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      人間染色體의 DNA複製에 關한 細胞遺傳學的 硏究  :  同時化시킨 淋巴球의 複製圖 Replication map of Synchronized Lymphocyte = Cytogenetic Study on Pattern of DNA Replication of Human Chromosomes

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      https://www.riss.kr/link?id=A40018403

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      Replication mapping of chromosomes has been developed very recently, employing 5-bromodeoxyuridine (BrdU), a base analogue of thymidine incorporated during the DNA-synthesis (S) phase of the cell cycle. Chromosomal regions with BrdU-substituted DNA possess the property of reducing the fluorescence of Hoechst 33258 fluorescent dyes or decreasing the staining intensity of Giemsa. These different cytological properties of BrdU-substituted DNA thus allow the precise localization of DNA replicating regions of chromosomes.
      The BrdU-Hoechst 33258-Giemsa technique was employed to study patterns of chromosomal replication in human lymphocytes synchronized by Methotrexate (MTX).
      PHA-stimulated human peripheral lymphocytes from chromosomally normal subjects were cultured synchronized, and pulsed with BrdU or thymidine.
      The results obtained are as follows:
      1. Synchronization of cultured lymphocytes with MTX and minimal exposure to colcemid produces sharp band definition and increased resolution in late prophase and prometaphase.
      2. Human chromosomes synthesize DNA in a segmental but highly coordinated fashion.
      3. The replication of the human genome is clearly biphasic. Euchromatin and intercalary and facultative heterochromatin replicate in a non-overlapping fashion.
      4. The late replicating elements, such as G-bands, the Yh, C-bands and the entire LX, initiate replication after it has been completed in the autosomal R-bands (euchromatin).
      5. Every prometaphase band is composed of a set of replication units or sub-band.
      This study confirms not only that chromosomal replication is tightly linked to chromosomal banding but also shows that this methodology is a potentially valuable clinical cytogenetic technique, because it:
      1) produces sharp band definition and increased resolution in late prophase and prometaphase subbands,
      2) differentiates not only the inactivated X chromosome from the rest of chromosomes but also segments of the Y Chromosome.
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      Replication mapping of chromosomes has been developed very recently, employing 5-bromodeoxyuridine (BrdU), a base analogue of thymidine incorporated during the DNA-synthesis (S) phase of the cell cycle. Chromosomal regions with BrdU-substituted DNA po...

      Replication mapping of chromosomes has been developed very recently, employing 5-bromodeoxyuridine (BrdU), a base analogue of thymidine incorporated during the DNA-synthesis (S) phase of the cell cycle. Chromosomal regions with BrdU-substituted DNA possess the property of reducing the fluorescence of Hoechst 33258 fluorescent dyes or decreasing the staining intensity of Giemsa. These different cytological properties of BrdU-substituted DNA thus allow the precise localization of DNA replicating regions of chromosomes.
      The BrdU-Hoechst 33258-Giemsa technique was employed to study patterns of chromosomal replication in human lymphocytes synchronized by Methotrexate (MTX).
      PHA-stimulated human peripheral lymphocytes from chromosomally normal subjects were cultured synchronized, and pulsed with BrdU or thymidine.
      The results obtained are as follows:
      1. Synchronization of cultured lymphocytes with MTX and minimal exposure to colcemid produces sharp band definition and increased resolution in late prophase and prometaphase.
      2. Human chromosomes synthesize DNA in a segmental but highly coordinated fashion.
      3. The replication of the human genome is clearly biphasic. Euchromatin and intercalary and facultative heterochromatin replicate in a non-overlapping fashion.
      4. The late replicating elements, such as G-bands, the Yh, C-bands and the entire LX, initiate replication after it has been completed in the autosomal R-bands (euchromatin).
      5. Every prometaphase band is composed of a set of replication units or sub-band.
      This study confirms not only that chromosomal replication is tightly linked to chromosomal banding but also shows that this methodology is a potentially valuable clinical cytogenetic technique, because it:
      1) produces sharp band definition and increased resolution in late prophase and prometaphase subbands,
      2) differentiates not only the inactivated X chromosome from the rest of chromosomes but also segments of the Y Chromosome.

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