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  4. Adamts18 Function in Mammary Gland Development
 
doctoral thesis

Adamts18 Function in Mammary Gland Development

Ataca, Dalya  
2019

Ovarian hormones control mammary gland development and impinge on breast carcinogenesis acting via their cognate receptors in the luminal epithelium. The extracellular matrix has a key role in physiology and disease but how the two are linked is poorly understood. Here we show that deletion of the secreted protease Adamts18 delays mammary gland development. The proteaseâ s role is mammary epithelial intrinsic and required for stem cell function and epithelial regeneration potential. Progesterone controls Adamts18 in the myoepithelium through upregulation of Wnt-4 expression with ensuing canonical Wnt signaling activation in basal cells. IP-Mass Spec shows that ADAMTS18 has binding partners located in the ECM and basement membrane. Consistent with Adamts18 being an important regulator of ECM function, deletion results in increased Collagen I and IV, Laminin, and Fibronectin deposition and synergizes genetically with the basal membrane proteoglycan Collagen18a1 in controlling mammary stem cell function. In vitro, Collagen18a1 and Fibronectin are cleaved by Adamts18. RNAseq analysis reveals that the stem cell regulatory hippo pathway is downstream of Adamts18 with consequent reduction of Fgfr2 expression. Our findings link hormonal signaling in luminal mammary epithelial cells to ECM remodeling via Adamts18, and demonstrate the importance of the ECM for stem cell function in the mammary gland.

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Type
doctoral thesis
DOI
10.5075/epfl-thesis-9165
Author(s)
Ataca, Dalya  
Advisors
Brisken, Cathrin  
Jury

Prof. Joachim Lingner (président) ; professeure Cathrin Brisken (directeur de thèse) ; Prof. Daniel Constam, Prof. Pascal Schneider, Dr Veronique Maguer Satta (rapporteurs)

Date Issued

2019

Publisher

EPFL

Publisher place

Lausanne

Public defense year

2019-02-01

Thesis number

9165

Total of pages

126

Subjects

Mammary gland development

•

Adamts18

•

Stem Cell

•

Extracellular Matrix

•

Progesterone Receptor signaling

•

Matrix Metalloproteinases

•

Hormones

•

Canonical Wnt signaling

EPFL units
UPBRI  
Faculty
SV  
School
ISREC  
Doctoral School
EDMS  
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/154215
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