Vous avez cherché: in vitro fertility (Anglais - Hindi)

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in vitro fertility

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Anglais

in vitro fertilisation

Hindi

इन विट्रो गर्भाधान

Dernière mise à jour : 2015-05-26
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Anglais

in vitro was prepared for its growth .

Hindi

पात्रे को उसके विकास के लिए तैयार किया गया ।

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Anglais

in vitro fertilization of the ovum was carried out .

Hindi

अझडाणु का निषेचन कांच के अन्दर किया गया

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Anglais

in vitro study of medicine is done for experiment

Hindi

दवा का अंतः पात्र अध्ययन प्रयोग के लिए किया गया है

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Anglais

in - vitro fertilization because both of these involve the

Hindi

इन - विट्रो निषेचन क्योंकि इन दोनों को शामिल

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Anglais

the bacteria were grown in vitro in a growth medium .

Hindi

जीवाणु कृत्रिम वातावरण में एक विकास माध्यम में विकसित हुए

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Anglais

and that ' s why in - vitro fertilization often results in

Hindi

और यही कारण है कि इन विट्रो निषेचन अक्सर परिणाम है में

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Anglais

in vitro differentiation of human embryonic stem cells to neural and non - neural lineages .

Hindi

मानव भ्रूणीय स्टेएम सेल के टेस्टर ट्यूब में न्यूीरल और नॉन न्यू रल ।

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Anglais

a total of 67 mulberry accessions have been conserved in vitro and 238 accessions have been successfully cry preserved .

Hindi

शहतूत की कुल 67 नई प्रजातियों को परखनलियों में संरक्षित किया गया और 238 को सफलतापूर्वक क्रायोप्रिजर्व किया गया ।

Dernière mise à jour : 2020-05-24
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Anglais

preliminary data indicate that high doses of ribavirin are necessary to inhibit sars-cov-2 in vitro.

Hindi

प्रारंभिक आँकड़ों से संकेत मिलता है कि कृत्रिम परिवेशीय sars-cov-2 के संदमन के लिए रिबाविरिन की उच्च खुराकें आवश्यक हैं।

Dernière mise à jour : 2020-08-25
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Anglais

the advent of new techniques made it possible to bring about mutations in vitro by deliberate design instead of blind chance .

Hindi

इन नयी तकनीकों के आगमन से शरीर के बाहर किसी पात्र में उत्परिवर्तन करना संभव हो गया हैz तथा ऐसा करना कोई संयोग से होने वाली घटना नहीं हे . यह किसी योजनाबद्ध तरीके से करवाया जा सकता है .

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Anglais

when the recombination in vitro between vehicle and passenger dna is completed , the recombinant dna must be introduced into he host cell where it can replicate .

Hindi

शरीर के बाहर वाहन तथा यात्री डी . एन . ए . का पुनर्मिलासप पूरा होने के बाद यह आवश्यक हो जाता है कि इस पुनर्मिलापी डी . एन . ए . को किसी ऐसी आतिथेयी कोशिका में प्रविष्ट कराया जाये जहां वह अपनी प्रतिकृति का निर्माण कर सकता है .

Dernière mise à jour : 2020-05-24
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Anglais

studies carried out at sree chitra tirunal institute for medical sciences and technology , trivandrum , using an in vitro cell culture model to evaluate the response of adult rat cardiac fibroblasts to hypoxia ;

Hindi

श्री चित्रा तिरूनल आयुर्विज्ञान और प्रौद्योगिकी संस्थान , तिरूवनंतपुरम में वयस्क चूहे के हृदय की फाइब्रोब्लास्ट की हाइपोक्सिया के प्रति प्रतिक्रिया के आकलन के लिए परखनली में कोशिका संवर्धन मॉडल में इस्तेमाल से अध्ययन किए गए ,

Dernière mise à jour : 2020-05-24
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Anglais

sars-cov and mers-cov can survive in vitro for 48 hours in a dry environment and up to 5 days under 20 °c and 40%-50% humidity.

Hindi

sars-cov और mers-cov कृत्रिम परिवेशीय शुष्क वातावरण में 48 घंटे और 20 °c से कम और 40%-50% आद्रता पर 5 दिन तक जीवित रह सकता है।

Dernière mise à jour : 2020-08-25
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Anglais

inputs and services - soil health : good quality seeds , disease free planting material , including in - vitro cultured propagules and soil health enhancement hold the key to raising small farm productivity .

Hindi

भूमि की देखभाल हेतु सेवाएँ और निवेश - अच्छी गुणवत्ता के बीज , रोगमुक्त रोपण सामग्री - जिसमें हरित गृह में उगाए बीज - और मिट्टी की गुणवत्ता को बढ़ाकर छोटे खेतों की उत्पादकता बढ़ाई जाएगी ।

Dernière mise à jour : 2020-05-24
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Anglais

duchenne muscular dystrophy, a severe type of muscle weakness that usually begins at an early age and worsens quickly, may soon have a new strategy of treatment through genetic regulation. there is no known cure for duchenne muscular dystrophy. treatments usually aim to control symptoms to improve quality of life. sandeep eswarappa, assistant professor indian institute of science (iisc), bengaluru one of the 21 recipients of this year’s swarnajayanti fellowship of the department of science and technology (dst), government of india proposes to supress the disease-causing premature stop codon or the genetic process that initiates these diseases. he is trying to bring about the suppression through translational readthrough, a gene regulatory principle found in humans, yeasts, bacteria and drosophila which takes place with the variation of the genetic code. prof. sandeep’s group has been developing strategies to induce translational readthrough across genetic diseases caused by non-sense mutations --a change in dna that causes a protein to terminate or end its translation earlier than expected. they were successful in achieving this in vitro in case of thalassemia and are working on other disease models. this research work has been published in the scientific journal ‘biochemistry’ recently. with the swarna jayanti fellowship, they will extend it to duchenne muscular dystrophy. if successful, this project may lead to novel therapeutics for the treatment of genetic diseases like thalassemia, duchenne muscular dystrophy, haemophilia. in case of any protein formation genetic information present in the genome is first transcribed into an mrna, which in turn is translated into a protein. protein synthesis or translation is executed by macromolecular machinery called ribosomes. ribosomes start this process at a specific location on an mrna called ‘start codon’ and terminate at a stop signal called ‘stop codon’. in case of diseases with nonsense mutations, such mutations result in premature stop signal in mrna often resulting in non-functional truncated protein. prof. sandeep eswarappa’s laboratory at iisc has shown that in certain mrnas, under certain conditions, translating ribosomes misread the stop signal and continue till they encounter another stop signal. in this translational readthrough process, a longer protein is synthesized with an extension. this extension might change the properties of the protein. the experiments carried out by his group have revealed that such long proteins can have different localization, stability and function. “the knowledge we have already gained from our experiment have opened an unexpected avenue to treat genetic diseases caused by non-sense mutations like duchenne muscular dystrophy, haemophilia and so on,” said prof. sandeep.

Hindi

duchenne muscular dystrophy, a severe type of muscle weakness that usually begins at an early age and worsens quickly, may soon have a new strategy of treatment through genetic regulation. there is no known cure for duchenne muscular dystrophy. treatments usually aim to control symptoms to improve quality of life. sandeep eswarappa, assistant professor indian institute of science (iisc), bengaluru one of the 21 recipients of this year’s swarnajayanti fellowship of the department of science and technology (dst), government of india proposes to supress the disease-causing premature stop codon or the genetic process that initiates these diseases. he is trying to bring about the suppression through translational readthrough, a gene regulatory principle found in humans, yeasts, bacteria and drosophila which takes place with the variation of the genetic code. prof. sandeep’s group has been developing strategies to induce translational readthrough across genetic diseases caused by non-sense mutations --a change in dna that causes a protein to terminate or end its translation earlier than expected. they were successful in achieving this in vitro in case of thalassemia and are working on other disease models. this research work has been published in the scientific journal ‘biochemistry’ recently. with the swarna jayanti fellowship, they will extend it to duchenne muscular dystrophy. if successful, this project may lead to novel therapeutics for the treatment of genetic diseases like thalassemia, duchenne muscular dystrophy, haemophilia. in case of any protein formation genetic information present in the genome is first transcribed into an mrna, which in turn is translated into a protein. protein synthesis or translation is executed by macromolecular machinery called ribosomes. ribosomes start this process at a specific location on an mrna called ‘start codon’ and terminate at a stop signal called ‘stop codon’. in case of diseases with nonsense mutations, such mutations result in premature stop signal in mrna often resulting in non-functional truncated protein. prof. sandeep eswarappa’s laboratory at iisc has shown that in certain mrnas, under certain conditions, translating ribosomes misread the stop signal and continue till they encounter another stop signal. in this translational readthrough process, a longer protein is synthesized with an extension. this extension might change the properties of the protein. the experiments carried out by his group have revealed that such long prote “the knowledge we have already gained from our experiment have opened an unexpected avenue to treat genetic diseases caused by non-sense mutations like duchenne muscular dystrophy, haemophilia and so on,” said prof. sandeep.

Dernière mise à jour : 2021-03-15
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