesires, to evaluate animals with zero, one, or two copies ofinactive myostatin allele. An overall 1:2:1 ratio (homozygousactive myostatin allele:heterozygous:homozygous inactive myostatinallele) was observed in the population; however, a comparisonbetween calves dying before weaning and those alive at slaughtershowed an unequal distribution across genotypes (P < 0.01).Calves with two copies of the inactive allele were more likely(P < 0.01) to die before weaning. Postweaning growth traitswere evaluated in the surviving animals (n = 1,370), includingbirth, weaning, and live weight at slaughter, and postweaningADG. Carcass composition traits analyzed were hot carcass weight,fat thickness, LM area, marbling score, USDA yield grade, estimatedkidney, pelvic, and heart fat, retail product yield and weight,fat yield and weight, bone yield and weight, and percentageof carcasses classified as Choice. Charolais lack the inactivemyostatin allele segregating in Belgian Blue; thus, in the populationsired by Charolais (n = 645), only animals with zero or onecopy of the inactive myostatin allele were evaluated. Animalscarrying one copy were heavier at birth and at weaning, andtheir carcasses were leaner and more muscled. In the populationsired by Belgian Blue x British Breed (n = 725), animals withtwo copies of inactive myostatin allele were heavier at birth,leaner, and had a higher proportion of muscle mass than animalswith zero or one copies. Heterozygous animals were heaviestat weaning and had the highest live weight, whereas animalswith zero copies had the highest fat content. The use of theinactive myostatin allele is an option to increase retail productyield, but considerations of conditions at calving are importantto prevent mortality.

Key Words: Carcasses • Crossbred Cattle • Growth • Mortality • Myostatin

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