Title
Ekspresija hemokinske osovine CXCL12/CXCR4/CXCR7, markera hipoksije i angiogeneze u karcinomima bubrežnog parenhima
Creator
Floranović, Milena Potić-,
CONOR:
8095847
Copyright date
2021
Object Links
Select license
Autorstvo-Nekomercijalno-Bez prerade 3.0 Srbija (CC BY-NC-ND 3.0)
License description
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Language
Serbian
Cobiss-ID
Theses Type
Doktorska disertacija
description
Datum odbrane:
Other responsibilities
predsednik komisije
Jovičić Milentijević, Maja
član komisije
Radojević Škodrić, Sanja
Academic Expertise
Medicinske nauke
University
Univerzitet u Nišu
Faculty
Medicinski fakultet
Group
Katedra za patologiju
Alternative title
Expression of the CXCL12/CXCR4/CXCR7, markers of hypoxia and angiogenesis in renal cell carcinomas
: doctoral dissertation
Publisher
[M. S. Potić Floranović]
Format
114 listova
description
Biografija autora: list 113,
Bibliografija: listovi 96-112.
description
Pathology
Abstract (en)
Renal cell carcinoma (RCC) is the most common kidney cancer.
Even though it represents 5% of all cancer diagnosis, it is considered
one of the most lethal urologic malignancies. The most common
subtype is clear cell RCC and the second in frequency is papillary RCC.
At diagnosis 23% of patients already have metastatic disease and 25%
will develop metastases within five years from nephrectomy. Up to date,
all the factors that affect the development and prognosis of these tumors
are still not fully clarified. Over the last decade, various biomarkers
have been studied in order to elucidate the behavior of RCC but no
consensus has been achieved.
In this study we immunohistochemically examined the
expression of chemokine CXCL12 and its receptors CXCR4 and
CXCR7 on 98 paraffin embedded RCC samples obtained after radical
nephrectomy. We have also studied the expression of Hypoxia inducible
factor 1α, which regulates cell survival in hypoxic conditions, and
Notch1 receptor, which is the component of the conservative Notch
signaling pathway. The localization, percentage and the intensity of the
expression of these biomarkers were studied with the application of
histoscore. We analyzed their co-expression and their association with
clinical and pathological parameters and survival of the patients.
Positive membranous and cytoplasmatic CXCL12 and CXCR7
expression was present in over 90% of the samples, while about 60%
expressed positive CXCR4 staining.We found association between
tumor size and higher cytoplasmatic CXCL12 and CXCR7 expression.
Over 70% of the samples were HIF1α positive, and higher values of
cytoplasmatic HIF1α histoscore were associated with higher tumor
grade. We also found the association between necrosis and
cytoplasmatic CXCR7, HIF1α and Notch1 histoscore.
Compared to ccRCC in pRCC significantly higher values of
membranous CXCL12 as well as cytoplasmatic CXCL12, CXCR4,
CXCR7 and HIF1α histoscore can be expected. CCRCC has 4 times
higher probability of positive membranous CXCR4 expression and 20 times higher probability of positive membranous Notch1 eexpression.
H higher membranous Notch1 histoscore is expected in cccRCC as well.
Strong positive correlation was found between cyoplasmatic
HIF1α histoscore and cytoplasmatic CXCL12 and CXCR7 histoscores,
suggesting their co expression and potential interaction.
Shorter survival can be predicted by higher clinical stage, the
value of CXCL12 cytoplasmatic histoscore above 73 and by higher
values of membranous CXCR7 histoscore.
Examining the roles of these biomarkers in RCC could in the
future bring useful implications in diagnosis, prognosis, prevention of
the recidives and the development of target therapy in the most lethal
urologic malignancy.
Authors Key words
Renal cell carcinoma, CXCL12/CXCR4/CXCR7 chemokine axis,
Hipoxia inducible factor 1α, Notch1 receptor, Immunohistochemistry,
survival
Authors Key words
Karcinom bubrežnih ćelija, hipoksija inducibilni faktor 1α, hemokinska
osovina CXCL12/CXCR4/CXCR7, receptor Notch 1, imunohistohemija,
preživljavanje
Classification
616.61-006.6-076(043.3)
Subject
B520 General pathology, pathological anatomy
B 200 Citology, oncology, cancerology
Type
Tekst
Abstract (en)
Renal cell carcinoma (RCC) is the most common kidney cancer.
Even though it represents 5% of all cancer diagnosis, it is considered
one of the most lethal urologic malignancies. The most common
subtype is clear cell RCC and the second in frequency is papillary RCC.
At diagnosis 23% of patients already have metastatic disease and 25%
will develop metastases within five years from nephrectomy. Up to date,
all the factors that affect the development and prognosis of these tumors
are still not fully clarified. Over the last decade, various biomarkers
have been studied in order to elucidate the behavior of RCC but no
consensus has been achieved.
In this study we immunohistochemically examined the
expression of chemokine CXCL12 and its receptors CXCR4 and
CXCR7 on 98 paraffin embedded RCC samples obtained after radical
nephrectomy. We have also studied the expression of Hypoxia inducible
factor 1α, which regulates cell survival in hypoxic conditions, and
Notch1 receptor, which is the component of the conservative Notch
signaling pathway. The localization, percentage and the intensity of the
expression of these biomarkers were studied with the application of
histoscore. We analyzed their co-expression and their association with
clinical and pathological parameters and survival of the patients.
Positive membranous and cytoplasmatic CXCL12 and CXCR7
expression was present in over 90% of the samples, while about 60%
expressed positive CXCR4 staining.We found association between
tumor size and higher cytoplasmatic CXCL12 and CXCR7 expression.
Over 70% of the samples were HIF1α positive, and higher values of
cytoplasmatic HIF1α histoscore were associated with higher tumor
grade. We also found the association between necrosis and
cytoplasmatic CXCR7, HIF1α and Notch1 histoscore.
Compared to ccRCC in pRCC significantly higher values of
membranous CXCL12 as well as cytoplasmatic CXCL12, CXCR4,
CXCR7 and HIF1α histoscore can be expected. CCRCC has 4 times
higher probability of positive membranous CXCR4 expression and 20 times higher probability of positive membranous Notch1 eexpression.
H higher membranous Notch1 histoscore is expected in cccRCC as well.
Strong positive correlation was found between cyoplasmatic
HIF1α histoscore and cytoplasmatic CXCL12 and CXCR7 histoscores,
suggesting their co expression and potential interaction.
Shorter survival can be predicted by higher clinical stage, the
value of CXCL12 cytoplasmatic histoscore above 73 and by higher
values of membranous CXCR7 histoscore.
Examining the roles of these biomarkers in RCC could in the
future bring useful implications in diagnosis, prognosis, prevention of
the recidives and the development of target therapy in the most lethal
urologic malignancy.
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