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3. Evaluation of Wear Behaviour Based on Mechanical Properties and Particle Size in LM26 MMC

Author

Konda Lakshmi Chaitanya and Srinivas K.

Subjects
mmc, al-alloys, garnet particles, stir casting, mechanical properties, Engineering (General). Civil engineering (General), TA1-2040
Abstract

Based on its superior casting and mechanical properties, LM26 is a well-known material in the automobile sector for the manufacturing of pistons for both diesel and gasoline engines. However, cast alloys diminishing the strength at higher temperatures leads to metal matrix composites. The present work deals with fabrication and characterisation of aluminium cast alloy LM26 reinforced with ceramic particles of Almandine Garnet with varying percentages fabricated by dual step stir casting technique The micro hardness and ultimate tensile strength (UTS) were determined and the sliding wear behaviour was estimated using a pin-on-disc apparatus. The effect of particle size and weight fraction of reinforcement on physical and mechanical properties were investigated and collated with unreinforced metal. Wear behaviour of the composite had a reasonably good correlation with composite mechanical properties were also observed. Validation of Experimental results with theoretical values were also discussed.

Published
2022
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7. Prevalence of self-medication in rural area of Andhra Pradesh

Author

Gaurav M Rangari, Roza G Bhaisare, Venkatasandhya Korukonda, Y Lakshmi Chaitanya, and N Hanumanth

Subjects
andhra pradesh, drugs, over the counter, rural, self-medication, Medicine
Abstract

Background: The consumption of medicine without consulting a doctor is called self-medication. In the recent decade, the prevalence of self-medication was increased mainly in the developing countries. The reason varies from the nonavailability of doctors to economical reason. But people are not aware of the side effects and interactions of drugs. This is risky behavior and may lead to death. The objective of this study is to find out the prevalence and various reasons, sources, and common drugs used for self-medication. Materials and Methods: A cross-sectional community-based study conducted in Visakhapatnam district, Andhra Pradesh. 166 houses were selected by using a simple random sampling method. One respondent from one household was interviewed by using a semi-structured questionnaire. The data obtained were analyzed by using SPSS V22. Chi-square and Fisher exact tests were applied to find associations. Phi, Cramer Rao V, and contingency coefficient were applied to find the strength of association. A value of P < 0.05 was considered significant. Results: Among 166 subjects, the majority (58.4%) of participants were in the age group between 18-30 and most of them were female 142 (85.5%). The prevalence of self-medication was 68.1%. The main source of self-medication was directly from the pharmacy, that is, pharmacists (72.6%). Analgesics were commonly (85%) self-medicated drug. The main indication for self-medication was headache (78.8%) and fever (66.4%). Conclusion: The prevalence of self-medication was high and which is hazardous to health. This needs prompt legislative action.

Published
2020
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8. Effectiveness of seminar as an educational tool among the undergraduate medical students: A study

Author

A Bhagyalakshmi, D Sridevi, Amrut Arvindrao Dambal, K Ravibabu, and G Lakshmi Chaitanya

Subjects
seminar, teaching learning(t/l) method, undergraduate medical curriculum, active learning, anc, weight gain, awareness, Medicine
Abstract

Background: The faculty of medical colleges have a greater responsibility in making the study methods of their subject innovative, interesting and participatory for the under graduate students. One such method is organizing seminars for the undergraduate students. Objective: To assess effectiveness of student seminars as a teaching learning method in the undergraduate medical curriculum. Methods: This study was conducted in the Department of Biochemistry, Malla Reddy Institute of Medical Sciences, Hyderabad on a group of 150 students. This study assesses the role of seminar as teaching-learning tool by recording the effectiveness and perception of medical students on seminars through a pre-test/post-test evaluation and questionnaire-based survey. Results: A highly significant improvement (p

Published
2020
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11. Evaluation of Wear Behaviour Based on Mechanical Properties and Particle Size in LM26 MMC

Author

Lakshmi Chaitanya Konda and K. Srinivas

Subjects
Mechanical Engineering
Abstract

Based on its superior casting and mechanical properties, LM26 is a well-known material in the automobile sector for the manufacturing of pistons for both diesel and gasoline engines. However, cast alloys diminishing the strength at higher temperatures leads to metal matrix composites. The present work deals with fabrication and characterisation of aluminium cast alloy LM26 reinforced with ceramic particles of Almandine Garnet with varying percentages fabricated by dual step stir casting technique The micro hardness and ultimate tensile strength (UTS) were determined and the sliding wear behaviour was estimated using a pin-on-disc apparatus. The effect of particle size and weight fraction of reinforcement on physical and mechanical properties were investigated and collated with unreinforced metal. Wear behaviour of the composite had a reasonably good correlation with composite mechanical properties were also observed. Validation of Experimental results with theoretical values were also discussed.

Published
2022
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13. An Empirical Analysis of the Capabilities for Digital Transformation Resilience in Selected Countries

Author

Datti, Lakshmi Chaitanya, Kuppusamy, Mudiarasan, Datti, Lakshmi Chaitanya, and Kuppusamy, Mudiarasan

Abstract

Purpose: The study examined the enabling capabilities of digital transformation resilience across 61 countries from 2013 to 2022. Theoretical framework: This study draws on four theoretical perspectives: resilience theory, dynamic capabilities view, knowledge-based view theory, and diffusion of innovation theory. These theoretical lenses focus on how organizations can succeed in a changing environment. Design/Methodology/Approach: This study used secondary data from the International Institute for Management Developments (IMD), the World Digital Competitiveness Ranking, and the World Intellectual Property Organization (WIPO) Global Innovation Index (GII). The data set analyzed included information from 61 countries between 2013 to 2022. Panel data regression was used to conduct the analysis. Findings: The findings indicate that only knowledge capability has a significant relationship with digital transformation resilience technology, and future readiness was considered a non-significant enabler. Research, practical & social implications: In the digital age, governments and industries must prioritize resilience by implementing policies, developing necessary skills, providing training activities, and investing in research and development. Originality/Value: The originality of this study lies in its investigation of resilience capabilities with the new theoretical lens. Organizations must develop resilience capabilities, particularly in the realm of digital transformation. Digital transformation resilience pertains to an organization's capacity to adjust and react to changes in the dynamic environment using digital technologies.

Published
2023

17. Soft computing based audio signal analysis for accident prediction

Author

Lakshmi Chaitanya Duggineni, Swaraja Kuraparthi, Swetha Namburu, B. Anil Kumar, and Hima Bindu Valiveti

Subjects
Soft computing, 0209 industrial biotechnology, 020901 industrial engineering & automation, Audio signal, General Computer Science, Computer science, Real-time computing, 0202 electrical engineering, electronic engineering, information engineering, 020206 networking & telecommunications, 02 engineering and technology, Accident (philosophy), Theoretical Computer Science
Abstract

Purpose Road accidents, an inadvertent mishap can be detected automatically and alerts sent instantly with the collaboration of image processing techniques and on-road video surveillance systems. However, to rely exclusively on visual information especially under adverse conditions like night times, dark areas and unfavourable weather conditions such as snowfall, rain, and fog which result in faint visibility lead to incertitude. The main goal of the proposed work is certainty of accident occurrence. Design/methodology/approach The authors of this work propose a method for detecting road accidents by analyzing audio signals to identify hazardous situations such as tire skidding and car crashes. The motive of this project is to build a simple and complete audio event detection system using signal feature extraction methods to improve its detection accuracy. The experimental analysis is carried out on a publicly available real time data-set consisting of audio samples like car crashes and tire skidding. The Temporal features of the recorded audio signal like Energy Volume Zero Crossing Rate 28ZCR2529 and the Spectral features like Spectral Centroid Spectral Spread Spectral Roll of factor Spectral Flux the Psychoacoustic features Energy Sub Bands ratio and Gammatonegram are computed. The extracted features are pre-processed and trained and tested using Support Vector Machine (SVM) and K-nearest neighborhood (KNN) classification algorithms for exact prediction of the accident occurrence for various SNR ranges. The combination of Gammatonegram with Temporal and Spectral features of the validates to be superior compared to the existing detection techniques. Findings Temporal, Spectral, Psychoacoustic features, gammetonegram of the recorded audio signal are extracted. A High level vector is generated based on centroid and the extracted features are classified with the help of machine learning algorithms like SVM, KNN and DT. The audio samples collected have varied SNR ranges and the accuracy of the classification algorithms is thoroughly tested. Practical implications Denoising of the audio samples for perfect feature extraction was a tedious chore. Originality/value The existing literature cites extraction of Temporal and Spectral features and then the application of classification algorithms. For perfect classification, the authors have chosen to construct a high level vector from all the four extracted Temporal, Spectral, Psycho acoustic and Gammetonegram features. The classification algorithms are employed on samples collected at varied SNR ranges.

Published
2021
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19. Role of serum magnesium in diabetes mellitus - A case control study

Author

G. Lakshmi Chaitanya, Harika Kolli, M. Girija Menon, Amrut Arvindrao Dambal, and D. Sridevi

Subjects
Plasma glucose, chemistry, Magnesium, Diabetes mellitus, Statistical significance, medicine, Case-control study, Physiology, chemistry.chemical_element, medicine.disease, Medical science, Homeostasis, Glycemic
Abstract

Introduction: Diabetes mellitus characterized by high glycemic levels is routinely associated with many mineral abnormalities. The purpose of this study was to evaluate the levels of serum magnesium among subjects with diabetes mellitus and to compare and analyze the same in normal non diabetics. Materials and Methods: In this case control study conducted at Malla Reddy Hospital, 50 subjects known to be diabetics were considered as cases and 50 apparently normal non- diabetics were the controls. Serum magnesium was estimated, compared and analyzed. Results: Serum magnesium levels were 1.89 ± 0.32 among cases and 2.26 ± 0.27 among controls. Extreme statistical significance was observed between both the groups. Conclusion: Serum magnesium levels were found to be decreased in subjects with diabetes mellitus. We conclude that diabetes mellitus could influence magnesium homeostasis. Keywords: Diabetes mellitus, Magnesium, Fasting plasma glucose.

Published
2020
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20. Serum lipids in sub clinical hypothyroidism: A retrospective study

Author

Prabhavati Modi, M Amala Krishna, D. Sridevi, Amrut Arvindrao Dambal, Audi Bhagyalakshmi, and Lakshmi Chaitanya

Subjects
medicine.medical_specialty, endocrine system diseases, medicine.diagnostic_test, Cholesterol, Blood lipids, 030209 endocrinology & metabolism, Retrospective cohort study, Lipid metabolism, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, chemistry, 030220 oncology & carcinogenesis, Internal medicine, Basal metabolic rate, medicine, lipids (amino acids, peptides, and proteins), Risk factor, Lipid profile, Subclinical infection
Abstract

Background: Thyroid hormones are a potent regulator of metabolism, playing a crucial role in regulating energy expenditure and in key physiological mechanisms. Their prominent and well-known role is an increase in basal energy expenditure obtained by acting on carbohydrate, protein and lipid-metabolism. Hypothyroidism is relatively common and is associated with an unfavorable effect on lipid metabolism. Few studies reveal subclinical hypothyroidism to be a risk factor for increased incidence of lipid abnormalities and resulting in cardiovascular abnormalities. Aim: Hence study was taken up to find the association of serum lipids with subclinical hypothyroidism. Methodology: This was a retrospective study conducted in the department of Biochemistry, Malla Reddy hospital. Biochemically identified 102 subjects of Subclinical hypothyroidism subjects between 15-50 years and evaluated for lipid profile were included in the study. In our study, the mean serum total cholesterol, triglycerides, HDL cholesterol and LDL cholesterol expressed in mg/dl were 189.9824.16, 166.48+17.4, 37.62+2.89 and 121.34+27.31mg/dl respectively. 41 subjects out of 102 had higher total cholesterol, triglycerides and LDL cholesterol with lesser HDL cholesterol from the acceptable limits. Conclusion: We conclude that impaired lipid parameters are associated with subclinical hypothyroidism. Hence a regular screening for lipid profile should be considered in subclinical hypothyroidism for early diagnosis, prevention and management of cardiovascular complications. Keywords: TSH, HDL cholesterol, LDL cholesterol, Sub clinical hypothyroidism.

Published
2020
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22. Sensitive Analysis on Selection of Piston Material Using MADM Techniques

Author

K Lakshmi Chaitanya and Kolla Srinivas

Subjects
Computer science, Mechanical Engineering, saw, ahp, Sensitive analysis, Mechanical engineering, 02 engineering and technology, 021001 nanoscience & nanotechnology, Engineering (General). Civil engineering (General), wpm, mcdm methods, law.invention, swing, Piston, 020303 mechanical engineering & transports, 0203 mechanical engineering, law, TA1-2040, 0210 nano-technology, entropy, Selection (genetic algorithm)
Abstract

Decision making in material selection plays important role in selecting appropriate material based on design and manufacturing attributes. Proposing a new material is always a challenging task so the researchers used Decision making assistance tools. In the Present paper the application of Multi-Attribute Decision Making (MADM) methods are applied to the piston material selection for optimal design process. Comparative study of subjective and objective criteria weights on selected MADM methods are done. Sensitivity analysis is conducted to prove the consistency in performance score ranking order as the criteria weights for each alternative varies.

Published
2019

23. Optimization Of Wear Behaviour Of LM26-Gr Composite Using Taguchi Based Grey Relational Analysis

Author

et. al., K. Lakshmi Chaitanya and et. al., K. Lakshmi Chaitanya

Abstract

The progression in present manufacturing technology created the need of developing new materials for superior wear resistance. The objective of this paper is to optimize the three process parameters wear loss, wear rate, specific wear at three different levels with Taguchi technique in L9 Orthogonal array. A multi-response optimization technique Grey relational analysis is used to obtain the single process parameter setting for both the responses. LM26 metal matrix composite is fabricated by stir casting technique with Almandine garnet particles as reinforcement in different weight percentages with two different particle sizes. Analysis of Variance (ANOVA) was conducted to recognize the prevalent factor and found all the three factors as being critical. The above process was validated by Linear regression technique after conformation tests has been performed.

Published
2021

24. Prevalence of self-medication in rural area of Andhra Pradesh

Author

Venkatasandhya Korukonda, Gaurav M. Rangari, Roza G. Bhaisare, Y Lakshmi Chaitanya, and N Hanumanth

Subjects
Consumption (economics), Contingency table, business.industry, lcsh:R, Developing country, lcsh:Medicine, Simple random sample, drugs, self-medication, over the counter, symbols.namesake, Environmental health, Respondent, symbols, Medicine, Original Article, rural, Rural area, andhra pradesh, business, Fisher's exact test, Self-medication
Abstract

Background: The consumption of medicine without consulting a doctor is called self-medication. In the recent decade, the prevalence of self-medication was increased mainly in the developing countries. The reason varies from the nonavailability of doctors to economical reason. But people are not aware of the side effects and interactions of drugs. This is risky behavior and may lead to death. The objective of this study is to find out the prevalence and various reasons, sources, and common drugs used for self-medication. Materials and Methods: A cross-sectional community-based study conducted in Visakhapatnam district, Andhra Pradesh. 166 houses were selected by using a simple random sampling method. One respondent from one household was interviewed by using a semi-structured questionnaire. The data obtained were analyzed by using SPSS V22. Chi-square and Fisher exact tests were applied to find associations. Phi, Cramer Rao V, and contingency coefficient were applied to find the strength of association. A value of P < 0.05 was considered significant. Results: Among 166 subjects, the majority (58.4%) of participants were in the age group between 18-30 and most of them were female 142 (85.5%). The prevalence of self-medication was 68.1%. The main source of self-medication was directly from the pharmacy, that is, pharmacists (72.6%). Analgesics were commonly (85%) self-medicated drug. The main indication for self-medication was headache (78.8%) and fever (66.4%). Conclusion: The prevalence of self-medication was high and which is hazardous to health. This needs prompt legislative action.

Published
2020

25. The HIrisPlex-S system for eye, hair and skin colour prediction from DNA: Introduction and forensic developmental validation

Author

Susan Walsh, Laura Wirken, Krystal Breslin, Fan Liu, Sofia Zuniga, Ewelina Pośpiech, Lakshmi Chaitanya, Wojciech Branicki, Magdalena Kukla-Bartoszek, Manfred Kayser, Titia Sijen, Peter de Knijff, and Genetic Identification

Subjects
0301 basic medicine, S system, Forensic Genetics, genetic structures, Forensic developmental validation, Genotyping Techniques, HIrisPlex-S, predictive DNA analysis, Skin Pigmentation, Computational biology, Biology, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, eye colour, Pathology and Forensic Medicine, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Species Specificity, Genetics, Animals, Humans, Multiplex, 030216 legal & forensic medicine, skin colour, Hair Color, Predictive DNA analysis, Skin colour, Eye Color, Reproducibility of Results, DNA, forensic developmental validation, Forensic DNA phenotyping, hair colour, 030104 developmental biology, Phenotype, DNA profiling, chemistry, Snapshot (computer storage), Eye colour, Degraded dna, Hair colour, DNA phenotyping, forensic DNA phenotyping
Abstract

Forensic DNA Phenotyping (FDP), i.e. the prediction of human externally visible traits from DNA, has become a fast growing subfield within forensic genetics due to the intelligence information it can provide from DNA traces. FDP outcomes can help focus police investigations in search of unknown perpetrators, who are generally unidentifiable with standard DNA profiling. Therefore, we previously developed and forensically validated the IrisPlex DNA test system for eye colour prediction and the HIrisPlex system for combined eye and hair colour prediction from DNA traces. Here we introduce and forensically validate the HIrisPlex-S DNA test system (S for skin) for the simultaneous prediction of eye, hair, and skin colour from trace DNA. This FDP system consists of two SNaPshot-based multiplex assays targeting a total of 41 SNPs via a novel multiplex assay for 17 skin colour predictive SNPs and the previous HIrisPlex assay for 24 eye and hair colour predictive SNPs, 19 of which also contribute to skin colour prediction. The HIrisPlex-S system further comprises three statistical prediction models, the previously developed IrisPlex model for eye colour prediction based on 6 SNPs, the previous HIrisPlex model for hair colour prediction based on 22 SNPs, and the recently introduced HIrisPlex-S model for skin colour prediction based on 36 SNPs. In the forensic developmental validation testing, the novel 17-plex assay performed in full agreement with the Scientific Working Group on DNA Analysis Methods (SWGDAM) guidelines, as previously shown for the 24-plex assay. Sensitivity testing of the 17-plex assay revealed complete SNP profiles from as little as 63 pg of input DNA, equalling the previously demonstrated sensitivity threshold of the 24-plex HIrisPlex assay. Testing of simulated forensic casework samples such as blood, semen, saliva stains, of inhibited DNA samples, of low quantity touch (trace) DNA samples, and of artificially degraded DNA samples as well as concordance testing, demonstrated the robustness, efficiency, and forensic suitability of the new 17-plex assay, as previously shown for the 24-plex assay. Finally, we provide an update to the publically available HIrisPlex website https://hirisplex.erasmusmc.nl/ , now allowing the estimation of individual probabilities for 3 eye, 4 hair, and 5 skin colour categories from HIrisPlex-S input genotypes. The HIrisPlex-S DNA test represents the first forensically validated tool for skin colour prediction, and reflects the first forensically validated tool for simultaneous eye, hair and skin colour prediction from DNA.

Published
2018

26. Towards broadening Forensic DNA Phenotyping beyond pigmentation: Improving the prediction of head hair shape from DNA

Author

Sarah E. Medland, Christopher Phillips, Sijie J. Wu, Ewelina Pośpiech, Lorena Girón-Santamaría, Theresa E. Gross, Ana Freire-Aradas, Ghu Zhu, Shuhua Xu, David Ballard, Manfred Kayser, Yan Chen, Fan Liu, Ana Mosquera-Miguel, Sijia Wang, Marielle Vennemann, Anastasia Aliferi, Peter M. Schneider, Niels Morling, Krystal Breslin, Nicholas G. Martin, Cordula Haas, Li Jin, Susan Walsh, Angel Carracedo, Gabriela Huber, Mario Gysi, Titia Sijen, Denise Syndercombe-Court, Lakshmi Chaitanya, Wojciech Branicki, Jeppe Dyrberg Andersen, Magdalena Kukla-Bartoszek, Małgorzata Skowron, Charanya Muralidharan, Walther Parson, Kristiaan J. van der Gaag, and Genetic Identification

Subjects
Adult, 0301 basic medicine, Genotyping Techniques, Single-nucleotide polymorphism, Computational biology, Biology, Polymorphism, Single Nucleotide, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Genotype-phenotype distinction, head hair, Genetics, Humans, SNP, 030216 legal & forensic medicine, Massive parallel sequencing, Models, Genetic, targeted massively parallel sequencing, High-Throughput Nucleotide Sequencing, Paleogenetics, DNA, Sequence Analysis, DNA, Ion semiconductor sequencing, hair shape, DNA prediction, Logistic Models, Phenotype, 030104 developmental biology, Genetic marker, Sample size determination, Forensic DNA Phenotyping, externally visible characteristics, Genome-Wide Association Study, Hair
Abstract

Human head hair shape, commonly classified as straight, wavy, curly or frizzy, is an attractive target for Forensic DNA Phenotyping and other applications of human appearance prediction from DNA such as in paleogenetics. The genetic knowledge underlying head hair shape variation was recently improved by the outcome of a series of genome-wide association and replication studies in a total of 26,964 subjects, highlighting 12 loci of which 8 were novel and introducing a prediction model for Europeans based on 14 SNPs. In the present study, we evaluated the capacity of DNA-based head hair shape prediction by investigating an extended set of candidate SNP predictors and by using an independent set of samples for model validation. Prediction model building was carried out in 9,674 subjects (6,068 from Europe, 2,899 from Asia and 707 of admixed European and Asian ancestries), used previously, by considering a novel list of 90 candidate SNPs. For model validation, genotype and phenotype data were newly collected in 2,415 independent subjects (2,138 Europeans and 277 non-Europeans) by applying two targeted massively parallel sequencing platforms, Ion Torrent PGM and MiSeq, or the MassARRAY platform. A binomial model was developed to predict straight vs. non-straight hair based on 32 SNPs from 26 genetic loci we identified as significantly contributing to the model. This model achieved prediction accuracies, expressed as AUC, of 0.664 in Europeans and 0.789 in non-Europeans; the statistically significant difference was explained mostly by the effect of one EDAR SNP in non-Europeans. Considering sex and age, in addition to the SNPs, slightly and insignificantly increased the prediction accuracies (AUC of 0.680 and 0.800, respectively). Based on the sample size and candidate DNA markers investigated, this study provides the most robust, validated, and accurate statistical prediction models and SNP predictor marker sets currently available for predicting head hair shape from DNA, providing the next step towards broadening Forensic DNA Phenotyping beyond pigmentation traits.

Published
2018
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29. Global skin colour prediction from DNA

Author

Krystal Breslin, Lakshmi Chaitanya, Andreas Wollstein, Susan Walsh, Leda Kovatsi, Julia Koller, Ewelina Pospiech, Wojciech Branicki, Charanya Muralidharan, Agnieszka Bronikowska, Manfred Kayser, Fan Liu, and Genetic Identification

Subjects
Genetic Markers, Male, 0301 basic medicine, Genotype, Genotyping Techniques, genetic structures, Black People, Skin Pigmentation, Single-nucleotide polymorphism, Human skin, Biology, Intermediate level, Polymorphism, Single Nucleotide, Sensitivity and Specificity, Publisher's Erratum, White People, Standard deviation, 03 medical and health sciences, 0302 clinical medicine, Statistics, Genetics, Humans, 030216 legal & forensic medicine, Hair Color, Genetics (clinical), Models, Statistical, Models, Genetic, DNA, Skin colour, Human genetics, Logistic Models, Phenotype, 030104 developmental biology, Genetic marker, Female, DNA phenotyping
Abstract

Human skin colour is highly heritable and externally visible with relevance in medical, forensic, and anthropological genetics. Although eye and hair colour can already be predicted with high accuracies from small sets of carefully selected DNA markers, knowledge about the genetic predictability of skin colour is limited. Here, we investigate the skin colour predictive value of 77 single-nucleotide polymorphisms (SNPs) from 37 genetic loci previously associated with human pigmentation using 2025 individuals from 31 global populations. We identified a minimal set of 36 highly informative skin colour predictive SNPs and developed a statistical prediction model capable of skin colour prediction on a global scale. Average cross-validated prediction accuracies expressed as area under the receiver-operating characteristic curve (AUC) ± standard deviation were 0.97 ± 0.02 for Light, 0.83 ± 0.11 for Dark, and 0.96 ± 0.03 for Dark-Black. When using a 5-category, this resulted in 0.74 ± 0.05 for Very Pale, 0.72 ± 0.03 for Pale, 0.73 ± 0.03 for Intermediate, 0.87±0.1 for Dark, and 0.97 ± 0.03 for Dark-Black. A comparative analysis in 194 independent samples from 17 populations demonstrated that our model outperformed a previously proposed 10-SNP-classifier approach with AUCs rising from 0.79 to 0.82 for White, comparable at the intermediate level of 0.63 and 0.62, respectively, and a large increase from 0.64 to 0.92 for Black. Overall, this study demonstrates that the chosen DNA markers and prediction model, particularly the 5-category level; allow skin colour predictions within and between continental regions for the first time, which will serve as a valuable resource for future applications in forensic and anthropologic genetics.

Published
2017
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30. A collaborative EDNAP exercise on SNaPshot (TM)-based mtDNA control region typing

Author

Cordula Haas, Lakshmi Chaitanya, Manfred Kayser, P. Woliński, K. Baca, Claus Børsting, Vania Pereira, J. Červenáková, Ana Mosquera-Miguel, Michael D. Coble, Fabrice Noel, Francesca Brisighelli, Magdalena Bogus, Walther Parson, Stijn Desmyter, M. Turanská, Natalie E.C. Weiler, Arnoud J. Kal, M. João Porto, A. Kúdelová, Niels Morling, Titia Sijen, K.J. van der Gaag, V. Decroyer, Peter M. Schneider, Christopher Phillips, F. Balsa, Athina Vidaki, L. Zatkalíková, David Ballard, Josephin Heinrich, D. Syndercombe Court, Katherine Butler Gettings, and Genetic Identification

Subjects
Forensic Genetics, 0301 basic medicine, Massively parallel sequencing, Forensic science, Haplogroup, mtDNA, SNaPshot, 2734, Genetics, Settore BIO/08 - ANTROPOLOGIA, Single-nucleotide polymorphism, Biology, DNA, Mitochondrial, Polymorphism, Single Nucleotide, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Humans, SNP, 030216 legal & forensic medicine, Typing, mtDNA control region, DNA Fingerprinting, 030104 developmental biology, Haplotypes, DNA profiling, Snapshot (computer storage), Laboratories, Human mitochondrial DNA haplogroup
Abstract

A collaborative European DNA Profiling (EDNAP) Group exercise was undertaken to assess the performance of an earlier described SNaPshot™-based screening assay (denoted mini-mtSNaPshot) (Weiler et al., 2016) [1] that targets 18 single nucleotide polymorphism (SNP) positions in the mitochondrial (mt) DNA control region and allows for discrimination of major European mtDNA haplogroups. Besides the organising laboratory, 14 forensic genetics laboratories were involved in the analysis of 13 samples, which were centrally prepared and thoroughly tested prior to shipment. The samples had a variable complexity and comprised straightforward single-source samples, samples with dropout or altered peak sizing, a point heteroplasmy and two-component mixtures resulting in one to five bi-allelic calls. The overall success rate in obtaining useful results was high (97.6%) given that some of the participating laboratories had no previous experience with the typing technology and/or mtDNA analysis. The majority of the participants proceeded to haplotype inference to assess the feasibility of assigning a haplogroup and checking phylogenetic consistency when only 18 SNPs are typed. To mimic casework procedures, the participants compared the SNP typing data of all 13 samples to a set of eight mtDNA reference profiles that were described according to standard nomenclature (Parson et al., 2014) [2], and indicated whether these references matched each sample or not. Incorrect scorings were obtained for 2% of the comparisons and derived from a subset of the participants, indicating a need for training and guidelines regarding mini-mtSNaPshot data interpretation.

Published
2017
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31. Bringing colour back after 70 years: Predicting eye and hair colour from skeletal remains of World War II victims using the HIrisPlex system

Author

Manfred Kayser, Susan Walsh, Irena Zupanič Pajnič, Lakshmi Chaitanya, Tomaž Zupanc, Jože Balažic, and Genetic Identification

Subjects
Genetic Markers, 0301 basic medicine, Genotype, World War II, Sample (material), Slovenia, Datasets as Topic, Biology, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Bone and Bones, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Genetics, Humans, 030216 legal & forensic medicine, Hair Color, Missing person, Amelogenin, Eye Color, Models, Genetic, Dna concentration, Disaster victim identification, DNA, DNA Fingerprinting, Str profiling, 030104 developmental biology, Evolutionary biology, Tooth, Microsatellite Repeats
Abstract

Retrieving information about externally visible characteristics from DNA can provide investigative leads to find unknown perpetrators, and can also help in disaster victim and other missing person identification cases. Aiming for the application to both types of forensic casework, we previously developed and forensically validated the HIrisPlex test system enabling parallel DNA prediction of eye and hair colour. Although a recent proof-of-principle study demonstrated the general suitability of the HIrisPlex system for successfully analysing DNA from bones and teeth of various storage times and conditions, practical case applications to human remains are scarce. In this study, we applied the HIrisPlex system to 49 DNA samples obtained from bones or teeth of World War II victims excavated at six sites, mostly mass graves, in Slovenia. PCR-based DNA quantification ranged from 4 pg/μl to 313 pg/μl and on an average was 41 pg/μl across all samples. All 49 samples generated complete HIrisPlex profiles with the exception of one MC1R DNA marker (N29insA) missing in 83.7% of the samples. In 44 of the 49 samples (89.8%) complete 15-loci autosomal STR (plus amelogenin) profiles were obtained. Of 5 pairs of skeletal remains for which STR profiling suggested an origin in the same individuals, respectively, 4 showed the same HIrisPlex profiles and predicted eye and hair colours, respectively, while discrepancies in one pair (sample 26 and 43) are likely to be explained by DNA quantity and quality issues observed in sample 43. Sample 43 had the lowest DNA concentration of only 4 pg/μl, producing least reliable STR results and could be misleading in concluding that samples 43 and 26 originate from the same individual. The HIrisPlex-predicted eye and hair colours from two skeletal samples, suggested to derive from two brothers via STR profiling together with a living sister, were confirmed by the living sister's report. Overall, we demonstrate that after more than 70 years, HIrisPlex-based eye and hair colour prediction from skeletal remains is feasible with high success rate. Our results further encourage the use of the HIrisPlex system in missing person/disaster victim identification to aid the identification process in cases where ante-mortem samples or putative relatives are not directly available, and DNA predicted eye and hair colour information provides leads for locating them, allowing STRbased individual identification.

Published
2017

32. Effectiveness of seminar as an educational tool among the undergraduate medical students: A study

Author

K Ravibabu, D. Sridevi, A Bhagyalakshmi, Amrut Arvindrao Dambal, and G. Lakshmi Chaitanya

Subjects
Medical education, Presentation, Medical curriculum, media_common.quotation_subject, Learning methods, Subject (documents), Citizen journalism, Communication skills, Teaching learning, Effective teaching, media_common
Abstract

Background: The faculty of medical colleges have a greater responsibility in making the study methods of their subject innovative, interesting and participatory for the under graduate students. One such method is organizing seminars for the undergraduate students. Objective: To assess effectiveness of student seminars as a teaching learning method in the undergraduate medical curriculum. Methods: This study was conducted in the Department of Biochemistry, Malla Reddy Institute of Medical Sciences, Hyderabad on a group of 150 students. This study assesses the role of seminar as teaching-learning tool by recording the effectiveness and perception of medical students on seminars through a pre-test/post-test evaluation and questionnaire-based survey. Results: A highly significant improvement (p

Published
2020
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33. Forensic ancestry analysis with two capillary electrophoresis ancestry informative marker (AIM) panels: Results of a collaborative EDNAP exercise

Author

D. Syndercombe Court, R. Banemann, P. Hoff-Olsen, Katherine Butler Gettings, Peter M. Schneider, Adrian Linacre, Priscila Kohler, A. Roseth, Ryan England, M. Mayr-Eduardoff, R.A.H. van Oorschot, Claus Børsting, Francesca Brisighelli, A. Hoffmann, Maria João Porto, Theresa E. Gross, M. Burrington, A.M. Bento, Marcos F. Fondevila, Jennifer E. L. Templeton, Wojciech Branicki, Angel Carracedo, Vlastimil Stenzl, M. Turanská, V. L. Pascali, Cordula Haas, V. Decroyer, Lakshmi Chaitanya, Geraldine O’Donnell, Carla Santos, Catherine McGovern, Niels Morling, Joyce Harteveld, Peter M. Vallone, Runa Daniel, Walther Parson, Tomas Capal, David Ballard, L. Zatkalíková, Christopher Phillips, Titia Sijen, Manfred Kayser, and Genetic Identification

Subjects
Forensic Genetics, Genetic Markers, Genotype, Concordance, Aims, Settore BIO/08 - ANTROPOLOGIA, Ancestry-informative marker, Biology, Polymorphism, Single Nucleotide, Bayes analysis, Pathology and Forensic Medicine, Genetics, Humans, principal component analysis (PCA), Indel, Genotyping, Ancestry, ancestry, aims, Electrophoresis, Capillary, DNA, Single-base extension, SNP genotyping, Indels, bayes analysis, Principal component analysis (PCA), DNA profiling, indels, SNPs, SNP array
Abstract

There is increasing interest in forensic ancestry tests, which are part of a growing number of DNA analyses that can enhance routine profiling by obtaining additional genetic information about unidentified DNA donors. Nearly all ancestry tests use single nucleotide polymorphisms (SNPs), but these currently rely on SNaPshot single base extension chemistry that can fail to detect mixed DNA. Insertion-deletion polymorphism (Indel) tests have been developed using dye-labeled primers that allow direct capillary electrophoresis detection of PCR products (PCR-to-CE). PCR-to-CE maintains the direct relationship between input DNA and signal strength as each marker is detected with a single dye, so mixed DNA is more reliably detected. We report the results of a collaborative inter-laboratory exercise of 19 participants (15 from the EDNAP European DNA Profiling group) that assessed a 34-plex SNP test using SNaPshot and a 46-plex Indel test using PCR-to-CE. Laboratories were asked to type five samples with different ancestries and detect an additional mixed DNA sample. Statistical inference of ancestry was made by participants using the Snipper online Bayes analysis portal plus an optional PCA module that analyzes the genotype data alongside calculation of Bayes likelihood ratios. Exercise results indicated consistent genotyping performance from both tests, reaching a particularly high level of reliability for the Indel test. SNP genotyping gave 93.5% concordance (compared to the organizing laboratory's data) that rose to 97.3% excluding one laboratory with a large number of miscalled genotypes. Indel genotyping gave a higher concordance rate of 99.8% and a reduced no-call rate compared to SNP analysis. All participants detected the mixture from their Indel peak height data and successfully assigned the correct ancestry to the other samples using Snipper, with the exception of one laboratory with SNP miscalls that incorrectly assigned ancestry of two samples and did not obtain informative likelihood ratios for a third. Therefore, successful ancestry assignments were achieved by participants in 92 of 95 Snipper analyses. This exercise demonstrates that ancestry inference tests based on binary marker sets can be readily adopted by laboratories that already have well-established CE regimes in place. The Indel test proved to be easy to use and allowed all exercise participants to detect the DNA mixture as well as achieving complete and concordant profiles in nearly all cases. Lastly, two participants successfully ran parallel next-generation sequencing analyses (each using different systems) and achieved high levels of genotyping concordance using the exercise PCR primer mixes unmodified. (C) 2015 Elsevier Ireland Ltd. All rights reserved.

Published
2015
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34. Simultaneous Whole Mitochondrial Genome Sequencing with Short Overlapping Amplicons Suitable for Degraded DNA Using the Ion Torrent Personal Genome Machine

Author

Mannis van Oven, Robert Lagacé, Lakshmi Chaitanya, Tomasz Kupiec, Joseph Chang, Arwin Ralf, Manfred Kayser, and Genetic Identification

Subjects
MPS, Method, next‐generation sequencing, Hybrid genome assembly, Genomics, Computational biology, Biology, Genome, DNA, Mitochondrial, Sensitivity and Specificity, DNA sequencing, Genetics, Methods, DNA Barcoding, Taxonomic, Humans, Genetics (clinical), Exome sequencing, Massive parallel sequencing, mtDNA, massively parallel sequencing, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Ion semiconductor sequencing, Amplicon, mitochondria, Haplotypes, NGS, Genome, Mitochondrial
Abstract

Whole mitochondrial (mt) genome analysis enables a considerable increase in analysis throughput, and improves the discriminatory power to the maximum possible phylogenetic resolution. Most established protocols on the different massively parallel sequencing (MPS) platforms, however, invariably involve the PCR amplification of large fragments, typically several kilobases in size, which may fail due to mtDNA fragmentation in the available degraded materials. We introduce a MPS tiling approach for simultaneous whole human mt genome sequencing using 161 short overlapping amplicons (average 200 bp) with the Ion Torrent Personal Genome Machine. We illustrate the performance of this new method by sequencing 20 DNA samples belonging to different worldwide mtDNA haplogroups. Additional quality control, particularly regarding the potential detection of nuclear insertions of mtDNA (NUMTs), was performed by comparative MPS analysis using the conventional long‐range amplification method. Preliminary sensitivity testing revealed that detailed haplogroup inference was feasible with 100 pg genomic input DNA. Complete mt genome coverage was achieved from DNA samples experimentally degraded down to genomic fragment sizes of about 220 bp, and up to 90% coverage from naturally degraded samples. Overall, we introduce a new approach for whole mt genome MPS analysis from degraded and nondegraded materials relevant to resolve and infer maternal genetic ancestry at complete resolution in anthropological, evolutionary, medical, and forensic applications.

Published
2015
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35. Genetics of skin color variation in Europeans: genome-wide association studies with functional follow-up

Author

Gu Zhu, Nicholas G. Martin, Pirro G. Hysi, Kaiyin Zhong, Massimo Mangino, Richard A. Sturm, Susan Walsh, Anjali K. Henders, Fan Liu, Tamar Nijsten, André G. Uitterlinden, Leonie C. Jacobs, Daniel Glass, Albert Hofman, Manfred Kayser, Tim D. Spector, Fernando Rivadeneira, Wilfred F. J. van IJcken, Lakshmi Chaitanya, Robert-Jan Palstra, David L. Duffy, Grant W. Montgomery, Mijke Visser, Oscar Lao, Andreas Wollstein, Veronique Bataille, Genetic Identification, Dermatology, Internal Medicine, Epidemiology, Cell biology, and Biochemistry

Subjects
Male, SLC45A2, Ubiquitin-Protein Ligases, Skin Pigmentation, Genome-wide association study, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, White People, Antigens, Neoplasm, Genetics, Chromosomes, Human, Guanine Nucleotide Exchange Factors, Humans, Genetics(clinical), Genetics (clinical), Original Investigation, Genetic association, OCA2, Membrane Transport Proteins, Middle Aged, United Kingdom, Human genetics, Skin Color Score, Genetic Loci, Genetic marker, Interferon Regulatory Factors, biology.protein, Agouti Signaling Protein, Female, Follow-Up Studies, Genome-Wide Association Study
Abstract

In the International Visible Trait Genetics (VisiGen) Consortium, we investigated the genetics of human skin color by combining a series of genome-wide association studies (GWAS) in a total of 17,262 Europeans with functional follow-up of discovered loci. Our GWAS provide the first genome-wide significant evidence for chromosome 20q11.22 harboring the ASIP gene being explicitly associated with skin color in Europeans. In addition, genomic loci at 5p13.2 (SLC45A2), 6p25.3 (IRF4), 15q13.1 (HERC2/OCA2), and 16q24.3 (MC1R) were confirmed to be involved in skin coloration in Europeans. In follow-up gene expression and regulation studies of 22 genes in 20q11.22, we highlighted two novel genes EIF2S2 and GSS, serving as competing functional candidates in this region and providing future research lines. A genetically inferred skin color score obtained from the 9 top-associated SNPs from 9 genes in 940 worldwide samples (HGDP-CEPH) showed a clear gradual pattern in Western Eurasians similar to the distribution of physical skin color, suggesting the used 9 SNPs as suitable markers for DNA prediction of skin color in Europeans and neighboring populations, relevant in future forensic and anthropological investigations. Electronic supplementary material The online version of this article (doi:10.1007/s00439-015-1559-0) contains supplementary material, which is available to authorized users.

Published
2015
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36. Erratum to: Global skin colour prediction from DNA

Author

Fan Liu, Charanya Muralidharan, Andreas Wollstein, Krystal Breslin, Julia Koller, Manfred Kayser, Leda Kovatsi, Lakshmi Chaitanya, Agnieszka Bronikowska, Susan Walsh, Ewelina Pospiech, and Wojciech Branicki

Subjects
0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Column (typography), ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, Genetics, Biology, Skin colour, Algorithm, Genetics (clinical), Original Investigation
Abstract

Human skin colour is highly heritable and externally visible with relevance in medical, forensic, and anthropological genetics. Although eye and hair colour can already be predicted with high accuracies from small sets of carefully selected DNA markers, knowledge about the genetic predictability of skin colour is limited. Here, we investigate the skin colour predictive value of 77 single-nucleotide polymorphisms (SNPs) from 37 genetic loci previously associated with human pigmentation using 2025 individuals from 31 global populations. We identified a minimal set of 36 highly informative skin colour predictive SNPs and developed a statistical prediction model capable of skin colour prediction on a global scale. Average cross-validated prediction accuracies expressed as area under the receiver-operating characteristic curve (AUC) ± standard deviation were 0.97 ± 0.02 for Light, 0.83 ± 0.11 for Dark, and 0.96 ± 0.03 for Dark-Black. When using a 5-category, this resulted in 0.74 ± 0.05 for Very Pale, 0.72 ± 0.03 for Pale, 0.73 ± 0.03 for Intermediate, 0.87±0.1 for Dark, and 0.97 ± 0.03 for Dark-Black. A comparative analysis in 194 independent samples from 17 populations demonstrated that our model outperformed a previously proposed 10-SNP-classifier approach with AUCs rising from 0.79 to 0.82 for White, comparable at the intermediate level of 0.63 and 0.62, respectively, and a large increase from 0.64 to 0.92 for Black. Overall, this study demonstrates that the chosen DNA markers and prediction model, particularly the 5-category level; allow skin colour predictions within and between continental regions for the first time, which will serve as a valuable resource for future applications in forensic and anthropologic genetics. Electronic supplementary material The online version of this article (doi:10.1007/s00439-017-1808-5) contains supplementary material, which is available to authorized users.

Published
2017

37. Developmental validation of the HIrisPlex system: DNA-based eye and hair colour prediction for forensic and anthropological usage

Author

Peter de Knijff, Fan Liu, Takaki Ishikawa, Susan Walsh, Lindy Clarisse, Hitoshi Maeda, Titia Sijen, Wojciech Branicki, Laura Wirken, Manfred Kayser, Leda Kovatsi, Lakshmi Chaitanya, Jolanta Draus-Barini, and Genetic Identification

Subjects
Forensic Genetics, Heterozygote, Validation study, Genotype, SNP, Computational biology, Biology, FDP, Polymorphism, Single Nucleotide, Pathology and Forensic Medicine, 03 medical and health sciences, Forensic dna, chemistry.chemical_compound, SWGDAM, 0302 clinical medicine, Hair colour prediction, Semen, Genetics, developmental validation, Humans, 030216 legal & forensic medicine, Hair Color, Saliva, Alleles, 030304 developmental biology, 0303 health sciences, Missing person, Eye colour prediction, Forensic DNA Phenotyping (FDP), eye colour prediction, Eye Color, DNA, 16. Peace & justice, Developmental validation, Ancient DNA, DNA profiling, chemistry, Forensic DNA Phenotyping, HIrisPlex, Degraded dna, DNA phenotyping, Blood Chemical Analysis, Forensic DNA Phenotyping, FDP, hair colour prediction, Hair
Abstract

Forensic DNA Phenotyping or 'DNA intelligence' tools are expected to aid police investigations and find unknown individuals by providing information on externally visible characteristics of unknown suspects, perpetrators and missing persons from biological samples. This is especially useful in cases where conventional DNA profiling or other means remain non-informative. Recently, we introduced the HIrisPlex system, capable of predicting both eye and hair colour from DNA. In the present developmental validation study, we demonstrate that the HIrisPlex assay performs in full agreement with the Scientific Working Group on DNA Analysis Methods (SWGDAM) guidelines providing an essential prerequisite for future HIrisPlex applications to forensic casework. The HIrisPlex assay produces complete profiles down to only 63 pg of DNA. Species testing revealed human specificity for a complete HIrisPlex profile, while only non-human primates showed the closest full profile at 20 out of the 24 DNA markers, in all animals tested. Rigorous testing of simulated forensic casework samples such as blood, semen, saliva stains, hairs with roots as well as extremely low quantity touch (trace) DNA samples, produced complete profiles in 88% of cases. Concordance testing performed between five independent forensic laboratories displayed consistent reproducible results on varying types of DNA samples. Due to its design, the assay caters for degraded samples, underlined here by results from artificially degraded DNA and from simulated casework samples of degraded DNA. This aspect was also demonstrated previously on DNA samples from human remains up to several hundreds of years old. With this paper, we also introduce enhanced eye and hair colour prediction models based on enlarged underlying databases of HIrisPlex genotypes and eye/hair colour phenotypes (eye colour: N = 9188 and hair colour: N = 1601). Furthermore, we present an online web-based system for individual eye and hair colour prediction from full and partial HIrisPlex DNA profiles. By demonstrating that the HIrisPlex assay is fully compatible with the SWGDAM guidelines, we provide the first forensically validated DNA test system for parallel eye and hair colour prediction now available to forensic laboratories for immediate casework application, including missing person cases. Given the robustness and sensitivity described here and in previous work, the HIrisPlex system is also suitable for analysing old and ancient DNA in anthropological and evolutionary studies. (C) 2013 Elsevier Ireland Ltd. All rights reserved.

Published
2014
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38. High-quality mtDNA control region sequences from 680 individuals sampled across the Netherlands to establish a national forensic mtDNA reference database

Author

Silke Brauer, Catarina Xavier, Walther Parson, Peter de Knijff, Bettina Zimmermann, Manfred Kayser, Gabriela Huber, Lakshmi Chaitanya, Mannis van Oven, and Genetic Identification

Subjects
0301 basic medicine, Forensic Genetics, Male, Mitochondrial DNA, Population, Forensic database, Biology, DNA, Mitochondrial, Polymerase Chain Reaction, Haplogroup, Pathology and Forensic Medicine, 03 medical and health sciences, Control region, 0302 clinical medicine, Databases, Genetic, Genetics, Sequencing, Humans, 030216 legal & forensic medicine, education, DNA Primers, Netherlands, mtDNA control region, education.field_of_study, Phylogenetic tree, mtDNA, Haplotype, Sequence Analysis, DNA, Accession number (bioinformatics), Reference Standards, Mitochondria, 030104 developmental biology, Genetics, Population, Haplotypes, Evolutionary biology, Haplogroups, Databases, Nucleic Acid, EMPOP, Human mitochondrial DNA haplogroup
Abstract

The use of mitochondrial DNA (mtDNA) for maternal lineage identification often marks the last resort when investigating forensic and missing-person cases involving highly degraded biological materials. As with all comparative DNA testing, a match between evidence and reference sample requires a statistical interpretation, for which high-quality mtDNA population frequency data are crucial. Here, we determined, under high quality standards, the complete mtDNA control-region sequences of 680 individuals from across the Netherlands sampled at 54 sites, covering the entire country with 10 geographic sub-regions. The complete mtDNA control region (nucleotide positions 16,024-16,569 and 1-576) was amplified with two PCR primers and sequenced with ten different sequencing primers using the EMPOP protocol. Haplotype diversity of the entire sample set was very high at 99.63% and, accordingly, the random-match probability was 0.37%. No population substructure within the Netherlands was detected with our dataset. Phylogenetic analyses were performed to determine mtDNA haplogroups. Inclusion of these high-quality data in the EMPOP database (accession number: EMP00666) will improve its overall data content and geographic coverage in the interest of all EMPOP users worldwide. Moreover, this dataset will serve as (the start of) a national reference database for mtDNA applications in forensic and missing person casework in the Netherlands. (C) 2015 Elsevier Ireland Ltd. All rights reserved.

Published
2016

40. Collaborative EDNAP exercise on the IrisPlex system for DNA-based prediction of human eye colour

Author

Christine Keyser, A.M. Bento, Ricky Ansell, Adrian Linacre, Lívia Zatkalíková, David Ballard, Helena Nilsson, Susan Walsh, Titia Sijen, Jens Söchtig, Tomasz Kupiec, Regine Banemann, Wojciech Branicki, Peter M. Vallone, Walther Parson, Vincenzo Lorenzo Pascali, L. Norén, Andreas O. Tillmar, Martina Turanska, Priscila Kohler, Peter M. Schneider, Clémence Hollard, Theresa E. Gross, Jukka U. Palo, Antti Sajantila, Kevin M. Kiesler, Anastassiya Zidkova, Tomas Capal, Lindy Clarisse, Kaye N. Ballantyne, Francesca Brisighelli, Denise Syndercombe-Court, Niels Morling, Manfred Kayser, Cordula Haas, Christiane Maria Bauer, Jeppe Dyrberg Andersen, Lakshmi Chaitanya, Renée Ottens, P. Hoff-Olsen, Maria João Porto, Christopher Phillips, Anglika Minawi, Kayser, Manfred, and Genetic Identification

Subjects
ISFG, genetic structures, Population, Settore BIO/08 - ANTROPOLOGIA, Context (language use), Biology, FDP, Pathology and Forensic Medicine, EDNAP, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, 030216 legal & forensic medicine, education, Multiplex genotyping, Genotyping, 030304 developmental biology, IrisPlex, International level, 0303 health sciences, education.field_of_study, Eye colour prediction, Eye Color, eye colour prediction, DNA, Forensic DNA phenotyping, medicine.anatomical_structure, DNA profiling, Human eye, forensic DNA phenotyping, Forensic genetics
Abstract

The IrisPlex system is a DNA-based test system for the prediction of human eye colour from biological samples and consists of a single forensically validated multiplex genotyping assay together with a statistical prediction model that is based on genotypes and phenotypes from thousands of individuals. IrisPlex predicts blue and brown human eye colour with, on average, > 94% precision accuracy using six of the currently most eye colour informative single nucleotide polymorphisms (HERC2 rs12913832, OCA2 rs1800407, SLC24A4 rs12896399, SLC45A2 (MATP) rs16891982, TYR rs1393350, and IRF4 rs12203592) according to a previous study, while the accuracy in predicting non-blue and non-brown eye colours is considerably lower. In an effort to vigorously assess the IrisPlex system at the international level, testing was performed by 21 laboratories in the context of a collaborative exercise divided into three tasks and organised by the European DNA Profiling (EDNAP) Group of the International Society of Forensic Genetics (ISFG). Task 1 involved the assessment of 10 blood and saliva samples provided on FTA cards by the organising laboratory together with eye colour phenotypes; 99.4% of the genotypes were correctly reported and 99% of the eye colour phenotypes were correctly predicted. Task 2 involved the assessment of 5 DNA samples extracted by the host laboratory from simulated casework samples, artificially degraded, and provided to the participants in varying DNA concentrations. For this task, 98.7% of the genotypes were correctly determined and 96.2% of eye colour phenotypes were correctly inferred. For Tasks 1 and 2 together, 99.2% (1875) of the 1890 genotypes were correctly generated and of the 15 (0.8%) incorrect genotype calls, only 2 (0.1%) resulted in incorrect eye colour phenotypes. The voluntary Task 3 involved participants choosing their own test subjects for IrisPlex genotyping and eye colour phenotype inference, while eye photographs were provided to the organising laboratory and judged; 96% of the eye colour phenotypes were inferred correctly across 100 samples and 19 laboratories. The high success rates in genotyping and eye colour phenotyping clearly demonstrate the reproducibility and the robustness of the IrisPlex assay as well as the accuracy of the IrisPlex model to predict blue and brown eye colour from DNA. Additionally, this study demonstrates the ease with which the IrisPlex system is implementable and applicable across forensic laboratories around the world with varying pre-existing experiences. (c) 2014 Elsevier Ireland Ltd. All rights reserved.

Published
2014
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43. The Use of Big Data in Pharmaceutical Clinical Development

Author

Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, Avasthi, Aditya, Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, and Avasthi, Aditya

Abstract

Pharmaceutical industry is working towards developing new tools that would help increase the efficiency of drug development while reducing the time and expenditure involved in research & development (R&D) and clinical trials. The lack of new blockbuster drugs and short patent periods is one of the key reasons the pharmaceutical industry is trying to reduce costs. Clinical trials absorb the major chunk of investment in the drug discovery and development process. One of the reasons most of the pharmaceutical companies are exploring the available opportunities to use Information Technology services is to improve the efficiency by gaining faster response while reducing the time and cost involved in clinical trials. Perceptive Informatics, a subsidiary of PAREXEL is a leading eClinical solutions provider that focuses on helping customers to increase the product development process through innovation. The solutions offered help their customers to maximize the benefits of clinical trial technologies by providing flexible software-as-a-service (SaaS) applications. The services offered by perceptive include Randomization and Trial Supply Management technologies, Medical Imaging, Clinical Trial Management Systems, Electronic Data Capture (EDC) etc. The solutions offered by Perceptive Informatics eClinical result in simplified workflow, improved efficiency, and enhanced productivity. Pharmaceutical Industry like the most of other industries is driven by customer choices, thus making it important for companies to understand customer’s choices and needs. Data analytics plays a key role in analysing and understanding customer behaviour and preferences. Pharmaceutical industry relies on past data for forecasting present and future trends about trials, thus it is important to have Big Data system that can store and analyse huge chunks of data. By using Big Data analytics solutions and specifically high performance analytics, companies can analyse huge amounts of data in seconds and

44. Data Visualization and Visual Analytics in Clinical trials

Author

Telladarla, Lakshmi Chaitanya and Telladarla, Lakshmi Chaitanya

Abstract

In clinical trials even small amounts of data is critical in shaping the successful formulation of a drug and there is an increasing demand for easy and intuitive access to the data. Large, multicentre studies with different data collection techniques yield critical clinical information through every phase. The more efficiently study data is managed, the quicker the data can be extracted and analysed. During the initial stages of clinical trials, access to data is a serious need for resolving issues while they are still controllable and within the predicted cost frame. Data visualization empowers clinical development teams to quickly visualize and interact with huge volumes of clinical data in a single interface to support progressive decisions, rather than reviewing and tracking of results. Streamlining clinical trial data analysis with real time access to clinical data during all phases of clinical developments allows the user to interact with the data as soon as it is collected. Interactive visualizations allow users to explore the data easily and play around with it by applying filter criteria and decision making questions. Review and analysis of peripheral data using visual analytics can bring into light site performance and study resources, allowing enhancement of trial operations. Benefits of exploring crucial data (adverse events, demographics, lab values, drug exposure and response) in primary stages of clinical trial process are many. They serve to increase productivity by 20-40% by reducing errors and improving quality. Besides survival analysis capabilities that offer detailed models for patient accrual, dropout and time-to-event, valuable tools for study management, pharmacometrics, trial operations, pre-marketing security and post-marketing observation are also more feasible now with Data Visualization and Visual Analytics. The illustrations, statistical graphics can be exported for use in a variety of submission formats like presentation, publication

45. The Use of Big Data in Pharmaceutical Clinical Development

Author

Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, Avasthi, Aditya, Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, and Avasthi, Aditya

Abstract

Pharmaceutical industry is working towards developing new tools that would help increase the efficiency of drug development while reducing the time and expenditure involved in research & development (R&D) and clinical trials. The lack of new blockbuster drugs and short patent periods is one of the key reasons the pharmaceutical industry is trying to reduce costs. Clinical trials absorb the major chunk of investment in the drug discovery and development process. One of the reasons most of the pharmaceutical companies are exploring the available opportunities to use Information Technology services is to improve the efficiency by gaining faster response while reducing the time and cost involved in clinical trials. Perceptive Informatics, a subsidiary of PAREXEL is a leading eClinical solutions provider that focuses on helping customers to increase the product development process through innovation. The solutions offered help their customers to maximize the benefits of clinical trial technologies by providing flexible software-as-a-service (SaaS) applications. The services offered by perceptive include Randomization and Trial Supply Management technologies, Medical Imaging, Clinical Trial Management Systems, Electronic Data Capture (EDC) etc. The solutions offered by Perceptive Informatics eClinical result in simplified workflow, improved efficiency, and enhanced productivity. Pharmaceutical Industry like the most of other industries is driven by customer choices, thus making it important for companies to understand customer’s choices and needs. Data analytics plays a key role in analysing and understanding customer behaviour and preferences. Pharmaceutical industry relies on past data for forecasting present and future trends about trials, thus it is important to have Big Data system that can store and analyse huge chunks of data. By using Big Data analytics solutions and specifically high performance analytics, companies can analyse huge amounts of data in seconds and

46. The Use of Big Data in Pharmaceutical Clinical Development

Author

Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, Avasthi, Aditya, Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, and Avasthi, Aditya

Abstract

Pharmaceutical industry is working towards developing new tools that would help increase the efficiency of drug development while reducing the time and expenditure involved in research & development (R&D) and clinical trials. The lack of new blockbuster drugs and short patent periods is one of the key reasons the pharmaceutical industry is trying to reduce costs. Clinical trials absorb the major chunk of investment in the drug discovery and development process. One of the reasons most of the pharmaceutical companies are exploring the available opportunities to use Information Technology services is to improve the efficiency by gaining faster response while reducing the time and cost involved in clinical trials. Perceptive Informatics, a subsidiary of PAREXEL is a leading eClinical solutions provider that focuses on helping customers to increase the product development process through innovation. The solutions offered help their customers to maximize the benefits of clinical trial technologies by providing flexible software-as-a-service (SaaS) applications. The services offered by perceptive include Randomization and Trial Supply Management technologies, Medical Imaging, Clinical Trial Management Systems, Electronic Data Capture (EDC) etc. The solutions offered by Perceptive Informatics eClinical result in simplified workflow, improved efficiency, and enhanced productivity. Pharmaceutical Industry like the most of other industries is driven by customer choices, thus making it important for companies to understand customer’s choices and needs. Data analytics plays a key role in analysing and understanding customer behaviour and preferences. Pharmaceutical industry relies on past data for forecasting present and future trends about trials, thus it is important to have Big Data system that can store and analyse huge chunks of data. By using Big Data analytics solutions and specifically high performance analytics, companies can analyse huge amounts of data in seconds and

47. Data Visualization and Visual Analytics in Clinical trials

Author

Telladarla, Lakshmi Chaitanya and Telladarla, Lakshmi Chaitanya

Abstract

In clinical trials even small amounts of data is critical in shaping the successful formulation of a drug and there is an increasing demand for easy and intuitive access to the data. Large, multicentre studies with different data collection techniques yield critical clinical information through every phase. The more efficiently study data is managed, the quicker the data can be extracted and analysed. During the initial stages of clinical trials, access to data is a serious need for resolving issues while they are still controllable and within the predicted cost frame. Data visualization empowers clinical development teams to quickly visualize and interact with huge volumes of clinical data in a single interface to support progressive decisions, rather than reviewing and tracking of results. Streamlining clinical trial data analysis with real time access to clinical data during all phases of clinical developments allows the user to interact with the data as soon as it is collected. Interactive visualizations allow users to explore the data easily and play around with it by applying filter criteria and decision making questions. Review and analysis of peripheral data using visual analytics can bring into light site performance and study resources, allowing enhancement of trial operations. Benefits of exploring crucial data (adverse events, demographics, lab values, drug exposure and response) in primary stages of clinical trial process are many. They serve to increase productivity by 20-40% by reducing errors and improving quality. Besides survival analysis capabilities that offer detailed models for patient accrual, dropout and time-to-event, valuable tools for study management, pharmacometrics, trial operations, pre-marketing security and post-marketing observation are also more feasible now with Data Visualization and Visual Analytics. The illustrations, statistical graphics can be exported for use in a variety of submission formats like presentation, publication

48. The Use of Big Data in Pharmaceutical Clinical Development

Author

Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, Avasthi, Aditya, Telladarla, Lakshmi Chaitanya, Rajasagi, Gayatri Devi, and Avasthi, Aditya

Abstract

Pharmaceutical industry is working towards developing new tools that would help increase the efficiency of drug development while reducing the time and expenditure involved in research & development (R&D) and clinical trials. The lack of new blockbuster drugs and short patent periods is one of the key reasons the pharmaceutical industry is trying to reduce costs. Clinical trials absorb the major chunk of investment in the drug discovery and development process. One of the reasons most of the pharmaceutical companies are exploring the available opportunities to use Information Technology services is to improve the efficiency by gaining faster response while reducing the time and cost involved in clinical trials. Perceptive Informatics, a subsidiary of PAREXEL is a leading eClinical solutions provider that focuses on helping customers to increase the product development process through innovation. The solutions offered help their customers to maximize the benefits of clinical trial technologies by providing flexible software-as-a-service (SaaS) applications. The services offered by perceptive include Randomization and Trial Supply Management technologies, Medical Imaging, Clinical Trial Management Systems, Electronic Data Capture (EDC) etc. The solutions offered by Perceptive Informatics eClinical result in simplified workflow, improved efficiency, and enhanced productivity. Pharmaceutical Industry like the most of other industries is driven by customer choices, thus making it important for companies to understand customer’s choices and needs. Data analytics plays a key role in analysing and understanding customer behaviour and preferences. Pharmaceutical industry relies on past data for forecasting present and future trends about trials, thus it is important to have Big Data system that can store and analyse huge chunks of data. By using Big Data analytics solutions and specifically high performance analytics, companies can analyse huge amounts of data in seconds and

49. Data Visualization and Visual Analytics in Clinical trials

Author

Telladarla, Lakshmi Chaitanya and Telladarla, Lakshmi Chaitanya

Abstract

In clinical trials even small amounts of data is critical in shaping the successful formulation of a drug and there is an increasing demand for easy and intuitive access to the data. Large, multicentre studies with different data collection techniques yield critical clinical information through every phase. The more efficiently study data is managed, the quicker the data can be extracted and analysed. During the initial stages of clinical trials, access to data is a serious need for resolving issues while they are still controllable and within the predicted cost frame. Data visualization empowers clinical development teams to quickly visualize and interact with huge volumes of clinical data in a single interface to support progressive decisions, rather than reviewing and tracking of results. Streamlining clinical trial data analysis with real time access to clinical data during all phases of clinical developments allows the user to interact with the data as soon as it is collected. Interactive visualizations allow users to explore the data easily and play around with it by applying filter criteria and decision making questions. Review and analysis of peripheral data using visual analytics can bring into light site performance and study resources, allowing enhancement of trial operations. Benefits of exploring crucial data (adverse events, demographics, lab values, drug exposure and response) in primary stages of clinical trial process are many. They serve to increase productivity by 20-40% by reducing errors and improving quality. Besides survival analysis capabilities that offer detailed models for patient accrual, dropout and time-to-event, valuable tools for study management, pharmacometrics, trial operations, pre-marketing security and post-marketing observation are also more feasible now with Data Visualization and Visual Analytics. The illustrations, statistical graphics can be exported for use in a variety of submission formats like presentation, publication

50. MODELING AND SIMULATION OF HIERARCHICALLY DECOMPOSED R-2R LADDER DAC USING VHDL-AMS

Author

DURGARAJU, LAKSHMI CHAITANYA

Abstract

A wide variety of applications require mixed-signal modeling capabilities to accurately represent system behavior. Digital designs sometimes require mixed-signal modeling of high-performance components for which the digital modeling abstraction is not adequate. Since digital systems are really abstractions of well-behaved analog systems, we can use mixed-signal modeling to explore portions of digital-system behavior in more detail. Other systems are explicitly mixed signal with digital and analog parts. The digital and analog portions of the mixed-signal systems interact through digital-to-analog and analog-to-digital converters. They are the basic components in any mixed-signal systems. These mixed-signal systems can be modeled in various techniques. The most commonly used technique in software development is the hierarchical decomposition approach. No work has yet been observed that directly addresses a developmental approach based on hierarchical decomposition of software development for modeling hardware mixed-signal systems. This thesis explores the possibility of this approach for modeling and simulation of the most rudimentary and commonly used R-2R ladder digital-to-analog converter (DAC). The hierarchical decomposition of software development is applied to decompose the R-2R ladder DAC into different levels of fidelity and abstraction. The performance metrics at each level of abstraction is explored. To obtain the performance capabilities of the models we employ the rich features of VHDL-AMS (acronym for VHDL Analog Mixed Signal) [1]. VHDL –AMS is an extension of VHDL [2] which supports modeling and simulation of digital, analog and mixed-signal systems.

Published
2005

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