Pathophysiology of a sickle cell trait mouse model: Human αβS transgenes with one mouse β-globin allele

Constance T. Noguchi; Mark Gladwin; Bhalchandra Diwan; Patrick Merciris; Reginald Smith; Xiaobing Yu; Gregory Buzard; Anthony Fitzhugh; Larry K. Keefer; Alan N. Schechter; Narla Mohandas

doi:10.1006/bcmd.2001.0469

Pathophysiology of a sickle cell trait mouse model: Human αβ^S transgenes with one mouse β-globin allele

Constance T. Noguchi, Mark Gladwin, Bhalchandra Diwan, Patrick Merciris, Reginald Smith, Xiaobing Yu, Gregory Buzard, Anthony Fitzhugh, Larry K. Keefer, Alan N. Schechter, Narla Mohandas

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

As a potential model for sickle cell trait (AS), we examined mice containing one normal mouse β-globin allele in combination with a human hemoglobin S (hαβ^s) transgene (mβ/hS). The mice segregated into two subpopulations containing low and high proportions of hemoglobin S (mβ/hS1 and mβ/hS2, respectively) that was associated with one or two human hαβ^s transgenes. We noted striking kidney pathology (cortical cysts, hyperplastic tubules, and glomerulonephritis), increasing with age and with greater severity in mβ/hS1. mβ/hS2 animals were largely tolerant to 5% O₂ for 1 h, whereas 80% of mβ/hS1 mice died, exhibiting acute sequestration of erythrocytes in spleen, liver, and heart. These pathologies appear to result from a decreased oxygen affinity of the hybrid (human α/mouse β) hemoglobins with a mild β-thalassemia phenotype. Thus, these mouse models of sickle trait seem to manifest their renal pathology and sensitivity to hypoxia by mechanisms related to low tissue oxygen delivery and are different from the human syndrome. Analyses of parameters such as P₅₀, red cell indices, and genetic background are necessary in establishing potential relevance of any mouse model of the sickle cell syndromes.

Original language	English
Pages (from-to)	971-977
Number of pages	7
Journal	Blood Cells, Molecules, and Diseases
Volume	27
Issue number	6
DOIs	https://doi.org/10.1006/bcmd.2001.0469
State	Published - 2001
Externally published	Yes

Keywords

Kidney pathology
Oxygen affinity
Pathophysiology
Sickle cell trait
Transgenic mouse

Access to Document

10.1006/bcmd.2001.0469

Cite this

@article{253a09db1c6c4e54bbda6c132c2aebbe,

title = "Pathophysiology of a sickle cell trait mouse model: Human αβS transgenes with one mouse β-globin allele",

abstract = "As a potential model for sickle cell trait (AS), we examined mice containing one normal mouse β-globin allele in combination with a human hemoglobin S (hαβs) transgene (mβ/hS). The mice segregated into two subpopulations containing low and high proportions of hemoglobin S (mβ/hS1 and mβ/hS2, respectively) that was associated with one or two human hαβs transgenes. We noted striking kidney pathology (cortical cysts, hyperplastic tubules, and glomerulonephritis), increasing with age and with greater severity in mβ/hS1. mβ/hS2 animals were largely tolerant to 5% O2 for 1 h, whereas 80% of mβ/hS1 mice died, exhibiting acute sequestration of erythrocytes in spleen, liver, and heart. These pathologies appear to result from a decreased oxygen affinity of the hybrid (human α/mouse β) hemoglobins with a mild β-thalassemia phenotype. Thus, these mouse models of sickle trait seem to manifest their renal pathology and sensitivity to hypoxia by mechanisms related to low tissue oxygen delivery and are different from the human syndrome. Analyses of parameters such as P50, red cell indices, and genetic background are necessary in establishing potential relevance of any mouse model of the sickle cell syndromes.",

keywords = "Kidney pathology, Oxygen affinity, Pathophysiology, Sickle cell trait, Transgenic mouse",

author = "Noguchi, {Constance T.} and Mark Gladwin and Bhalchandra Diwan and Patrick Merciris and Reginald Smith and Xiaobing Yu and Gregory Buzard and Anthony Fitzhugh and Keefer, {Larry K.} and Schechter, {Alan N.} and Narla Mohandas",

note = "Funding Information: We thank Dr. Jerrold Ward for assistance with pathology and photomicrography and Dan Logsdon for expert technical help with the mice. The project was funded in part by the National Cancer Institute, Contract NO1-CO-56000, and by NIH Grant HL31579.",

year = "2001",

doi = "10.1006/bcmd.2001.0469",

language = "English",

volume = "27",

pages = "971--977",

journal = "Blood Cells, Molecules, and Diseases",

issn = "1079-9796",

publisher = "Academic Press Inc.",

number = "6",

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TY - JOUR

T1 - Pathophysiology of a sickle cell trait mouse model

T2 - Human αβS transgenes with one mouse β-globin allele

AU - Noguchi, Constance T.

AU - Gladwin, Mark

AU - Diwan, Bhalchandra

AU - Merciris, Patrick

AU - Smith, Reginald

AU - Yu, Xiaobing

AU - Buzard, Gregory

AU - Fitzhugh, Anthony

AU - Keefer, Larry K.

AU - Schechter, Alan N.

AU - Mohandas, Narla

N1 - Funding Information: We thank Dr. Jerrold Ward for assistance with pathology and photomicrography and Dan Logsdon for expert technical help with the mice. The project was funded in part by the National Cancer Institute, Contract NO1-CO-56000, and by NIH Grant HL31579.

PY - 2001

Y1 - 2001

N2 - As a potential model for sickle cell trait (AS), we examined mice containing one normal mouse β-globin allele in combination with a human hemoglobin S (hαβs) transgene (mβ/hS). The mice segregated into two subpopulations containing low and high proportions of hemoglobin S (mβ/hS1 and mβ/hS2, respectively) that was associated with one or two human hαβs transgenes. We noted striking kidney pathology (cortical cysts, hyperplastic tubules, and glomerulonephritis), increasing with age and with greater severity in mβ/hS1. mβ/hS2 animals were largely tolerant to 5% O2 for 1 h, whereas 80% of mβ/hS1 mice died, exhibiting acute sequestration of erythrocytes in spleen, liver, and heart. These pathologies appear to result from a decreased oxygen affinity of the hybrid (human α/mouse β) hemoglobins with a mild β-thalassemia phenotype. Thus, these mouse models of sickle trait seem to manifest their renal pathology and sensitivity to hypoxia by mechanisms related to low tissue oxygen delivery and are different from the human syndrome. Analyses of parameters such as P50, red cell indices, and genetic background are necessary in establishing potential relevance of any mouse model of the sickle cell syndromes.

AB - As a potential model for sickle cell trait (AS), we examined mice containing one normal mouse β-globin allele in combination with a human hemoglobin S (hαβs) transgene (mβ/hS). The mice segregated into two subpopulations containing low and high proportions of hemoglobin S (mβ/hS1 and mβ/hS2, respectively) that was associated with one or two human hαβs transgenes. We noted striking kidney pathology (cortical cysts, hyperplastic tubules, and glomerulonephritis), increasing with age and with greater severity in mβ/hS1. mβ/hS2 animals were largely tolerant to 5% O2 for 1 h, whereas 80% of mβ/hS1 mice died, exhibiting acute sequestration of erythrocytes in spleen, liver, and heart. These pathologies appear to result from a decreased oxygen affinity of the hybrid (human α/mouse β) hemoglobins with a mild β-thalassemia phenotype. Thus, these mouse models of sickle trait seem to manifest their renal pathology and sensitivity to hypoxia by mechanisms related to low tissue oxygen delivery and are different from the human syndrome. Analyses of parameters such as P50, red cell indices, and genetic background are necessary in establishing potential relevance of any mouse model of the sickle cell syndromes.

KW - Kidney pathology

KW - Oxygen affinity

KW - Pathophysiology

KW - Sickle cell trait

KW - Transgenic mouse

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DO - 10.1006/bcmd.2001.0469

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AN - SCOPUS:0035544703

SN - 1079-9796

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