Linkage between sperm abnormality level and major urinary protein phenotype in mice

Abstract

Segregation of sperm abnormality level and the pattern of major urinary proteins (MUPs) were investigated in F₂ and B₁ hybrid males obtained from crosses involving two contrasting inbred strains of mice: CBA/Kw (Mup-1^a1^a, 3·3% abnormal sperm) and C57BL/Kw (Mup-1^b1^b, 21·9% abnormal sperm). In the progeny of both crosses mean levels of abnormal spermatozoa were significantly higher for males typed as Mup-1^b1^b than for heterozygous Mup-1^a1^b males. Moreover, all F₂ hybrid males showing very high percentages of abnormal sperm were Mup-1^b1^bhomozygotes. Similarly, among B₁ males with a high level of deformed spermatozoa, a statistically significant majority were Mup-1^b1^b genotypes. Our results suggest that at least two genes which influence sperm abnormality level are segregating in these crosses. Both appear to be recessive for high sperm abnormality level, and one shows weak linkage to Mup-1 on chromosome 4.