Reciprocal Chromosome Translocation, rcp(7;17)(q26;q11), in a Boar Giving Reduced Litter Size and Increased Rate of Piglets Dying in the Early Life

A singular focus on maternal health at the time of a pregnancy leaves much about perinatal mortality unexplained, especially when there is growing evidence for maternal early life effects. Further, lumping stillbirth and early neonatal death into a single category of perinatal mortality may obscure different causes and thus different avenues of screening and prevention. The common marmoset monkey (Callithrix jacchus), a litter-bearing nonhuman primate, is an ideal species in which to study the independent effects of a mother’s early life and adult phenotypes on pregnancy outcomes. We tested two hypotheses in 59 marmoset pregnancies at the Southwest National Primate Research Center and the Barshop Institute for Longevity and Aging Studies. We explored 1) whether pregnancy outcomes were predicted independently by maternal adult weight versus maternal litter size and birth weight, and 2) whether stillbirth and early neonatal death were differentially predicted by maternal variables. No maternal characteristics predicted stillbirth and no maternal adult characteristics predicted early neonatal death. In univariate Poisson models, triplet-born females had a significantly increased rate of early neonatal death (IRR[se] = 3.00[1.29], p = 0.011), while higher birth weight females had a decreased rate (IRR[se] = 0.89[0.05], p = 0.039). In multivariate Poisson models, maternal litter size remained an independent predictor, explaining 13% of the variance in early neonatal death. We found that the later in the first week those neonates died, the more weight they lost. Together these findings suggest that triplet-born and low birth weight females have distinct developmental trajectories underlying greater rates of infant loss, losses that we suggest may be attributable to developmental disruption of infant feeding and carrying. Our findings of early life contributions to adult pregnancy outcomes in the common marmoset disrupt mother-blaming narratives of pregnancy outcomes in humans. These narratives hold that the pregnant person is solely responsible for pregnancy outcomes and the health of their children, independent of socioecological factors, a moralistic framing that has shaped clinical pregnancy management. It is necessary to differentiate temporal trajectories and causes of perinatal loss and view them as embedded in external processes to develop screening, diagnostic, and treatment tools that consider the full arc of a mother’s lived experience, from womb to womb and beyond.

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Late pregnancy ewe feeding and lamb performance in early life. 2. Factors associated with perinatal lamb mortality

Animal Science ◽

10.1017/s0003356100023667 ◽

1979 ◽

Vol 29 (3) ◽

pp. 401-410 ◽

Cited By ~ 27

Author(s):

A. M. Khalaf ◽

D. L. Doxey ◽

J. T. Baxter ◽

W. J. M. Black ◽

J. FitzSimons ◽

...

Keyword(s):

Birth Weight ◽

Litter Size ◽

Early Life ◽

Gamma Globulin ◽

Late Pregnancy ◽

Total Serum Protein ◽

Total Serum ◽

Factors Affecting ◽

Factors Associated ◽

Average Litter Size

ABSTRACTSome factors affecting perinatal lamb mortality were studied with 63 Finn × Dorset Horn ewes and 85 Scottish Half bred and Greyface ewes, having an average litter size of 2·26. Total perinatal lamb mortality averaged 29 % of which 44% were stillborn, 1 % attributed to dystocia, 35 % died between birth and 48 h of age, 14 % from 48 h to 10 days, and 5 % after 10 days.For the Finn × Dorset ewes, the 41 viable twin lambs weighed at birth 3·47 kg and 12 twin lambs which did not survive weighed 2·51 kg. Triplet weights were: viable 2·98 kg (34 lambs) and nonsurviving 2·00 kg (14). Quadruplet weights were: viable 2·79 kg (12) and non-surviving 1·90 kg (16). Quintuplet and sextuplet weights were: viable 2·45 kg (2) and non-surviving 1·35 kg (14).In the aggregated Halfbred and Greyface breeds, viable twin lambs weighed 4·5 kg at birth (91) and non-surviving 3·64 kg (11). Viable triplets weighed 3·77 kg (23) and non-surviving 2·68 kg (16).Serum gamma-globulin and total serum protein values were lower in the lambs which failed to survive, and this was particularly marked with triplets. Fractionating the gamma-globulins (IgG) indicated that IgGi was particularly low in non-viable lambs.Litter size, lamb birth weight, and colostrum intake by the lamb had important effects on perinatal lamb mortality.

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Reciprocal chromosome translocation between c-myc and immunoglobulin γ2b genes

Nature ◽

10.1038/305240a0 ◽

1983 ◽

Vol 305 (5931) ◽

pp. 240-243 ◽

Cited By ~ 31

Author(s):

Michael S. Neuberger ◽

Franco Calabi

Keyword(s):

Chromosome Translocation ◽

Reciprocal Chromosome Translocation

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Reciprocal Chromosome Translocation Between the Left-End 220kb of Chromosome II and the Right-End 270kb of Chromosome X in Saccharomyces cerevisiae

International Journal of Biology ◽

10.5539/ijb.v10n4p1 ◽

2018 ◽

Vol 10 (4) ◽

pp. 1

Author(s):

Masaharu Takeda ◽

Takahito Okushiba

Keyword(s):

Saccharomyces Cerevisiae ◽

Chromosome Translocation ◽

Original Strain ◽

Chromosome X ◽

A Cell ◽

Colony Color ◽

The Stability ◽

The Right ◽

Chromosome Ii ◽

Reciprocal Chromosome Translocation

Southern hybridization of chromosomes and the physical mapping of the genes used as several probes on the respective chromosomes II and X showed that the left-end ca. 220kb of chromosome II including ATP1 was exchanged the right-end ca. 270kb of chromosome X including ATP2 resulting the reciprocal chromosome translocation in the yeast strain YNN290, Saccharomyces cerevisiae. YTO290, the mutated strain by the reciprocal chromosome translocation as above described, was changed from red to white of the colony-color, and sizes of chromosome II lengthened from ca. 830kb to ca. 900kb and chromosome X shortened from ca. 760kb to ca. 690kb, respectively, in compared with the original strain YNN290. But, YTO290 strain was the same as the original strain YNN290 for other properties; the nutrient requiring of the genotype, the ploidy, the mitochondrial respiratory activity, the cell-size, and the growth-rate (doubling time), the number of chromosomes in a cell, It should be as a total number of nucleotides (bases) of genome.ATP1 or ATP2 and their neighboring base sequences respectively should be transferred from chromosome II left-end ca. 220kb to chromosome X right-end or chromosome X right-end ca. 270kb to chromosome II left-end accompanying with this reciprocal chromosome translocation. This mutated (the reciprocal chromosomes II and X translocation = exchanged those end-sequences as above described) strain, YTO290, seemed to lead to decrease the stability of the changed chromosomes II and X. The mutated strain, YTO290 might be observed to go back to the respective chromosomes II and X of the original strain, YNN290, in several months later even at 4°C.

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Molecular Characterization of the t(8; 13)(p11;q12) Translocation Associated With an Atypical Myeloproliferative Disorder: Evidence for Three Discrete Loci Involved in Myeloid Leukemias on 8p11

Blood ◽

10.1182/blood.v90.8.3136 ◽

1997 ◽

Vol 90 (8) ◽

pp. 3136-3141 ◽

Cited By ~ 34

Author(s):

Ivan H. Still ◽

Olga Chernova ◽

David Hurd ◽

Richard M. Stone ◽

John K. Cowell

Keyword(s):

Structural Rearrangement ◽

Chromosome Translocation ◽

Myeloproliferative Disorder ◽

Chromosome 8 ◽

Somatic Cell Hybrids ◽

Myeloid Leukemias ◽

Translocation Breakpoints ◽

Peripheral Blood Eosinophilia ◽

Reciprocal Chromosome Translocation

Abstract A reciprocal chromosome translocation between 13q12 and 8p11 is the consistent cytogenetic abnormality seen in a nonspecific myeloproliferative disorder that is associated with T-cell leukemia/lymphoma and peripheral blood eosinophilia. Detailed molecular analyses of the translocation breakpoints associated with this rearrangement have not been reported to date. We have now generated somatic cell hybrids from a newly described patient with this specific structural rearrangement and analyzed the breakpoints on the derivative chromosomes. We have shown that the breakpoint on chromosome 13 lies within a 300- to 500-kb region defined by the KIAA177 gene and D13S1123 marker. In addition, we have identified a 1.2-Mb YAC, 959A4, that crosses the translocation breakpoint on the short arm of chromosome 8 in this patient. The location of this breakpoint in 8p11 is distinct from the t(8; 16) and t(8; 22) translocations associated with M4/M5 myeloid leukemias, and suggests that three distinct loci located within 8p11 are involved in the pathogenesis of myeloid neoplasias.

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