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19 Sentences With "synergizes"

How to use synergizes in a sentence? Find typical usage patterns (collocations)/phrases/context for "synergizes" and check conjugation/comparative form for "synergizes". Mastering all the usages of "synergizes" from sentence examples published by news publications.

Much of its visual charm comes from the monochromatic minimalism of its exterior, which synergizes very well with the brilliant OLED display's perfect blacks.
I find all the small design touches in this new software coalesce into a unified user experience that lives up to the high standards of, and synergizes with, Samsung's great hardware.
There are two plug-in Friends at launch: a Hi-Fi Plus module for better headphone audio and a Cam Plus camera grip that synergizes with the G53's dual-camera system.
It doesn't matter how many people in the world use Android, the slickest and best applications are still happening on iOS first, which synergizes nicely with the company's present lead in having the slickest user interface.
There's also a new active suspension system that synergizes nicely with the various self-driving sensors — such as the front camera, which helps the system predict and preemptively adapt to bumps in the road — to ensure a smoother and safer ride.
So the president spent much of Saturday quote-tweeting Goldman, an ad executive whose line of defense—that the Russians were more interested in seeding chaos than electing Trump, a statement seemingly designed to minimize Facebook's responsibility for our current national situation—synergizes nicely with Trump's now-familiar habit of latching on to anything with the faintest possibility of exonerating him.
The use of flunitrazepam in combination with alcoholic beverages synergizes the adverse effects, and can lead to toxicity and death.
SUCNR1 is highly expressed on immature dendritic cells, where succinate binding stimulates chemotaxis. Furthermore, SUCNR1 synergizes with toll-like receptors to increase the production of proinflammatory cytokines such as TNF alpha and interleukin-1beta. Succinate may enhance adaptive immunity by triggering the activity of antigen-presenting cells that, in turn, activate T-cells.
It is produced by monocytes, macrophages, osteoblasts, keratinocytes. It is synthesized as an inactive precursor that is proteolytically cleaved to the active 18 kDa form. IL-18 stimulates IFN-γ production by T cells and NK cells. It acts either independently or synergizes with IL-12, which may lead to rapid activation of the monocyte / macrophage system.
A group of carbohydrate derivatives present in dehydrated tomato products interact with lycopene against prostate cancer. FruHis strongly synergizes with lycopene against the proliferation of highly metastatic rat prostate cancer cell lines in vitro. The FruHis/lycopene combination significantly inhibits in vivo tumorigenesis in syngeneic rats. The ketosamine completely blocks DNA oxidative degradation at >250 μmol/L in vitro, whereas neither ascorbate nor phenolic antioxidants from tomato are effective protectors.
R-spondin 2 also known as roof plate-specific spondin-2 is a protein that in humans that is encoded by the RSPO2 gene. R-spondin 2 synergizes with Wnt to activate beta-catenin. RSPO2 has been proposed to regulate craniofacial patterning and morphogenesis within pharyngeal arch 1 through ectoderm- mesenchyme signaling via the endothelin-Dlx5/6 pathway. In dogs, a variant on the Rspo2 gene is associated moustache and eyebrow thickness.
Proguanil acts as a mitochondrial sensitiser and synergizes with atovaquone. When atovaquone is used as a sole agent, a high natural frequency of cytochrome b mutants leads to a high failure rate. This is potentially due to the high lipophilicity and slow uptake of atovaquone, which results in a relatively prolonged period of parasite exposure at ineffective concentrations. Specific mutations (Y268S, Y268C) have been shown to confer resistance in vivo, but the other mechanisms of resistance remain unknown.
S1PR1 is one of the main receptors responsible for vascular growth and development, at least during embryogenesis. In vascular endothelial cells the binding of S1P to S1PR1 induces migration, proliferation, cell survival and morphogenesis into capillary-like structures. Moreover, the binding of S1P to S1PR1 is implicated in the formation of cell-cell adherens junctions, therefore inhibiting paracellular permeability of solutes and macromolecules. It was also shown in vivo that S1P synergizes with angiogenic factors such as FGF-2 and VEGF in inducing angiogenesis and vascular maturation through S1PR1.
Economic corridor development (ECD) is an approach that integrates and synergizes industry, infrastructure, logistics, and urbanization through industrial production clusters linked to urban centers and international gateways by an efficient multimodal transport network. A successful ECD strategy requires quality infrastructure and a policy framework that contributes to an efficient industrial base, attracts investment in the manufacturing sector, and facilitates production for domestic and export markets. Urban centers within a corridor are not only major markets for manufactured and imported goods, but also sources of labor, technology, knowledge, and innovation. GoI is currently building a host of industrial corridors across the country.
Due to the essential role of NADPH in lipid and DNA biosynthesis and the hyperproliferative nature of most cancers, NADK is an attractive target for cancer therapy. Furthermore, NADPH is required for the antioxidant activities of thioredoxin reductase and glutaredoxin. Thionicotinamide and other nicotinamide analogs are potential inhibitors of NADK, and studies show that treatment of colon cancer cells with thionicotinamide suppresses the cytosolic NADPH pool to increase oxidative stress and synergizes with chemotherapy. While the role of NADK in increasing the NADPH pool appears to offer protection against apoptosis, there are also cases where NADK activity appears to potentiate cell death.
It is therefore not surprising that it has broad spectrum antitumor activity and synergizes with antitumor drugs that target DNA. It is a very strong iron chelator and in the body it is likely that the iron chelate is the active species that quenches the active site tyrosyl radical required by ribonucleotide reductase for its enzymatic activity. The 3AP iron chelate is redox active and there have been several reports in the literature ascribing this property to some of the biological activities of 3AP. 3AP is a product of the laboratory of Dr Alan C. Sartorelli, a renowned cancer researcher in the Yale University School of Medicine Pharmacology Department.
Mutations affecting the coding region of this gene or the splicing of the transcript have been associated with Börjeson- Forssman-Lehmann syndrome (BFLS), a disorder characterized by mental retardation, epilepsy, hypogonadism, hypometabolism, obesity, swelling of subcutaneous tissue of the face, narrow palpebral fissures, and large ears. Alternate transcriptional splice variants, encoding different isoforms, have been characterized. The PHF6 gene in humans is also frequently mutated in human hematological malignancies, including T-cell acute lymphoblastic Leukemia (T-ALL) and Acute Myeloid Leukemia (AML) and at least two BFLS patients have developed leukemia or lymphoma. PHF6 has been shown to be important for the regulation of blood stem and progenitor cells and loss of PHF6 protein synergizes with over-expression of the TLX3 protein to cause lymphoid neoplasms.
Rothenfusser S, Hornung V, Krug A, Towarowski A, Krieg AM, Endres S, Hartmann G. Distinct CpG oligonucleotide sequences activate human γδ T cells via interferon-alpha/beta. Eur J Immunol 2001; 31: 3525-3534Hornung V, Rothenfusser S, Britsch S, Krug A, Jahrsdoerfer B, Giese T, Endres S, Hartmann G. Quantitative expression of TLR1-10 mRNA in cellular subsets of human PBMC and sensitivity to CpG ODN. J Immunol 2002; 168: 4531-37Krug A, Towarowski A, Britsch S, Rothenfusser S, Hornung V, Bals R, Giese T, Engelmann H, Endres S, Krieg AM, Hartmann G. Toll-like receptor expression reveals CpG DNA as a unique microbial stimulus for plasmacytoid dendritic cells which synergizes with CD40L to induce high amounts of IL-12. Eur J Immunol 2001, 31: 3026-37Krug A, Rothenfusser S, Hornung V, Jahrsdörfer B, Ballas Z, Endres S, Krieg AM, Hartmann G. Identification of CpG oligonucleotide sequences with high induction of IFN-a/-b in plasmacytoid dendritic cells. Eur J Immunol 2001; 31: 2154-63 First in Munich and then in Bonn, his group went on to study RNA recognition by TLR7, specifically the TLR7-mediated detection of short interfering RNAs (siRNA).
S100A4, a member of the S100 calcium-binding protein family secreted by tumor and stromal cells, supports tumorigenesis by stimulating angiogenesis. Research demonstrated that S100A4 synergizes with vascular endothelial growth factor (VEGF), via the RAGE receptor, in promoting endothelial cell migration by increasing KDR expression and MMP-9 activity. In vivo overexpression of S100A4 led to a significant increase in tumor growth and vascularization in a human melanoma xenograft M21 model. Conversely, when silencing S100A4 by shRNA technology, a dramatic decrease in tumor development of the pancreatic MIA PaCa-2 cell line was observed. Based on these results 5C3 was developed, a neutralizing monoclonal antibody against S100A4. This antibody abolished endothelial cell migration, tumor growth and angiogenesis in immunodeficient mouse xenograft models of MiaPACA-2 and M21-S100A4 cells. It is concluded that extracellular S100A4 inhibition is an attractive approach for the treatment of human cancer. S100A4 is highly associated with components of the cytoskeleton and when this gene is upregulated, it changes the cell’s morphology, making it more susceptible to invasion from proteins, such as cathepsin B and cyclin B1, that contribute to metastasis.

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