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Featured researches published by Sania Kuzmac.


Experimental Hematology | 2014

Acute hematopoietic stress in mice is followed by enhanced osteoclast maturation in the bone marrow microenvironment

Sania Kuzmac; Danka Grčević; Alan Šućur; Sanja Ivčević; Vedran Katavić

Osteoclasts are components of hematopoietic stem cell (HSC) niches, but their role as contributors to the HSC homeostasis and release are still controversial. We aimed to investigate whether an acute blood loss of 10% of total blood content, along with the consequent intense hematopoiesis, would affect osteoclast differentiation and activity. Isolated peripheral blood, spleen, and bone marrow (BM) cells from bones of hind limbs were investigated for the presence of specific subpopulations of osteoclast precursors: B220(-)CD3(-)NK1.1(-)CD11b(-/low)CD115(+)CD117(+) cells in BM, and B220(-)CD3(-)NK1.1(-)Gr-1(-)CD11b(+)CD115(+) cells in peripheral blood and spleen as well as the receptor activator of nuclear factor κ-B(+) cycle-arrested quiescent osteoclast precursors. Expression of osteoclastogenesis-related genes CD115, receptor activator of nuclear factor κ-B, and cathepsin K, the potential of BM cells to form osteoclast-like cells in vitro, and osteoclast activity in vivo were also evaluated. We observed an increase in spleen cellularity and myelopoiesis during week 1 following blood loss, without any significant effects on BM cellularity or BM myeloid precursors, including cells with high osteoclastogenic potential. However, at 1 week postbleeding, hematopoiesis significantly promoted the expression of cathepsin K, interleukin-34, and bone morphogenetic protein-6. Quiescent osteoclast precursors increased significantly in spleen 2 days following bleeding, whereas osteoclast activity remained unchanged up to 2 weeks postbleeding. Osteoclast-dependent B-cell differentiation was affected at the pre-B stage of maturation in BM, whereas the Lin(-)Sca-1(+)c-kit(+) population expanded in BM and spleen after 2 days postbleeding. Our data demonstrate that an acute blood loss promotes differentiation and maturation of osteoclasts at 1 week but does not enhance osteoresorption at 2 weeks postbleeding. Our data also identify osteoclast differentiation as a consequent and important event in establishing HSC homeostasis following hematopoietic stress.


Acta stomatologica Croatica | 2017

Učestalost nalaza bakterijskog sadržaja u perzistentnim periapikalnim lezijama

Joško Grgurević; Ana Ivanišević Malčić; Arjana Tambić Andrašević; Goranka Prpić Mehičić; Sania Kuzmac; Silvana Jukić

Objectives To determine the percentage of persistant apical lesions positive for bacterial nucleic acids, to detect microorganisms difficult to cultivate in persistant apical lesions by PCR and relate them to endodontic failure, clinical symptoms and diabetes mellitus. Materials and methods The samples of persistent apical lesions were collected during apicoectomy. Bacterial ubiquitous primer 16S rRNA was used to detect 16S ribosomal RNA in 36 samples. A species–specific PCR was performed with primers targeted to the bacterial 16S rRNA genes of Prevotella Nigrescens, Pseudoramibacter alactolyticus, and Propionobacterium propionicum. Results Six samples (16.67%) were positive for bacterial ribosomal RNA. Pseudoramibacter alactolyticus was detected in three samples. Propionibacterium propionicum and Prevotella nigrescens were detected in one sample each. The prevalence of infection of such lesions with P. intermedia, P. propionicum and P. alactolyticus is low. Conslusion The study we conducted gave insufficient data about extraradicular infection and its connection with diabetes mellitus and clinical symptoms. Conclusions Apical lesions persisting after endodontic treatment could harbor microorganisms other than Actinomyces and Propionicum species.


Periodicum Biologorum | 2014

Interactions between bone and immune systems: A focus on the role of inflammation in bone resorption and fracture healing

Tomislav Kelava; Alan Šućur; Sania Kuzmac


European Calcified Tissue Society Congress 2014 | 2014

Increased expression of PTX3 in non-hematopoietic periosteal cells during fracture healing

Tomislav Kelava; Sanja Ivčević; Vedran Katavić; Nataša Kovačić; Hrvoje Cvija; Katerina Zrinski Petrović; Sania Kuzmac; Ivo Kalajzic; Barbara Bottazzi; Danka Grčević


Blood Cells Molecules and Diseases | 2014

Recurrent critical hemorrhage is not sufficient to alter bone remodeling in mice

Sania Kuzmac; Danka Grčević; Sanja Ivčević; Tomislav Kelava; Nataša Kovačević; Elvira Lazic Mosler; Vedran Katavić


PLOS ONE | 2013

Critical role for PTX3 in bone regeneration and fracture healing

Tomislav Kelava; Sanja Ivčević; Vedran Katavić; Nataša Kovačić; Hrvoje Cvija; Sania Kuzmac; Ivo Kalajzic; Barbara Bottazzi; Danka Grčević


2nd Meeting of Middle-European Societies for Immunology and Allergology: Book of Abstracts | 2013

The important role of Pentraxin 3 in bone formation and fracture healing

Tomislav Kelava; Sanja Ivčević; Vedran Katavić; Nataša Kovačić; Hrvoje Cvija; Sania Kuzmac; Ivo Kalajzic; Barbara Bottazzi; Danka Grčević


THE ANNUAL SYMPOSIUM OF THE CROATIAN PHYSIOLOGICAL SOCIETY WITH INTERNATIONAL PARTICIPATION. | 2012

Pentraxin 3 has role in physiological bone formation

Tomislav Kelava; Hrvoje Cvija; Sanja Ivčević; Nataša Kovačić; Sania Kuzmac; Barbara Bottazzi; Danka Grčević


Arthritis Research & Therapy | 2012

Fas deficiency attenuates bone loss during antigen induced arthritis in mice

Elvira Lazic Mosler; Sania Kuzmac; Sanja Ivčević; Danka Grčević; Ana Marušić; Nataša Kovačić


Bone | 2009

Osteoclastogenic potential of bone marrow- and peripheral-hematopoietic cells in collagen induced arthritis

M. Ikic; Elvira Lazić; Sania Kuzmac; H. Cvija; Ana Marušić; Danka Grčević

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Barbara Bottazzi

Mario Negri Institute for Pharmacological Research

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Ivo Kalajzic

University of Connecticut Health Center

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