Evidence of clonal attenuation, clonal succession, and clonal expansion in mass cultures of aging Werner’s syndrome skin fibroblasts

Salk, Darrell; Au, Kam; Hoehn, Holger; Stenchever, Marc R.; Martin, George M.

doi:10.1159/000131597

Cited by 62 publications

(32 citation statements)

References 8 publications

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“…Other data support the concept of clonal succession during in vitro passage of human fibroblast cultures (30), and heterogeneity in growth characteristics of clones has been reported by several others (1,4,14,22,24,31). Indeed, it has also been shown that a large proportion of cells in a mass culture possess very limited proliferative capacity (32) and that the maximum MPD of clones which make up the mass culture are bimodally distributed (31, 33).…”

Section: -He Clonat Selection Hypothesissupporting

confidence: 76%

“…Three clones (13,26,32) were assayed only at one stage. Of the remaining clones, two groups could be identified: group A, comprising seven clones (2,10,13,18,29,30,36), in which the error frequency remained relatively constant through subsequent passage although clones 10 and 29 were only assayed singly at two passage levels; group B, comprising two clones (8 and 14) in which an abrupt increase in error frequency at later passage was observed. It bears emphasis that these two clones were the only cases in which an increase in error frequency was observed with passage among all such determinations on mass cultures or clonal populations.…”

Section: Clonal Error Frequenciesmentioning

confidence: 99%

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Clonal selection in cultured human fibroblasts: role of protein synthetic errors.

Wojtyk¹,

Goldstein²

1982

The Journal of Cell Biology

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Protein synthetic error frequency, determined in cell-free extracts as Aleu/Aphe incorporation following poly(U) stimulation, has been found to decrease progressively in several strains of human diploid fibroblasts during their limited replicative lifespan. To explore the basis of this phenomenon, we followed a mass (uncloned) culture of one normal strain at 13 stages of its replicative lifespan. We found a progressive tenfold decline in error frequency that was inversely correlated with passage level (r = -.93, p <.001). This could not be ascribed to the slow rates of replication associated with fibroblast senescence because slowing of growth by serum deprivation did not change error frequency. Additionally, terminal mass cultures maintained for 16 wk at saturation density to minimize cell selection did not change error frequency over this time. Error frequencies in 12 individual clones purified from the parental culture did not decline on repeated passage, either remaining constant or, in two clones, rising abruptly three-to five-fold after initial assays. Error frequencies of clones showed a weak inverse correlation with growth vigor but not with the maximum doubling number. We conclude that selective pressures favor more vigorously dividing clones with low protein synthetic error frequencies leading to their predominance in mass cultures.

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Section: -He Clonat Selection Hypothesissupporting

confidence: 76%

Section: Clonal Error Frequenciesmentioning

confidence: 99%

Clonal selection in cultured human fibroblasts: role of protein synthetic errors.

Wojtyk¹,

Goldstein²

1982

The Journal of Cell Biology

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“…A plausible explanation is that this reflects a phenomenon termed clonal succession, described in Salk et al [37]. In this report, mass cultures of skin fibroblasts derived from Werner syndrome patients were examined cytogenetically throughout their entire replicative lifespans.…”

Section: Discussionmentioning

confidence: 80%

Accelerated telomere shortening and replicative senescence in human fibroblasts overexpressing mutant and wild-type lamin A

Huang

Risques

Martin

et al. 2008

Experimental Cell Research

115

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LMNA mutations are responsible for a variety of genetic disorders, including muscular dystrophy, lipodystrophy, and certain progeroid syndromes, notably Hutchinson-Gilford Progeria. Although a number of clinical features of these disorders are suggestive of accelerated aging, it is not known whether cells derived from these patients exhibit cellular phenotypes associated with accelerated aging. We examined a series of isogenic skin fibroblast lines transfected with LMNA constructs bearing known pathogenic point mutations or deletion mutations found in progeroid syndromes. Fibroblasts overexpressing mutant lamin A exhibited accelerated rates of loss of telomeres and shortened replicative lifespans, in addition to abnormal nuclear morphology. To our surprise, these abnormalities were also observed in lines overexpressing wild-type lamin A. Copy number variants are common in human populations; those involving LMNA, whether arising meiotically or mitotically, might lead to progeroid phenotypes. In an initial pilot study of 23 progeroid cases without detectible WRN or LMNA mutations, however, no cases of altered LMNA copy number were detected. Nevertheless, our findings raise a hypothesis that changes in lamina organization may cause accelerated telomere attrition, with different kinetics for overexpession of wild-type and mutant lamin A, which leads to rapid replicative senescence and progroid phenotypes.

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“…Death generally occurs in the fifth decade of life, primarily from cancer and cardiovascular disease. Cells from WS individuals have a short replicative lifespan in culture, and exhibit genomic instability characterized by chromosomal variegated translocation mosaicism (Salk et al ., 1981). WRN , the gene defective in WS, encodes a protein that is homologous to the E. coli RECQ helicase, which plays an important role in recombinational repair of DNA damage (Yu et al ., 1996).…”

Section: Introductionmentioning

confidence: 99%

WRN, the protein deficient in Werner syndrome, plays a critical structural role in optimizing DNA repair

et al. 2003

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SummaryWerner syndrome (WS) predisposes patients to cancer and premature aging, owing to mutations in WRN . The WRN protein is a RECQ-like helicase and is thought to participate in DNA double-strand break (DSB) repair by non-homologous end joining (NHEJ) or homologous recombination (HR). It has been previously shown that non-homologous DNA ends develop extensive deletions during repair in WS cells, and that this WS phenotype was complemented by wild-type ( Moreover, WRN appears to play a structural role, independent of its enzymatic activities, in optimizing HR and efficient NHEJ repair. Another human RECQ helicase, BLM, suppressed HR but had little or no effect on NHEJ, suggesting that mammalian RECQ helicases have distinct functions that can finely regulate recombination events.

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Evidence of clonal attenuation, clonal succession, and clonal expansion in mass cultures of aging Werner’s syndrome skin fibroblasts

Cited by 62 publications

References 8 publications

Clonal selection in cultured human fibroblasts: role of protein synthetic errors.

Clonal selection in cultured human fibroblasts: role of protein synthetic errors.

Accelerated telomere shortening and replicative senescence in human fibroblasts overexpressing mutant and wild-type lamin A

WRN, the protein deficient in Werner syndrome, plays a critical structural role in optimizing DNA repair

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