Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus

Dong Ye Youn; Dong Hyoung Lee; Mi Hyun Lim; Jung Sook Yoon; Hee Lim Ji; Eun Jung Seung; Eun Yeum Chung; Whee Park Cheol; Ho Joong Youn; Jae Seon Lee; Seong Beom Lee; Masahito Ikawa; Masaru Okabe; Yoshihide Tsujimoto; Jeong Hwa Lee

doi:10.1152/ajpendo.90704.2008

Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus

Dong Ye Youn, Dong Hyoung Lee, Mi Hyun Lim, Jung Sook Yoon, Hee Lim Ji, Eun Jung Seung, Eun Yeum Chung, Whee Park Cheol, Ho Joong Youn, Jae Seon Lee, Seong Beom Lee, Masahito Ikawa, Masaru Okabe, Yoshihide Tsujimoto, Jeong Hwa Lee

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

30 Scopus citations

Abstract

Bcl-2 interacting cell death suppressor (Bis), also known as Bag3 or CAIR-1, is involved in antistress and antiapoptotic pathways. In addition to Bcl-2, Bis binds to several proteins, suggesting it has diverse functions in normal and pathological conditions. To better define the physiological function of Bis in vivo, we developed bis-deficient mice with a cre-loxP system. Targeted disruption of exon 4 of the bis gene was demonstrated by Southern blotting and PCR, and Western blotting showed that no intact or truncated Bis protein was synthesized in bis^-/- mice. While heterozygotes were fertile and appeared normal, Bis-deficient mice showed growth retardation and died by 3 wk after birth. The relative weight of the thymus and spleen was reduced and the total numbers of white blood cells, splenocytes, and thymocytes were significantly reduced compared with wild-type littermates. Serum profiles indicated significant hypoglycemia as well as decrease in triglyceride and cholesterol levels. Expression profiles of metabolic genes indicated that gluconeogenesis and β-oxidation are activated in the liver of bis ^-/- mice. This activation, as well as a decrease in peripheral fat and an induction of fatty liver, appears to be an adaptive response to hypoglycemia. Our study reveals that the absence of Bis has considerable influences on postnatal growth and survival, possibly due to a nutritional impairment.

Original language	English
Pages (from-to)	E1349-E1357
Journal	American Journal of Physiology - Endocrinology and Metabolism
Volume	295
Issue number	6
DOIs	https://doi.org/10.1152/ajpendo.90704.2008
State	Published - Dec 2008

Keywords

Hypoglycemia
Knockout
bis

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1152/ajpendo.90704.2008

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Youn, D. Y., Lee, D. H., Lim, M. H., Yoon, J. S., Ji, H. L., Seung, E. J., Chung, E. Y., Cheol, W. P., Youn, H. J., Lee, J. S., Lee, S. B., Ikawa, M., Okabe, M., Tsujimoto, Y., & Lee, J. H. (2008). Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus. American Journal of Physiology - Endocrinology and Metabolism, 295(6), E1349-E1357. https://doi.org/10.1152/ajpendo.90704.2008

@article{ffcd89d0e1b94a85abe63bd0eb07079f,

title = "Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus",

abstract = "Bcl-2 interacting cell death suppressor (Bis), also known as Bag3 or CAIR-1, is involved in antistress and antiapoptotic pathways. In addition to Bcl-2, Bis binds to several proteins, suggesting it has diverse functions in normal and pathological conditions. To better define the physiological function of Bis in vivo, we developed bis-deficient mice with a cre-loxP system. Targeted disruption of exon 4 of the bis gene was demonstrated by Southern blotting and PCR, and Western blotting showed that no intact or truncated Bis protein was synthesized in bis-/- mice. While heterozygotes were fertile and appeared normal, Bis-deficient mice showed growth retardation and died by 3 wk after birth. The relative weight of the thymus and spleen was reduced and the total numbers of white blood cells, splenocytes, and thymocytes were significantly reduced compared with wild-type littermates. Serum profiles indicated significant hypoglycemia as well as decrease in triglyceride and cholesterol levels. Expression profiles of metabolic genes indicated that gluconeogenesis and β-oxidation are activated in the liver of bis -/- mice. This activation, as well as a decrease in peripheral fat and an induction of fatty liver, appears to be an adaptive response to hypoglycemia. Our study reveals that the absence of Bis has considerable influences on postnatal growth and survival, possibly due to a nutritional impairment.",

keywords = "Hypoglycemia, Knockout, bis",

author = "Youn, {Dong Ye} and Lee, {Dong Hyoung} and Lim, {Mi Hyun} and Yoon, {Jung Sook} and Ji, {Hee Lim} and Seung, {Eun Jung} and Chung, {Eun Yeum} and Cheol, {Whee Park} and Youn, {Ho Joong} and Lee, {Jae Seon} and Lee, {Seong Beom} and Masahito Ikawa and Masaru Okabe and Yoshihide Tsujimoto and Lee, {Jeong Hwa}",

year = "2008",

month = dec,

doi = "10.1152/ajpendo.90704.2008",

language = "English",

volume = "295",

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journal = "American Journal of Physiology - Endocrinology and Metabolism",

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Youn, DY, Lee, DH, Lim, MH, Yoon, JS, Ji, HL, Seung, EJ, Chung, EY, Cheol, WP, Youn, HJ, Lee, JS, Lee, SB, Ikawa, M, Okabe, M, Tsujimoto, Y & Lee, JH 2008, 'Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus', American Journal of Physiology - Endocrinology and Metabolism, vol. 295, no. 6, pp. E1349-E1357. https://doi.org/10.1152/ajpendo.90704.2008

TY - JOUR

T1 - Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus

AU - Youn, Dong Ye

AU - Lee, Dong Hyoung

AU - Lim, Mi Hyun

AU - Yoon, Jung Sook

AU - Ji, Hee Lim

AU - Seung, Eun Jung

AU - Chung, Eun Yeum

AU - Cheol, Whee Park

AU - Youn, Ho Joong

AU - Lee, Jae Seon

AU - Lee, Seong Beom

AU - Ikawa, Masahito

AU - Okabe, Masaru

AU - Tsujimoto, Yoshihide

AU - Lee, Jeong Hwa

PY - 2008/12

Y1 - 2008/12

N2 - Bcl-2 interacting cell death suppressor (Bis), also known as Bag3 or CAIR-1, is involved in antistress and antiapoptotic pathways. In addition to Bcl-2, Bis binds to several proteins, suggesting it has diverse functions in normal and pathological conditions. To better define the physiological function of Bis in vivo, we developed bis-deficient mice with a cre-loxP system. Targeted disruption of exon 4 of the bis gene was demonstrated by Southern blotting and PCR, and Western blotting showed that no intact or truncated Bis protein was synthesized in bis-/- mice. While heterozygotes were fertile and appeared normal, Bis-deficient mice showed growth retardation and died by 3 wk after birth. The relative weight of the thymus and spleen was reduced and the total numbers of white blood cells, splenocytes, and thymocytes were significantly reduced compared with wild-type littermates. Serum profiles indicated significant hypoglycemia as well as decrease in triglyceride and cholesterol levels. Expression profiles of metabolic genes indicated that gluconeogenesis and β-oxidation are activated in the liver of bis -/- mice. This activation, as well as a decrease in peripheral fat and an induction of fatty liver, appears to be an adaptive response to hypoglycemia. Our study reveals that the absence of Bis has considerable influences on postnatal growth and survival, possibly due to a nutritional impairment.

AB - Bcl-2 interacting cell death suppressor (Bis), also known as Bag3 or CAIR-1, is involved in antistress and antiapoptotic pathways. In addition to Bcl-2, Bis binds to several proteins, suggesting it has diverse functions in normal and pathological conditions. To better define the physiological function of Bis in vivo, we developed bis-deficient mice with a cre-loxP system. Targeted disruption of exon 4 of the bis gene was demonstrated by Southern blotting and PCR, and Western blotting showed that no intact or truncated Bis protein was synthesized in bis-/- mice. While heterozygotes were fertile and appeared normal, Bis-deficient mice showed growth retardation and died by 3 wk after birth. The relative weight of the thymus and spleen was reduced and the total numbers of white blood cells, splenocytes, and thymocytes were significantly reduced compared with wild-type littermates. Serum profiles indicated significant hypoglycemia as well as decrease in triglyceride and cholesterol levels. Expression profiles of metabolic genes indicated that gluconeogenesis and β-oxidation are activated in the liver of bis -/- mice. This activation, as well as a decrease in peripheral fat and an induction of fatty liver, appears to be an adaptive response to hypoglycemia. Our study reveals that the absence of Bis has considerable influences on postnatal growth and survival, possibly due to a nutritional impairment.

KW - Hypoglycemia

KW - Knockout

KW - bis

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U2 - 10.1152/ajpendo.90704.2008

DO - 10.1152/ajpendo.90704.2008

M3 - Article

C2 - 18840758

AN - SCOPUS:57349143456

SN - 0193-1849

VL - 295

SP - E1349-E1357

JO - American Journal of Physiology - Endocrinology and Metabolism

JF - American Journal of Physiology - Endocrinology and Metabolism

IS - 6

ER -

Bis deficiency results in early lethality with metabolic deterioration and involution of spleen and thymus

Abstract

Keywords

UN SDGs

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