Female mice are more susceptible to developing inflammatory disorders due to impaired transforming growth factor beta signaling in salivary glands

Nandula, Seshagiri R.; Amarnath, Shoba; Molinolo, Alfredo; Bandyopadhyay, Bidhan C.; Hall, Bradford; Goldsmith, Corinne M.; Zheng, Changyu; Larsson, Jonas; Sreenath, Taduru; Chen, WanJun; Ambudkar, Indu S.; Karlsson, Stefan; Baum, Bruce J.; Kulkarni, Ashok B.

Female mice are more susceptible to developing inflammatory disorders due to impaired transforming growth factor beta signaling in salivary glands

Mark

Nandula, Seshagiri R. ; Amarnath, Shoba ; Molinolo, Alfredo ; Bandyopadhyay, Bidhan C. ; Hall, Bradford ; Goldsmith, Corinne M. ; Zheng, Changyu ; Larsson, Jonas ^LU ; Sreenath, Taduru and Chen, WanJun , et al. (2007) In Arthritis and Rheumatism 56(6). p.1798-1805

Abstract: Objective. Transforming growth factor 13 (TGF)3) plays a key role in the onset and resolution of autoimmune diseases and chronic inflammation. The aim of this study was to delineate the precise function of TGF beta signaling in salivary gland inflammation. Methods. We impaired TGF beta signaling in mouse salivary glands by conditionally inactivating expression of TGF beta receptor type I (TGF beta RI), either by using mouse mammary tumor virus-Cre mice or by delivering adenoviral vector containing Cre to mouse salivary glands via retrograde infusion of the cannulated main excretory ducts of submandibular glands. Results. TGF beta RI-conditional knockout (TGF beta RI-coko) mice were born normal; however, female TGF beta RI-coko mice... (More); Objective. Transforming growth factor 13 (TGF)3) plays a key role in the onset and resolution of autoimmune diseases and chronic inflammation. The aim of this study was to delineate the precise function of TGF beta signaling in salivary gland inflammation. Methods. We impaired TGF beta signaling in mouse salivary glands by conditionally inactivating expression of TGF beta receptor type I (TGF beta RI), either by using mouse mammary tumor virus-Cre mice or by delivering adenoviral vector containing Cre to mouse salivary glands via retrograde infusion of the cannulated main excretory ducts of submandibular glands. Results. TGF beta RI-conditional knockout (TGF beta RI-coko) mice were born normal; however, female TGF beta RI-coko mice developed severe multifocal inflammation in salivary and mammary glands and in the heart. The inflammatory disorder affected normal growth and resulted in the death of the mice at ages 4-5 weeks. Interestingly, male TGF beta RI-coko mice did not exhibit any signs of inflammation. The female TGF beta RI-coko mice also showed an increase in Th1 proinflammatory cytokines in salivary glands and exhibited an up-regulation of peripheral T cells. In addition, these mice showed an atypical distribution of aquaporin 5 in their salivary glands, suggesting likely secretory impairment. Administration of an adenoviral vector encoding Cre recombinase into the salivary glands resulted in inflammatory foci only in the glands of female TGF beta RI-loxP-flanked (floxed) mice (TGF beta RI-f/f mice), but not in those of male and female wild-type mice or male TGF beta RI-f/f mice. Conclusion. These results suggest that female mice are uniquely more susceptible to developing inflammatory disorders due to impaired TGF beta signaling in their salivary glands. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/649002

author

Nandula, Seshagiri R. ; Amarnath, Shoba ; Molinolo, Alfredo ; Bandyopadhyay, Bidhan C. ; Hall, Bradford ; Goldsmith, Corinne M. ; Zheng, Changyu ; Larsson, Jonas ^LU ; Sreenath, Taduru and Chen, WanJun , et al. (More)

Nandula, Seshagiri R. ; Amarnath, Shoba ; Molinolo, Alfredo ; Bandyopadhyay, Bidhan C. ; Hall, Bradford ; Goldsmith, Corinne M. ; Zheng, Changyu ; Larsson, Jonas ^LU ; Sreenath, Taduru ; Chen, WanJun ; Ambudkar, Indu S. ; Karlsson, Stefan ^LU

; Baum, Bruce J. and Kulkarni, Ashok B. (Less)

organization

Division of Molecular Medicine and Gene Therapy

publishing date

2007

type

Contribution to journal

publication status

published

subject

Rheumatology and Autoimmunity

in

Arthritis and Rheumatism

volume

56

issue

6

pages

1798 - 1805

publisher

John Wiley & Sons Inc.

external identifiers

wos:000247164300009
scopus:34447526525
pmid:17530708

ISSN

1529-0131

DOI

10.1002/art.22715

language

English

LU publication?

yes

id

35ff0f3c-4cd6-448c-9e10-2d02c1c15566 (old id 649002)

date added to LUP

2016-04-01 11:59:37

date last changed

2022-01-26 21:17:17

@article{35ff0f3c-4cd6-448c-9e10-2d02c1c15566,
  abstract     = {{Objective. Transforming growth factor 13 (TGF)3) plays a key role in the onset and resolution of autoimmune diseases and chronic inflammation. The aim of this study was to delineate the precise function of TGF beta signaling in salivary gland inflammation. Methods. We impaired TGF beta signaling in mouse salivary glands by conditionally inactivating expression of TGF beta receptor type I (TGF beta RI), either by using mouse mammary tumor virus-Cre mice or by delivering adenoviral vector containing Cre to mouse salivary glands via retrograde infusion of the cannulated main excretory ducts of submandibular glands. Results. TGF beta RI-conditional knockout (TGF beta RI-coko) mice were born normal; however, female TGF beta RI-coko mice developed severe multifocal inflammation in salivary and mammary glands and in the heart. The inflammatory disorder affected normal growth and resulted in the death of the mice at ages 4-5 weeks. Interestingly, male TGF beta RI-coko mice did not exhibit any signs of inflammation. The female TGF beta RI-coko mice also showed an increase in Th1 proinflammatory cytokines in salivary glands and exhibited an up-regulation of peripheral T cells. In addition, these mice showed an atypical distribution of aquaporin 5 in their salivary glands, suggesting likely secretory impairment. Administration of an adenoviral vector encoding Cre recombinase into the salivary glands resulted in inflammatory foci only in the glands of female TGF beta RI-loxP-flanked (floxed) mice (TGF beta RI-f/f mice), but not in those of male and female wild-type mice or male TGF beta RI-f/f mice. Conclusion. These results suggest that female mice are uniquely more susceptible to developing inflammatory disorders due to impaired TGF beta signaling in their salivary glands.}},
  author       = {{Nandula, Seshagiri R. and Amarnath, Shoba and Molinolo, Alfredo and Bandyopadhyay, Bidhan C. and Hall, Bradford and Goldsmith, Corinne M. and Zheng, Changyu and Larsson, Jonas and Sreenath, Taduru and Chen, WanJun and Ambudkar, Indu S. and Karlsson, Stefan and Baum, Bruce J. and Kulkarni, Ashok B.}},
  issn         = {{1529-0131}},
  language     = {{eng}},
  number       = {{6}},
  pages        = {{1798--1805}},
  publisher    = {{John Wiley & Sons Inc.}},
  series       = {{Arthritis and Rheumatism}},
  title        = {{Female mice are more susceptible to developing inflammatory disorders due to impaired transforming growth factor beta signaling in salivary glands}},
  url          = {{http://dx.doi.org/10.1002/art.22715}},
  doi          = {{10.1002/art.22715}},
  volume       = {{56}},
  year         = {{2007}},
}

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Female mice are more susceptible to developing inflammatory disorders due to impaired transforming growth factor beta signaling in salivary glands