Analysis of function of Gap-Rac, CalB regions of the bcr/abl cDNA using bcr/abl-expressing transgenic mice

2004 Fiscal Year Final Research Report Summary

• Project/Area Number: 15591028
• Research Category: Grant-in-Aid for Scientific Research (C)
• Allocation Type: Single-year Grants
• Section: 一般
• Research Field: Hematology
• Research Institution: Nippon Medical School
• Principal Investigator: INOKUCHI Koiti Nippon Medical School, Dept.of Internal Medicine, Associate Professor, 医学部, 助教授 (10203267)
• Project Period (FY): 2003 – 2004
• Keywords: P230 BCR / ABL / Transgenic mouse / MPD / GAP^<rac> domain / thrombocytosis / Abl / CalB

Research Abstract

Leukemogenesis was investigated with molecular biological methods using bcr/abl cDNA micro-injection into eggs. Micro type bcr-abl (p230 bcr/abl) transcript was revealed to make CML patients atypical clinical courses other than typical CML. A novel transgenic mouse expressing p230 bcr/abl cDNA was succeeded to make. The transgenic mouse has a disease phenotype of CML with thrombocytosis. Transgenic mice expressing abnormal p51/p63 or the novel gene are now under making. Biological function of abnormalities of these p51/p63 and the novel gene are investigating with mutagenesis method. The reported transgenic mice expressed the p230 BCR/ABL gene under control of the promoter of the long terminal repeat, PCMV, of the murine stem cell virus of the MSCV vector. Two founder mice exhibited myeloproliferative disease(MPD) mimicking CML. The disease phenotype of the MPD caused by P230BCR/ABL was characterized by mild granulocytosis, a high platelet count, infiltration of megakaryocytes in some organs, and a longer disease latency compared with the MPD caused by P210 BCR/ABL. The leukemic cells expanded extramedullarily in the liver. Many immature and mature granulocytes and many megakaryocytes had infiltrated various tissues, i.e., the lung, spleen, bone marrow and kidney. The phenotype of the blasts analysed by immunohistochemistry and flow cytometry revealed the characteristics of the myeloblasts. The leukocyte counts for the transgenic progeny gradually increased after 11 months. The mean platelet counts gradually increased after 9 months of age. MPD becomes overt 13-15 months after birth.
The reason for making this MPD model mice may be its use of the p230 BCR/ABL gene, which is less cytotoxic than p210 BCR/ABL. The level of bcr/abl expression is low in all tissues except the hematopoietic cells[29]. This limited expression pattern may permit successful creation of MPD model mice.
There is a hypothesis that in humans the relative level of BCR/ABL expression may be a determinant in the severity of the phenotype of BCR/ABL-positive leukemia. Patients having P230 BCR/ABL had the two disease phenotype of Ph-positive ET or chronic neutrophilic leukemia(CNL) [36,39,40]. The disease phenotypes of ET and CNL are possibly a result of the expression level of the P230 BCR/ABL protein. The difference in the expression level may influence the disease phenotype in the transgenic mice. To clarify this, additional molecular studies will be needed. The transgenic mouse system using PCMV expresses P230 BCR/ABL transcripts at a high level [29]. This evidence of an overt disease phenotype in P230 BCR/ABL expression model mouse supports the hypothesis.
A second hypothesis is the existernce of molecular differences in bcr/abl molecules [41-43]. Molecular differences between p210 BCR/ABL cDNA and p230 BCR/ABL cDNA may be an important disease determinant in both humans and transgenic mice. P210 and P230 BCR/ABL contain some potential functional motifs encoded by the BCR portion of the fusion gene. The Dbl-like and pleckstrin homology domains exist in the bcr sequence of both P210 and P230 Bcr/Abl [43]. The CalB and GAP^<rac> domains [44,45] in P230 Bcr/Abl may directly influence the ability of this protein to transform various hematopoietic precursors by inhibition of lymphoid development and/or by promotion of myeloid and megakaryocyte development. It is possible that the additional her sequences included within P230 BCR/ABL, specifically the GAP^<rac> domain, may function to partially abrogate the properties of activated p21 Rac in P230 Bcr/Abl-expressing hematopoietic cells. These potential motifs might be involved in the differences in the disease phenotype between P210 BCR/ABL and P230 BCR/ABL transgenic mice.

Research Products

• [Journal Article] Antiangiogenic gene therapy of myeloproliferative disease developed in transgenic mice expressing P230 bcr/abl. (2005)
  • Author(s): Miyake K, Inokuchi K, et al.
  • Journal Title: Gene Therapy 12(6) Pages: 541-545
  • Description: 「研究成果報告書概要(和文)」より
• [Journal Article] A case presenting concurrence of Marfan syndrome, Basedow's disease and Arg353Gln polymorphism-related factor VII deficiency. (2005)
  • Author(s): Tanaka K, Seino Y, et al.
  • Journal Title: International Journal of Cardiology 98(3) Pages: 345-348
  • Description: 「研究成果報告書概要(和文)」より
• [Journal Article] Transgenic mouse models of BCR/ABL-positive myelogenous...... (2005)
  • Author(s): Koiti Inokuchi.
  • Journal Title: Current Genomics 6(3) Pages: 1-7
  • Description: 「研究成果報告書概要(和文)」より
• [Journal Article] Antiangiogenic gene therapy of myeloproliferative disease developed in transgenic mice expressing P230 bcr/abl. (2005)
  • Author(s): Koiti Inokuchi, Koichi Miyake, Noriko Miyake, Kazuo Dan, Takashi Shimada
  • Journal Title: Gene Ther. 12(6) Pages: 541-545
  • Description: 「研究成果報告書概要(欧文)」より
• [Journal Article] Transgenic mouse models of BCR/ABL-positive chronic myelogenous leukemia : A review. (2005)
  • Author(s): Koiti Inokuchi
  • Journal Title: Current Genomics [Epub ahead of print] 6(3) Pages: 1-7
  • Description: 「研究成果報告書概要(欧文)」より
• [Journal Article] Abnormalities of p51,p53,FLT3 and N-ras genes and their prognostic value in relapsed acute myeloid leukemia. (2004)
  • Author(s): Nakamura H, Inokuchi K, et al.
  • Journal Title: Journal of Nippon Medical School 71(4) Pages: 270-278
  • Description: 「研究成果報告書概要(和文)」より
• [Journal Article] P230BCR/ABLトランスジェニックマウス (2003)
  • Author(s): 猪口孝一
  • Journal Title: 血液・腫瘍科 46 Pages: 436-443
  • Description: 「研究成果報告書概要(和文)」より
• [Journal Article] Novel transgenic mice expressing P230 Bcr/Abl developed myeloproliferative disorder : longer disease latency, thrombocytosis and mild leukocytosis (2003)
  • Author(s): Koiti Inokuchi, Kazuo Dan, Miyuki Takatori, Hidemasa Takahuji, Naoya Uchida, Mitsuharu Inami, Koichi Miyake, Hiroaki Honda, Hisamaru Hirai, Takashi Shimada
  • Journal Title: Blood 102(1) Pages: 320-323
  • Description: 「研究成果報告書概要(欧文)」より
• [Journal Article] Simultaneous novel BCR-ABL gene mutation and increased expression of BCR-ABL mRNA caused clinical resistance to STI571 in double-Ph-positive acute biphenotypie leukemia. (2003)
  • Author(s): Mitsuharu Inami, Koiti Inokuchi, Kazutaka Nakayama, Hideo Yamura, Takashi Shimada, Kazuo Dan
  • Journal Title: International Journal of Hematology 78(2) Pages: 173-175
  • Description: 「研究成果報告書概要(欧文)」より
• [Journal Article] Abnormality of c-Kit Oncoprotein in Certain Patients With Chronic Myelogenous Leukemia - Potential Clinical Significance. (2002)
  • Author(s): Koiti Inokuchi, Hiroki Yamaguchi, Miki Tarusawa, Makoto Futaki, Hideki Hanawa, Sakae Tanosaki, Kazuo Dan
  • Journal Title: Leukemia 16 Pages: 170-177
  • Description: 「研究成果報告書概要(欧文)」より
• [Journal Article] Loss of DCC gene expression is of prongostic importantce in acute myelogenous leukemia. (2002)
  • Author(s): Koiti Inokuchi, Hiroki Yamaguchi, Hideki Hanawa, Tanosaki S, Nakamura K, Miki Tarusawa, Miyake K, Shimada T, Kazuo Dan
  • Journal Title: Clinical Cancer Research 8(6) Pages: 1882-1888
  • Description: 「研究成果報告書概要(欧文)」より