Gotowe bibliografie tematyczne / Les Mutations

Spis treści

  1. Artykuły w czasopismach
  2. Rozprawy doktorskie
  3. Książki
  4. Części książek
  5. Streszczenia konferencji
  6. Raporty organizacyjne

Gotowa bibliografia na temat „Les Mutations”

Autor: Grafiati
Data publikacji: 14 grudnia 2024
Data aktualizacji: 31 lipca 2025

Utwórz poprawne odniesienie w stylach APA, MLA, Chicago, Harvard i wielu innych

Wybierz rodzaj źródła:

Zobacz listy aktualnych artykułów, książek, rozpraw, streszczeń i innych źródeł naukowych na temat „Les Mutations”.

Przycisk „Dodaj do bibliografii” jest dostępny obok każdej pracy w bibliografii. Użyj go – a my automatycznie utworzymy odniesienie bibliograficzne do wybranej pracy w stylu cytowania, którego potrzebujesz: APA, MLA, Harvard, Chicago, Vancouver itp.

Możesz również pobrać pełny tekst publikacji naukowej w formacie „.pdf” i przeczytać adnotację do pracy online, jeśli odpowiednie parametry są dostępne w metadanych.

Artykuły w czasopismach na temat "Les Mutations"

1

Hyodo, Toshiki, Nobuyuki Kuribayashi, Chonji Fukumoto, et al. "Abstract 4649: Proposal of the concept of “p53 mutational spectrum”: Its clinical implication in oral squamous cell carcinoma." Cancer Research 85, no. 8_Supplement_1 (2025): 4649. https://doi.org/10.1158/1538-7445.am2025-4649.

Pełny tekst źródła
Streszczenie:
Abstract The p53 gene is the most frequently mutated gene in malignant tumors. We found that p53 abnormalities were observed in most cases of oral squamous cell carcinoma (OSCC). Therefore, it is necessary to search for type of the functional abnormality (complete loss of function, partial loss of function, or gain of oncogenic function) of the p53 gene rather than the presence or absence of gene mutation. Here we would like to propose the concept “p53 mutational spectrum”. In this study we performed whole-exome sequencing of p53 using clinical specimens from OSCC and attempted to clarify the
Style APA, Harvard, Vancouver, ISO itp.
2

Tarlock, Katherine, Todd M. Cooper, Todd A. Alonzo, et al. "Mutational Concordance from Diagnosis and Relapse in Pediatric Acute Myeloid Leukemia: A Report from the Children's Oncology Group." Blood 128, no. 22 (2016): 2846. http://dx.doi.org/10.1182/blood.v128.22.2846.2846.

Pełny tekst źródła
Streszczenie:
Abstract The range of genomic drivers of leukemogenesis and clonal nature of the disease illustrate the heterogeneity of the mutational spectrum in AML. Genomic interrogation of the evolution of AML has begun to highlight the scope of somatic changes that occur between diagnosis and relapse. A total of 1,214 patients were treated on the Children's Oncology Group trials AAML03P1 and AAML0531, of which 398 had relapse after initial remission. Of this cohort, 201 patients had matching diagnostic and relapse specimens for molecular profiling for the most common somatic mutations in pediatric AML (
Style APA, Harvard, Vancouver, ISO itp.
3

GARCÍA-DORADO, A., C. LÓPEZ-FANJUL, and A. CABALLERO. "Properties of spontaneous mutations affecting quantitative traits." Genetical Research 74, no. 3 (1999): 341–50. http://dx.doi.org/10.1017/s0016672399004206.

Pełny tekst źródła
Streszczenie:
Recent mutation accumulation results from invertebrate species suggest that mild deleterious mutation is far less frequent than previously thought, implying smaller expressed mutational loads. Although the rate (λ) and effect (s) of very slight deleterious mutation remain unknown, most mutational fitness decline would come from moderately deleterious mutation (s ≈ 0·2, λ ≈ 0·03), and this situation would not qualitatively change in harsh environments. Estimates of the average coefficient of dominance (h¯) of non-severe deleterious mutations are controversial. The typical value of h¯ = 0·4 can
Style APA, Harvard, Vancouver, ISO itp.
4

Watters, M. K., and D. R. Stadler. "Spontaneous mutation during the sexual cycle of Neurospora crassa." Genetics 139, no. 1 (1995): 137–45. http://dx.doi.org/10.1093/genetics/139.1.137.

Pełny tekst źródła
Streszczenie:
Abstract The DNA sequences of 42 spontaneous mutations of the mtr gene in Neurospora crassa have been determined. The mutants were selected among sexual spores to represent mutations arising in the sexual cycle. Three sexual-cycle-specific mutational classes are described: hotspot mutants, spontaneous repeat-induced point mutation (RIPs) and mutations occurring during a mutagenic phase of the sexual cycle. Together, these three sexual-cycle-specific mutational classes account for 50% of the mutations in the sexual-cycle mutational spectrum. One third of all mutations occurred at one of two mut
Style APA, Harvard, Vancouver, ISO itp.
5

Pawlik, Timothy M., Darrell R. Borger, Yuhree Kim, et al. "Genomic profiling of intrahepatic cholangiocarcinoma: Refining prognostic determinants and identifying therapeutic targets." Journal of Clinical Oncology 32, no. 3_suppl (2014): 210. http://dx.doi.org/10.1200/jco.2014.32.3_suppl.210.

Pełny tekst źródła
Streszczenie:
210 Background: The molecular alterations that drive tumorigenesis in intrahepatic cholangiocarcinoma (ICC) remain poorly defined. We sought to define the incidence and prognostic significance of mutations associated with ICC among patients undergoing surgical resection. Methods: 138 patients who underwent resection at 6 centers in the United States and Europe were included in the cohort. Mutational profiling was performed using nucleic acids that were extracted from resected ICC tumor specimens; mutations were identified using a multiplexed mutational profiling platform. The frequency of muta
Style APA, Harvard, Vancouver, ISO itp.
6

Kang, S., S. S. Seo, H. J. Chang, C. W. Yoo, S. Y. Park, and S. M. Dong. "Mutual exclusiveness between PIK3CA and KRAS mutations in endometrial carcinoma." International Journal of Gynecologic Cancer 18, no. 6 (2008): 1339–43. http://dx.doi.org/10.1111/j.1525-1438.2007.01172.x.

Pełny tekst źródła
Streszczenie:
In endometrial carcinomas (ECs), previous report suggested that PIK3CA mutations do not coexist with KRAS mutations, but the significant mutual exclusiveness has not been demonstrated. In this study, we examined the mutation frequency of PIK3CA in EC and its mutual exclusiveness with KRAS mutation. We performed mutational analysis of PIK3CA through a polymerase chain reaction single-strand conformation polymorphism assay in 44 cases of endometrial cancer and analyzed the correlation with loss of PTEN, KRAS mutation, and RASSF1A hypermethylation. Somatic mutations of PIK3CA were detected in 14
Style APA, Harvard, Vancouver, ISO itp.
7

Chao, Mwe, Kathrin Thomay, Gudrun Goehring, et al. "Mutational Spectrum of Fanconi Anemia Associated Myeloid Neoplasms." Klinische Pädiatrie 229, no. 06 (2017): 329–34. http://dx.doi.org/10.1055/s-0043-117046.

Pełny tekst źródła
Streszczenie:
AbstractIndividuals with Fanconi anemia (FA) have a high risk of developing myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML), yet the secondary somatic mutations lending to these malignancies remain to be further elucidated. We employed a next-generation sequencing myeloid neoplasia gene panel to determine the mutational spectrum of FA-related MDS/AML. Ten of 16 patients showed missense, nonsense, insertion or duplication mutations in 13 genes. In contrast to findings in MDS in the general population, mutations in genes involved in RNA splicing were rarely affected. Mutations in
Style APA, Harvard, Vancouver, ISO itp.
8

Ellis, Nathan A. "Mutation-causing mutations." Nature 381, no. 6578 (1996): 110–11. http://dx.doi.org/10.1038/381110a0.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
9

Pálinkás, Hajnalka Laura, Lőrinc Pongor, Máté Balajti, et al. "Primary Founder Mutations in the PRKDC Gene Increase Tumor Mutation Load in Colorectal Cancer." International Journal of Molecular Sciences 23, no. 2 (2022): 633. http://dx.doi.org/10.3390/ijms23020633.

Pełny tekst źródła
Streszczenie:
The clonal composition of a malignant tumor strongly depends on cellular dynamics influenced by the asynchronized loss of DNA repair mechanisms. Here, our aim was to identify founder mutations leading to subsequent boosts in mutation load. The overall mutation burden in 591 colorectal cancer tumors was analyzed, including the mutation status of DNA-repair genes. The number of mutations was first determined across all patients and the proportion of genes having mutation in each percentile was ranked. Early mutations in DNA repair genes preceding a mutational expansion were designated as founder
Style APA, Harvard, Vancouver, ISO itp.
10

Ahn, TaeJin, and Taesung Park. "Pathway-Driven Discovery of Rare Mutational Impact on Cancer." BioMed Research International 2014 (2014): 1–10. http://dx.doi.org/10.1155/2014/171892.

Pełny tekst źródła
Streszczenie:
Identifying driver mutation is important in understanding disease mechanism and future application of custom tailored therapeutic decision. Functional analysis of mutational impact usually focuses on the gene expression level of the mutated gene itself. However, complex regulatory network may cause differential gene expression among functional neighbors of the mutated gene. We suggest a new approach for discovering rare mutations that have real impact in the context of pathway; the philosophy of our method is iteratively combining rare mutations until no more mutations can be added under the c
Style APA, Harvard, Vancouver, ISO itp.
Więcej źródeł

Rozprawy doktorskie na temat "Les Mutations"

1

Komp, Lindgren Patricia. "Mutations and Mutation Rate in the Development of Fluoroquinolone Resistance." Doctoral thesis, Uppsala : Acta Universitatis Upsaliensis, 2007. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-8275.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
2

Ibrahim, Daniel Murad. "ChIP-seq reveals mutation-specific pathomechanisms of HOXD13 missense mutations." Doctoral thesis, Humboldt-Universität zu Berlin, Mathematisch-Naturwissenschaftliche Fakultät I, 2015. http://dx.doi.org/10.18452/17102.

Pełny tekst źródła
Streszczenie:
Mutationen von Transkriptionsfaktoren (TF) betreffen nicht nur die Funktion des TFs, sondern auch die Expression seiner Zielgene und liegen häufig angeborenen Entwicklungsdefekten zugrunde. Über 20 Mutationen in HOXD13, einem TF der die Entwicklung der Extremitäten kontrolliert, sind bisher als Ursache verschiedenartiger Extremitätenfehlbildungen entdeckt worden. Eine molekularbiologische Grundlage für die Vielgestaltigkeit der HOXD13-Mutationen ist jedoch unbekannt. Die bisherigen Methoden zur funktionellen Charakterisierung von TF-Mutationen ermöglichten eine lediglich eingeschränkte Inte
Style APA, Harvard, Vancouver, ISO itp.
3

Krasovec, Marc. "Estimation des taux de mutation : implications pour la diversification et l'évolution du phytoplancton eucaryote." Thesis, Paris 6, 2016. http://www.theses.fr/2016PA066371/document.

Pełny tekst źródła
Streszczenie:
Les mutations sont la principale source de diversité sur laquelle agit la sélection pour permettre aux espèces de s'adapter. Les études de l'effet des mutations sur la survie et du taux de mutation sont donc essentielles pour mieux comprendre l'évolution. Par une approche d'expérience d'accumulation de mutations, nous étudions ces deux questions chez cinq modèles d'algues vertes (Ostreococcus tauri, O. mediterraneus, Bathycoccus prasinos, Micromonas pusilla, et Picochlorum RCC4223). Il est mis en évidence une diminution de la fitness au cours du temps en raison des mutations délétères, et une
Style APA, Harvard, Vancouver, ISO itp.
4

Krasovec, Marc. "Estimation des taux de mutation : implications pour la diversification et l'évolution du phytoplancton eucaryote." Electronic Thesis or Diss., Paris 6, 2016. https://accesdistant.sorbonne-universite.fr/login?url=https://theses-intra.sorbonne-universite.fr/2016PA066371.pdf.

Pełny tekst źródła
Streszczenie:
Les mutations sont la principale source de diversité sur laquelle agit la sélection pour permettre aux espèces de s'adapter. Les études de l'effet des mutations sur la survie et du taux de mutation sont donc essentielles pour mieux comprendre l'évolution. Par une approche d'expérience d'accumulation de mutations, nous étudions ces deux questions chez cinq modèles d'algues vertes (Ostreococcus tauri, O. mediterraneus, Bathycoccus prasinos, Micromonas pusilla, et Picochlorum RCC4223). Il est mis en évidence une diminution de la fitness au cours du temps en raison des mutations délétères, et une
Style APA, Harvard, Vancouver, ISO itp.
5

Maxwell, Megan Amanda, and n/a. "PEX1 Mutations in Australasian Patients with Disorders of Peroxisome Biogenesis." Griffith University. School of Biomolecular and Biomedical Science, 2004. http://www4.gu.edu.au:8080/adt-root/public/adt-QGU20040219.100649.

Pełny tekst źródła
Streszczenie:
The peroxisome is a subcellular organelle that carries out a diverse range of metabolic functions, including the b-oxidation of very long chain fatty acids, the breakdown of peroxide and the a-oxidation of fatty acids. Disruption of peroxisome metabolic functions leads to severe disease in humans. These diseases can be broadly grouped into two categories: those in which a single enzyme is defective, and those known as the peroxisome biogenesis disorders (PBDs), which result from a generalised failure to import peroxisomal matrix proteins (and consequently result in disruption of multiple metab
Style APA, Harvard, Vancouver, ISO itp.
6

Maxwell, Megan Amanda. "PEX1 Mutations in Australasian Patients with Disorders of Peroxisome Biogenesis." Thesis, Griffith University, 2004. http://hdl.handle.net/10072/366184.

Pełny tekst źródła
Streszczenie:
The peroxisome is a subcellular organelle that carries out a diverse range of metabolic functions, including the b-oxidation of very long chain fatty acids, the breakdown of peroxide and the a-oxidation of fatty acids. Disruption of peroxisome metabolic functions leads to severe disease in humans. These diseases can be broadly grouped into two categories: those in which a single enzyme is defective, and those known as the peroxisome biogenesis disorders (PBDs), which result from a generalised failure to import peroxisomal matrix proteins (and consequently result in disruption of multiple metab
Style APA, Harvard, Vancouver, ISO itp.
7

COCCIADIFERRO, DARIO. "Mutational analysis of Kabuki Syndrome patients and functional dissection of KMT2D mutations." Doctoral thesis, Università di Foggia, 2018. http://hdl.handle.net/11369/369451.

Pełny tekst źródła
Streszczenie:
The discovery of histone methyltransferase KMT2D and demethylase KDM6A genetic alterations in Kabuki Syndrome (KS) expanded and highlighted the role of histone modifiers in causing congenital anomalies and intellectual disability syndromes. KS is a rare autosomal dominant condition characterized by facial features, various organ malformations, postnatal growth deficiency, and intellectual disability. Since 2011 we performed a mutational screening of our KS cohort, that includes now 505 KS patients, by Sanger sequencing and MLPA of KMT2D, followed by KDM6A analysis in those patients resulted as
Style APA, Harvard, Vancouver, ISO itp.
8

Davis, Brad. "Compensatory and deleterious mutations." Thesis, University of British Columbia, 2009. http://hdl.handle.net/2429/7722.

Pełny tekst źródła
Streszczenie:
My Ph.D. research has focused on some general properties of compensatory mutations, as well as the impact of compensatory mutations on fitness recovery and deleterious mutations on populations extinction risks. I have addressed these topics using a variety of techniques. Chapter 2 addresses mutational meltdown using computer simulation models to explicitly incorporate both environmental stochasticity and mutation accumulation. The results show that a small amount of environmental stochasticity can significantly hasten extinction times and that the mutational meltdown process hastens time to e
Style APA, Harvard, Vancouver, ISO itp.
9

Bendall, Kate E. "Inheritance of mitochondrial mutations." Thesis, University of Oxford, 1996. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.320141.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
10

Salamat, Majid. "Coalescent, recombinaisons et mutations." Thesis, Aix-Marseille 1, 2011. http://www.theses.fr/2011AIX10059.

Pełny tekst źródła
Streszczenie:
Cette thèse se concentre sur certains sujets en génétique des populations. Dans la première partie, nous donnons des formules y compris l'espérance et la variance de la hauteur et celles de la longueur du graphe de recombinaison ancestral (ARG) et l'espérance et la variance du nombre de recombinaison et nous montrons que l'espérance de la longueur de l'ARG est une combinaison linéaire de l'espérance de la longueur de la coalescence de Kingman et l'espérance de la hauteur de l'ARG. En outre, nous avons obtenu une relation entre l'espérance la longueur de l'ARG et l'espérance du nombre de recomb
Style APA, Harvard, Vancouver, ISO itp.
Więcej źródeł

Książki na temat "Les Mutations"

1

Thomas, Hugh. Mutations. BookThug, 2004.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
2

Centre d'études et de recherche sur les civilisations et les littératures européennes (Boulogne-sur-Mer, France) and Université du Littoral Côte d'Opale. Équipe de recherche "HLLI.", eds. Mutations de société, mutations de cinéma. Shaker Verlag, 2015.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
3

Aubin, Denis. Mutations/fluctuations. NBJ, 1985.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
4

Wedge, Martin. Per-mutations. Ormeau Baths Gallery, 1997.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
5

Francesco, Casetti, Odin Roger, and Centre d'études transdisciplinaires, eds. Télévisions mutations. Éditions du Seuil [for] Centre d'Études Transdisciplinaires, 1990.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
6

Carlos, Pacheco, Townsend Timothy, Hosek Dan, Harris Bob, and Atomic Media, eds. X-Men: Mutations. Marvel Comics, 1996.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
7

Jay, Prosser, ed. Sublime mutations: Photographs. Konkursbuch Verlag, 2000.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
8

international, Institut CEDIMES Colloque, ed. Mutations contemporaines & développement. CEDIMES, 2003.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
9

Castella, Vincenzo, Davis Lynn 1944-, and Roberto Pugliese. Recursions and mutations. Silvana editoriale, 2019.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
10

Couturier, Stéphane. Stéphane Couturier: Mutations. Bibliothèque nationale de France, 2004.

Znajdź pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
Więcej źródeł

Części książek na temat "Les Mutations"

1

Konzak, C. F. "Mutations and Mutation Breeding." In Agronomy Monographs. American Society of Agronomy, Crop Science Society of America, Soil Science Society of America, 2015. http://dx.doi.org/10.2134/agronmonogr13.2ed.c24.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
2

Sebald, Madeleine. "Mutations." In Brock/Springer Series in Contemporary Bioscience. Springer New York, 1993. http://dx.doi.org/10.1007/978-1-4615-7087-5_5.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
3

Sharma, Dhirendra Kumar. "Mutations." In Encyclopedia of Animal Cognition and Behavior. Springer International Publishing, 2022. http://dx.doi.org/10.1007/978-3-319-55065-7_567.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
4

Sharma, Dhirendra Kumar. "Mutations." In Encyclopedia of Animal Cognition and Behavior. Springer International Publishing, 2019. http://dx.doi.org/10.1007/978-3-319-47829-6_567-1.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
5

Biswas, Nabendu. "Mutations." In Practical GraphQL. Apress, 2023. http://dx.doi.org/10.1007/978-1-4842-9621-9_3.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
6

Abe, Tomoko, Hiroyuki Ichida, Yoriko Hayashi, et al. "Ion beam mutagenesis - an innovative and effective method for plant breeding and gene discovery." In Mutation breeding, genetic diversity and crop adaptation to climate change. CABI, 2021. http://dx.doi.org/10.1079/9781789249095.0042.

Pełny tekst źródła
Streszczenie:
Abstract We have developed a unique technology for mutation induction of plants using energetic ion beams at the RI Beam Factory (RIBF) of Rikagaku Kenkyūjo (RIKEN) (Institute of Physical and Chemical Research). Ion beams effectively induce mutations at relatively low doses without severely inhibiting growth. The irradiation treatment can be given to various plant materials and mutation can be induced in a short time, between seconds and a few minutes. The linear energy transfer (LET) of ions depends on the nuclide and velocity. Since LET value affects the mutation frequency, it is an importan
Style APA, Harvard, Vancouver, ISO itp.
7

van Eyk, Clare L., and Robert I. Richards. "Dynamic Mutations." In Advances in Experimental Medicine and Biology. Springer New York, 2012. http://dx.doi.org/10.1007/978-1-4614-5434-2_5.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
8

Michaelides, K., R. Schwaab, M. R. A. Lalloz, W. Schmidt,, and E. G. D. Tuddenham. "Mutational analysis: new mutations." In PCR2. Oxford University PressOxford, 1995. http://dx.doi.org/10.1093/oso/9780199634255.003.0013.

Pełny tekst źródła
Streszczenie:
Abstract In the last few years the search for mutations and sequence polymorphisms has been dramatically accelerated by the use of PCR and subsequently by direct sequencing of PCR products (1, 2). In spite of these powerful new methods, direct sequencing is not always practicable in detecting mutations because they may be positioned anywhere in some of the very large genes which are being studied. For example, mutations have now been found in nearly every one of the 26 exons of the factor VIII gene. Thus a number of prescreening methods have been developed, such as discriminant oligonucleotide
Style APA, Harvard, Vancouver, ISO itp.
9

Newton, Clive R. "Mutational analysis: known mutations." In PCR2. Oxford University PressOxford, 1995. http://dx.doi.org/10.1093/oso/9780199634255.003.0012.

Pełny tekst źródła
Streszczenie:
Abstract This chapter attempts to illustrate the various PCR options that are available to detect specific mutations and/or polymorphisms in genomic DNA. In so doing, the relative merits and drawbacks of each technique are addressed in the respective sections. For some methods of PCR-assisted mutation detection covered in this chapter, a protocol has not been included. In these instances the respective method is rarely used and is therefore discussed and the seminal reference cited. Protocols have, as far as possible, been described so that they can be applied in a generic fashion. However, de
Style APA, Harvard, Vancouver, ISO itp.
10

Levine, Michael A., and Steven A. Lietman. "Molecular and Clinical Characteristics of the McCune–Albright Syndrome." In Oxford Textbook of Endocrinology and Diabetes 3e, edited by John A. H. Wass, Wiebke Arlt, and Robert K. Semple. Oxford University Press, 2021. http://dx.doi.org/10.1093/med/9780198870197.003.0121.

Pełny tekst źródła
Streszczenie:
The McCune–Albright syndrome (MAS) is characterized by the clinical triad of polyostotic fibrous dysplasia, café-au-lait pigmented skin lesions, and endocrinopathy. MAS is due to postzygotic mutation of the GNAS gene that leads to activation of Gα‎<sub>s</sub>, the alpha chain of the heterotrimeric G protein, Gs. Cells that carry the activating GNAS mutation, termed gsp, are distributed in a mosaic pattern, and the extent of the distribution of mutation-bearing cells is based on the timing of the mutational event. Thus, gsp mutations that occur late in development can cause mono-ostotic fibrou
Style APA, Harvard, Vancouver, ISO itp.

Streszczenia konferencji na temat "Les Mutations"

1

Pekarcik, Peter, and Eva Chovancová. "Mutations of Cryptographic Algorithms." In 2024 International Conference on Emerging eLearning Technologies and Applications (ICETA). IEEE, 2024. https://doi.org/10.1109/iceta63795.2024.10850786.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
2

SEPE, MARICHELA. "MEASURING UNCERTAINTY: FACING PLACE MUTATIONS SUSTAINABLY." In SDP 2024. WIT Press, 2024. http://dx.doi.org/10.2495/sdp240131.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
3

Badamshin, E. A., A. V. Skudnov, K. Y. Popadin, K. V. Gunbin, and S. V. Denisov. "NUCLEOTIDE BIAS BETWEEN LEADING AND LAGGING STRAND IN BACTERIA IS CAUSED BY ASYMMETRIC MUTAGENESIS." In XI МЕЖДУНАРОДНАЯ КОНФЕРЕНЦИЯ МОЛОДЫХ УЧЕНЫХ: БИОИНФОРМАТИКОВ, БИОТЕХНОЛОГОВ, БИОФИЗИКОВ, ВИРУСОЛОГОВ, МОЛЕКУЛЯРНЫХ БИОЛОГОВ И СПЕЦИАЛИСТОВ ФУНДАМЕНТАЛЬНОЙ МЕДИЦИНЫ. IPC NSU, 2024. https://doi.org/10.25205/978-5-4437-1691-6-12.

Pełny tekst źródła
Streszczenie:
The Mutation Accumulation Experiment (MAE) is a commonly employed technique to obtain the most pure mutational spectrum. According to the parity rule 1 (hypothesis) frequencies of complementary mutations have to be equal. For this reason, the 6-component mutation spectrum (2 base pair types × 3 possible mutations) is commonly used in research which doesn’t differentiate between complementary mutations (e.g. C&gt;T and G&gt;A), some which accumulates on leading and lagging strands differently. In this work we present 12-component strand-specific mutation spectra which is able to show difference
Style APA, Harvard, Vancouver, ISO itp.
4

Souza, Beatriz, and Rohit Gheyi. "A Lightweight Technique to Identify Equivalent Mutants." In XI Congresso Brasileiro de Software: Teoria e Prática. Sociedade Brasileira de Computação - SBC, 2020. http://dx.doi.org/10.5753/cbsoft_estendido.2020.14630.

Pełny tekst źródła
Streszczenie:
Mutation analysis is a popular but costly approach to assess the quality of test suites. Equivalent mutants are useless and contribute to increase costs. We propose a lightweight technique to identify equivalent mutants by proving equivalences with Z3 in the context of weak mutation testing. To evaluate our approach, we apply our technique for 40 mutation targets (mutations of an expression or statement) and automatically identify 13 equivalent mutations for seven mutation targets. We manually confirm that the equivalent mutants detected by our technique are indeed equivalent. Moreover, we eva
Style APA, Harvard, Vancouver, ISO itp.
5

Cambraia, Amanda, Mario Campos Junior, Fernanda Gubert, et al. "A novel mutation in the RRM2 domain of TDP-43 in a Brazilian sporadic ALS patient." In XIII Congresso Paulista de Neurologia. Zeppelini Editorial e Comunicação, 2021. http://dx.doi.org/10.5327/1516-3180.486.

Pełny tekst źródła
Streszczenie:
Introduction: Amyotrophic Lateral Sclerosis (ALS) is an adult-onset progressive and fatal neurodegenerative disease that selectively affects upper and lower motor neurons. Death occurs within 3 to 5 years of onset, usually from respiratory complications. Most cases of ALS are sporadic (SALS), but familial forms of the disease (FALS) represent approximately 10% of the cases. More than 30 genes have been associated with ALS and mutations in these genes account for more than a half of all familial cases and about 10% of sporadic cases. One of the most prevalent genes is TARDBP, responsible for ap
Style APA, Harvard, Vancouver, ISO itp.
6

Iliushchenko, D. V., B. E. Efimenko, K. V. Gunbin, and K. Y. Popadin. "DEEP MUTATIONAL SPECTRUM OF MITOCHONDRIAL GENOME IN VERTEBRATES AS A NEW TYPE OF SPECIES — SPECIFIC MOLECULAR PHENOTYPE." In OpenBio-2023. ИПЦ НГУ, 2023. http://dx.doi.org/10.25205/978-5-4437-1526-1-4.

Pełny tekst źródła
Streszczenie:
The deep mutational spectrum (MS), an informative representation of de novo mutations with contextual data, offers valuable biological insights into the primary sources ofmutations across diverse genes, cancers, and species. However, reconstructing a comprehensive mutational spectrum demands substantial data, which is often lacking for non-model species. To address this challenge, we present a novel approach integrating sparse species-specific mitochondrial DNA (mtDNA) mutational spectra based on 122,031 polymorphic reconstructed synonymous mutations within the CytB gene of 974 vertebrate spec
Style APA, Harvard, Vancouver, ISO itp.
7

Zheleznova, A. S., M. Yu Kartashov, and S. A. Svirin. "THE PREVALENCE OF MUTANT FORMS OF HEPATITIS B VIRUS CIRCULATING IN SIBERIA." In XI МЕЖДУНАРОДНАЯ КОНФЕРЕНЦИЯ МОЛОДЫХ УЧЕНЫХ: БИОИНФОРМАТИКОВ, БИОТЕХНОЛОГОВ, БИОФИЗИКОВ, ВИРУСОЛОГОВ, МОЛЕКУЛЯРНЫХ БИОЛОГОВ И СПЕЦИАЛИСТОВ ФУНДАМЕНТАЛЬНОЙ МЕДИЦИНЫ. IPC NSU, 2024. https://doi.org/10.25205/978-5-4437-1691-6-184.

Pełny tekst źródła
Streszczenie:
55 full-genome HBV sequences were obtained, which were genotyped and analyzed for the presence of drug resistance and vaccine escape mutations. The following distribution of subgenotypes was revealed in the studied sample: D2 — 33.0 %, D3 — 31.0 %, D1 — 29.0 %, A2 — 7.0 %. Mutations of drug resistance were not found among the identified isolates. A vaccine-elusive mutation Y134H was found in a single isolate.
Style APA, Harvard, Vancouver, ISO itp.
8

Mukhopadhyay, Asima, Nicola Curtin, and Richard Edmondson. "Evaluation of different methods to assess homologous recombination status and sensitivity to PARP inhibitors in ovarian cancer." In 16th Annual International Conference RGCON. Thieme Medical and Scientific Publishers Private Ltd., 2016. http://dx.doi.org/10.1055/s-0039-1685289.

Pełny tekst źródła
Streszczenie:
Methods: Matched samples of ascites and tumor tissue were taken from patients undergoing surgery for epithelial ovarian cancer. Tumor samples were formalin fixed and paraffin embedded (FFPE); ascites samples were used to generate primary cultures (PC). HR status was determined in PCs as previously described.[1] IC50 for the PARP inhibitor Rucaparib was estimated using SRB assays. DNA was extracted from the FFPE tissue. The following techniques were evaluated in PCs or paired FFPE samples: DR-GFP reporter assay, PARP activity assay, BRCA1 expression on immunohistochemistry, BRCA1 methylation st
Style APA, Harvard, Vancouver, ISO itp.
9

Svirin, K. A., O. G. Polovkova, E. S. Fedorova, M. N. Kamalov, A. S. Zheleznova, and M. Yu Kartashov. "ANALYSIS OF RESISTANCE MUTATIONS IN HEPATITIS C VIRUS ISOLATES SUBGENOTYPES 1B AND 3A IN TUBERCULOSIS-INFECTED INDIVIDUALS IN THE TOMSK REGION." In XI МЕЖДУНАРОДНАЯ КОНФЕРЕНЦИЯ МОЛОДЫХ УЧЕНЫХ: БИОИНФОРМАТИКОВ, БИОТЕХНОЛОГОВ, БИОФИЗИКОВ, ВИРУСОЛОГОВ, МОЛЕКУЛЯРНЫХ БИОЛОГОВ И СПЕЦИАЛИСТОВ ФУНДАМЕНТАЛЬНОЙ МЕДИЦИНЫ. IPC NSU, 2024. https://doi.org/10.25205/978-5-4437-1691-6-200.

Pełny tekst źródła
Streszczenie:
Hepatitis C virus (HCV) has high mutational variability, which leads to the emergence of mutational forms that are resistant to direct-acting antivirals. Among 25 isolates of HCV subtype 3a found in tuberculosis patients in the Tomsk region, mutations Y93H and S/T62L were found in the NS5A gene, and A166S/T substitutions were detected in the NS3 gene. In nine isolates of subtype 1b, mutations L31M and P58S were detected in the NS5A gene; substitutions L159F, C316, and S556G were detected in the NS5B gene.
Style APA, Harvard, Vancouver, ISO itp.
10

Bittencourt, Yuri Cardoso Rodrigues Beckedorff, Lucas Soares Almada, Tatiana Strava Corrêa, et al. "SOMATIC MUTATIONAL LANDSCAPE CHARACTERIZATION OF METASTATIC BREAST CANCER IN BRAZIL." In Brazilian Breast Cancer Symposium 2022. Mastology, 2022. http://dx.doi.org/10.29289/259453942022v32s2025.

Pełny tekst źródła
Streszczenie:
Objective: Breast cancer (BC) is the most common malignancy among Brazilian women after non-melanoma skin cancer. The mutational landscape of BC in Brazil is unknown. This study describes the mutational profile of a cohort of patients with metastatic breast cancer (MBC) who had undergone next-generation sequencing (NGS) using a comprehensive somatic tumor panel. Methods: We retrospectively reviewed medical records from MBC patients. The mutational profile, clinical, and demographic characteristics were abstracted. Furthermore, the patterns of ordering the panel and its usefulness for a clinica
Style APA, Harvard, Vancouver, ISO itp.

Raporty organizacyjne na temat "Les Mutations"

1

Yang, Mengge, and Lin Liao. Mutations and clinical characteristics of dRTA caused by SLC4A1 mutations. INPLASY - International Platform of Registered Systematic Review and Meta-analysis Protocols, 2022. http://dx.doi.org/10.37766/inplasy2022.12.0031.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
2

Henry, Stephen Michael, Mark A. Smith, and John P. Eddy. Holistic Portfolio Optimization using Directed Mutations. Office of Scientific and Technical Information (OSTI), 2016. http://dx.doi.org/10.2172/1618206.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
3

Yeung, Anthony T. Detection of Mutations Using a Novel Endonuclease. Defense Technical Information Center, 1998. http://dx.doi.org/10.21236/adb238444.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
4

โขวิฑูรกิจ, วีรพันธุ์, วาณี เปล่งพาณิชย์, ปาล์ม ชาติยิ่งเจริญ та LeGoff, Wilfried. โครงการวิจัยการศึกษารหัสพันธุกรรมในคนไทยที่มีไขมันในเลือดชนิดเอชดีแอลสูงมาก โดยวิธีถอดรหัสและวิเคราะห์การเปลี่ยนแปลงหน้าที่. จุฬาลงกรณ์มหาวิทยาลัย, 2011. https://doi.org/10.58837/chula.res.2011.33.

Pełny tekst źródła
Streszczenie:
วัตถุประสงค์: ปัจจัยทางพันธุกรรมที่เกี่ยวข้องกับภาวะเอชดีแอลในเลือดสูงยังไม่เป็นที่เข้าใจแน่ชัด คณะผู้วิจัยทำการถอดรหัสพันธุกรรมยีน 3 ยีน คือ CETP, LIPC และ LIPG ซึ่งสร้างโปรตีน คอเลสเตอริล เอสเทอร์ ทรานสเฟอร์ โปรตีน, เฮบพาติค ไลเปส และ เอนทีเลียล ไลเปส ตามลำดับ ในคนไทยที่มีระดับเอชดีแอลในเลือดสูงมากเทียบกับประชากรกลุ่มควบคุมวิธีดำเนินการวิจัย คณะผู้วิจัยทำการถอดรหัสยีน CETP, LIPC และ LIPG ในส่วนของ exon และ exon-intron junctions เพื่อค้นหาการเปลี่ยนแปลงพันธุกรรมในคนไทย 64 คนที่มีระดับเอชดีแอล ≥ 2.59 มิลลิโมล/ลิตร (100 มิลลิกรัม/เดซิเมตร) และเปรียบเทียบกับผลในประชากรกลุ่มควบคุม 113 คนผลการวิจั
Style APA, Harvard, Vancouver, ISO itp.
5

Dr. Elizabeth Iorns, Dr Elizabeth Iorns. Can we prevent the transmission of BRCA mutations? Experiment, 2013. http://dx.doi.org/10.18258/0090.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
6

Lapedes, A. S., B. G. Giraud, L. C. Liu, and G. D. Stormo. Correlated mutations in protein sequences: Phylogenetic and structural effects. Office of Scientific and Technical Information (OSTI), 1998. http://dx.doi.org/10.2172/296863.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
7

Beernink, P., D. Barsky, and B. Pesavento. Mutations that Cause Human Disease: A Computational/Experimental Approach. Office of Scientific and Technical Information (OSTI), 2006. http://dx.doi.org/10.2172/898012.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
8

Grapes, Laura, Stephen Rudd, Rohan L. Fernando, Karine Megy, Dominique Rocha, and Max F. Rothschild. Searching for mutations in pigs using the human genome. Iowa State University, 2005. http://dx.doi.org/10.31274/ans_air-180814-1070.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
9

Barkan, A. Transposon-induced nuclear mutations that alter chloroplast gene expression. Office of Scientific and Technical Information (OSTI), 1992. http://dx.doi.org/10.2172/6686800.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
10

Nelson, Peter S. Global Characterization of Protein-Altering Mutations in Prostate Cancer. Defense Technical Information Center, 2012. http://dx.doi.org/10.21236/ada568599.

Pełny tekst źródła
Style APA, Harvard, Vancouver, ISO itp.
Możesz być także zainteresowany rozszerzonymi bibliografiami na temat „Les Mutations” dla poszczególnych typów źródeł:
Artykuły w czasopismach Rozprawy doktorskie Książki
Oferujemy zniżki na wszystkie plany premium dla autorów, których prace zostały uwzględnione w tematycznych zestawieniach literatury. Skontaktuj się z nami, aby uzyskać unikalny kod promocyjny!

Do bibliografii