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Sex can put men at heart attack

The study which has been led by an Indian-origin researcher has revealed that although the incidence of sudden cardiac arrest is very rare, survival rates in such cases remain low.
Sex can put men at heart attack risk

New Delhi: A new study says that men having a history of cardiovascular disease may be at more risk of facing a sudden cardiac arrest during or after having sex, says a study.
The study which has been led by an Indian-origin researcher has revealed that although the incidence of sudden cardiac arrest is very rare, survival rates in such cases remain low.
It is because, the partners failed to immediately perform cardiopulmonary resuscitation (CPR), which could save more lives, the researchers said.
"Even though SCA during sexual activity was witnessed by a partner, bystander CPR was performed in only one-third of the cases," said Sumeet Chugh, Associate Director at the Cedars-Sinai Heart Institute. 
For the study, published in the Journal of the American College of Cardiology, the team examined records of more than 4,500 cardiac arrests over a period of 13 years in persons above 18 years. 
Out of these only 34 were during or within an hour of having sex, and 32 of those were men, who were already taking drugs for heart conditions.
Patients who experienced sudden cardiac arrest related to sexual activity also had a higher rate of ventricular fibrillation/tachycardia than those who did not.
Only one-third of these SCA cases received bystander CPR. This low bystander CPR rate accounted for less than 20 per cent of patients who survived to hospital discharge, the researchers noted.
Moreover, some cases of SCA after sexual activity may also involve medications, stimulants and alcohol use, the researchers said.
"These findings highlight the importance of continued efforts to educate the public on the importance of bystander CPR for SCA, irrespective of the circumstance," Chugh added.

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Did Sanofi, WHO ignore warning signals on dengue vaccine?

CHICAGO/LONDON: When French drugmaker Sanofi published the results of clinical trials of children given its dengue vaccine two years ago, the overall findings were that it protected against the world’s biggest and fastest growing mosquito-borne disease.
But the trial also showed that in the third year after receiving the Dengvaxia inoculation, younger children were more likely to end up in hospital with a severe case of dengue than those who didn’t get the vaccine.
The study’s authors cited two main possibilities: the children had immature immune systems that made the vaccine less protective, or the vaccine itself made them more susceptible to severe disease if they had never had dengue and later became infected.More than two years later, it turns out the latter was the primary factor – a revelation at the end of last month that has triggered alarm among hundreds of thousands of anxious parents in the Philippines, where the vaccine has been given to over 830,000 children.
It has also torpedoed initial expectations by analysts and the company that Dengvaxia, the first dengue vaccine to be developed, might become a $1 billion-a-year blockbuster product. Sanofi says it will take a charge of around 100 million euros ($118 million) for the fourth quarter.
Initially, to address the issue seen in younger children, Sanofi had recommended that the vaccine only be given to those aged 9 and older in areas where the disease was widespread. The World Health Organisation analyzed Sanofi’s data and came to the same conclusion. It made a conditional recommendation to use the vaccine.
But after a new analysis of data from the trials, Sanofi confirmed last month the vaccine could increase the risk of severe dengue in some cases in people who had not been previously exposed to the disease. The WHO has now backed a decision by the Philippines government to suspend a mass immunization program and said it has begun reviewing safety data.
In Sanofi’s large-scale trials, blood samples were not collected from all the children before they were vaccinated, which would have identified prior exposure to the disease by showing the presence of antibodies.
“The development process around the first dengue vaccine led to a degree of momentum and judgments being made that we should learn lessons from,” Neil Ferguson, a professor at Imperial College London and an unpaid adviser to both Sanofi and the WHO, told Reuters.
The case raises questions whether Sanofi and the WHO, in their pursuit of a new weapon to fight a deadly disease, should have foreseen the risk. Their decisions on how the vaccine was rolled out could set back efforts to combat dengue by a generation, some disease experts say.
REJECTED SUGGESTIONS
Sanofi has rejected suggestions it ignored any risks or took any short-cuts. However, it has acknowledged that clinical tests of the vaccine did not fully investigate whether a previous dengue infection could influence the outcome.
”When you are the first in class, we’re the ones having to develop and understand the science as we go,“ said Dr. Su-Peing Ng, the global medical head of Sanofi Pasteur, the vaccines division of the drugmaker. ”We don’t have another vaccine to follow the lead on.
“The findings we have today, we would have loved to have (earlier),” she told Reuters. “Now that we have these findings, of course it’s our responsibility again to … share this information.”
The protocols for the tests, devised in 2009, were “thoroughly vetted by many dengue experts, including with WHO’s technical advisory group and various regulators”, Ng added.
The WHO said it acted promptly to address concerns when they arose. It has also said its recommendations on use of Dengvaxia were conditional and confined to children aged 9 and older in areas where dengue was endemic.
Complicating matters, scientists were sharply divided about the risks of the vaccine.
Four decades ago, Dr. Scott Halstead, a leading figure in dengue research, first proposed that antibodies from an initial exposure to one of four types of the disease could increase the risk of a potentially lethal complication called severe dengue when a person was infected a second time, a process know as antibody-dependent enhancement or ADE.
This phenomenon could make development of a dengue vaccine tricky.
Rather than being protective, a shot given to someone who had never had dengue could act like a first infection, increasing their risk of severe dengue when they were exposed a second time.
Halstead, an adjunct professor at the Uniformed Services University of the Health Sciences in Bethesda, Maryland, said when he saw Sanofi’s 2015 paper, he was convinced the increased risk that some children would contract severe dengue was evidence of ADE.
Halstead wrote a series of papers published in Vaccine, the Journal of Infectious Diseases and other journals urging Sanofi and the WHO to proceed with caution in rolling out the vaccine. “It was not obvious to Sanofi and the World Health Organization, but it was obvious to me,” he told Reuters.
CONDITIONAL GUIDANCE
Dr. Joachim Hombach, senior health adviser in WHO’s vaccine department, said he understood Halstead’s concerns but the organization could only work with data generated by research.
He told Reuters that WHO “strongly encouraged” Sanofi to conduct follow-up studies to clarify whether children who had never had dengue before being vaccinated were more prone to severe dengue.
“It was recognized it was something that would be important to follow as part of our long-term program,” said Sanofi’s Ng. “This is exactly what we’ve done with our recent analysis.”
In the end, WHO issued its conditional guidance on Dengvaxia in July, 2016, after a year of deliberations, favoring use of the vaccine only in countries with a high burden of dengue, and stipulated that it only be given to children aged 9 and older.
Ferguson, at Imperial College, also raised concerns about the vaccine in a paper published in the journal Science in September 2016, suggesting the vaccine could increase severe dengue in some places with low transmission of dengue.
But until last month, many other scientists were on the fence about whether the signals in Sanofi’s trials were evidence of true ADE.
“I‘m not sure it was nailed down until now,” Jeremy Farrar, director of the Wellcome Trust medical charity who has served on WHO’s working group on dengue vaccines, told Reuters.
A paper in PLOS Medicine in November 2016 described a “split” among dengue experts between those like Farrar who supported the WHO recommendations on cautious use of Dengvaxia and those such as Halstead who said it was too risky.
To do the follow-up study, Sanofi had to solve a major problem. The company said it had only collected blood samples that would have revealed prior exposure to dengue in 10 percent of the more than 30,000 children in its clinical trials before they had been vaccinated.
Sanofi did have blood samples from nearly all of the children but only after they had been vaccinated. So it would be hard to tell from those samples whether the antibodies in their blood were produced in response to a natural dengue infection or the vaccine itself.
Responding to questions from Reuters, the company said in an email it would have been considered ‘unethical’ to take blood samples from all the kids prior to vaccination, because there wasn’t a clear reason to do so when it set up the protocols for the trial.
SHEER MOMENTUM
In 2014, Sanofi had entered into a scientific collaboration with the University of Pittsburgh Center for Vaccine Research to measure responses to the vaccine in its trials. At the time, the company had no reason to suspect that the vaccine would increase risks in children who had never had dengue, Ng said, but this test ultimately proved critical in allowing the company to differentiate those who had been infected before vaccination from those who had not.
That test only became ready to use this past July, said Dr. Ernesto Marques, an infectious disease specialist at the University of Pittsburgh, who helped develop the test.
Sanofi used the test to re-analyze blood samples collected in its trials and alerted public health officials last month that there was an increased risk of severe dengue in people who had not been previously infected, even among the children 9 and older who had been recommended for the vaccine.
By the time Sanofi announced findings from its follow-up study at the end of last month, the vaccine had been given to over 830,000 children in the Philippines, and about 300,000 people in Brazil.
One factor in decision-making was the sheer momentum behind the project, said Ferguson, the unpaid adviser, referring to the surge in the incidence of dengue and the fact that Dengvaxia was the first vaccine developed to contain the disease.
The WHO says dengue is now endemic in more than 100 countries, up from 9 countries before 1970. An estimated half a million people suffering from dengue require hospitalization each year and about 12,500 die.
“Clearly, in retrospect, it was a mistake” not to have taken baseline blood samples, said Ferguson, “The question is, could it (the need to do so) have been anticipated?

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Kapilakō śō banda garēra sōnīlē sunilalā'ī chuṭṭai śō sañcālana garna dinē

Ējēnsī. Bhāratiya kamēḍiyana bādasāhakāē upanāma pā'ukā kapila sarmā ra śunila grāēbharabica bivāda bha'ēpachi sāēnī cyānalalē da kapila śarmā sāē banda garna saknē ra śunila grāēbharalār'i arkai kāryakrā sañcālana garna dinē tayārī thālēkāē bhāratiya sañcāramādhyamaharūlē janā'ēkā chana.
Kapilakai kāraṇa sāēnī cyānalalē 107 karōḍa bhāru nāēksāna byavahāēranū parirahēkāē kāraṇa cyānalakāē ṭia̔ārapī pani ghaṭēkāē ra kapilamāthī kunaipani bēlā ēksana lina saknē bhāratiya sañcāramādhyamaharūlē janā'ēkā chana.
Sōnīlē kapilakō śōkō saṭṭā sunila grōbharalā'ī āphnai śō dinasaknē pani batā'i'ēkō cha. Sunila ra kapilakō vivāda baḍhēpachi sōnīkō pratispardhī cyānala kalarsalē sunilasaṅga samparka garēkō batā'i'ēkō cha. Tara kalarsasaṅga sunilalē kunai samjhautā garēkā chainan.x

Yī huna mahilākā 10 guṇa jasalē parivāralā'ī samr̥d'dha banā'ucha

Prācina hindu sanskāramā mahilākō 32 lakṣaṇakō parikalpanā gari'ēkō cha. 32 Lakṣaṇalē yukta mahilālā'ī pūrṇa guṇī, sanskārī mānincha. Mānisamā rāmrō/narāmrō dubai guṇa huncha. Sabai rāmrō guṇalē bharipūrṇa huncha bhannē chaina. Yadyapī kēhi rāmrō svabhāva ra vyavahāralē pani mānisalā'ī unnata banā'um̐cha. Unīharukō svabhāva, satkarma, satbicāralē parivāralā'ī samr̥d'dha tulyā'um̐cha.1. Ēka yastō mahilā jō āphnā pati barābara hunchan. Parivāramā unakō upasthitī ahamma huncha. Unalē śālina vyaktitva nirmāṇa garēkī hunchin. Parivāra ēvaṁ patīprati śrad'dhābhāva rākhchan.2. Tī mahilā, jō sānsārika ghaṭanākō bārēmā jānakārī rākhchin. Unī bud'dhimāna ra śikṣita hunchin.3. Tī mahilā, jō āsapāsakā māhaulamā satarka rahanchan. Sabaisam̐ga samāna ra sauhārdapūrṇa vyavahāra garchin.4. Tī mahilā, jō dharmalā'ī sam'māna garchin. Sāmājika dāyitva pani bōdha garchin.5. Tī mahilā, jō hiphājata ēvaṁ jatana garnē svabhāvakā hunchan. Bacata garēra gharalā'ī ārthika rupalē samr̥d'dha banā'una sahayōga garchin.6. Tī mahilā, jō āphnō parivāramā ā'iparnē saṅkaṭabāṭa pāra lagā'una harasambhava prayāsa garchin. Ucita samayamā ucita nirṇaya ēvaṁ sallāha dinchan.7. Tī mahilā, jō ēkadamai dhairyavāna hunchin. Pratikula paristhitīmā pani āphulā'ī samhālna sakchin.8. Tī mahilā, jō sabailā'ī prēmapūrvaka vyavahāra garchin.9. Tī mahilā, jō āphubhandā ṭhūlākō sam'māna garchin, unīharukō sarasallāha linchin.10. Tī mahilā, jasalā'ī pākakalākō rāmrō jñāna cha.Tapā'īmā yō guṇa cha? Chaina bhanē āja dēkhi nai sudhārnusa1. Ēka yastō mahilā jō āphnā pati barābara hunchan. Parivāramā unakō upasthitī ahamma huncha. Unalē śālina vyaktitva nirmāṇa garēkī hunchin. Parivāra ēvaṁ patīprati śrad'dhābhāva rākhchan.2. Tī mahilā, jō sānsārika ghaṭanākō bārēmā jānakārī rākhchin. Unī bud'dhimāna ra śikṣita hunchin.3. Tī mahilā, jō āsapāsakā māhaulamā satarka rahanchan. Sabaisam̐ga samāna ra sauhārdapūrṇa vyavahāra garchin.4. Tī mahilā, jō dharmalā'ī sam'māna garchin. Sāmājika dāyitva pani bōdha garchin.5. Tī mahilā, jō hiphājata ēvaṁ jatana garnē svabhāvakā hunchan. Bacata garēra gharalā'ī ārthika rupalē samr̥d'dha banā'una sahayōga garchin.6. Tī mahilā, jō āphnō parivāramā ā'iparnē saṅkaṭabāṭa pāra lagā'una harasambhava prayāsa garchin. Ucita samayamā ucita nirṇaya ēvaṁ sallāha dinchan.7. Tī mahilā, jō ēkadamai dhairyavāna hunchin. Pratikula paristhitīmā pani āphulā'ī samhālna sakchin.8. Tī mahilā, jō sabailā'ī prēmapūrvaka vyavahāra garchin.9. Tī mahilā, jō āphubhandā ṭhūlākō sam'māna garchin, unīharukō sarasallāha linchin.10. Tī mahilā, jasalā'ī pākakalākō rāmrō jñāna cha.Tapā'īmā yō guṇa cha? Chaina bhanē āja dēkhi nai sudhārnusa

Lōḍasēḍiṅa antyakō vāstavikatā aba philmamā (bhiḍiyō)

Lōḍasēḍiṅamukta dēśa banā'unē abhiyānakō kathāvastumā kēndrita calacitra ‘ujyālō nēpāla’ nirmāṇa bha'ēkō cha. Lōḍasēḍiṅa antyakā lāgi bha'ēkā prayāsa ra upalabdhīlā'ī samēṭēra calacitra ‘ujyālō nēpāla’ nirmāṇa bha'ēkō hō. Urjāmantrī bha'ēpachi jarnādana śarmālē linubha'ēkō aṭhōṭa ra vidyuta prādhikaraṇakō kāryakārī nirdēśakamā kulamāna ghisiṅa niyukta gari'ēpachikō parirvatanalā'ī calacitramā dēkhā'i'ēkō cha.

Unīharukō icchāśaktikā kāraṇa urjā kṣētramā ā'ēkō nāṭakīya parirvatana ra sakārātmaka prabhāvalā'ī calacitramā citrita gari'ēkō cha. Calacitralē vidyuta utpādana baḍhā'ēra dēśa ujyālō banā'unē mantrī śarmākō aṭhōṭa ra vidyutakō ucita vyavasthāpanamā kulamāna ghisiṅalē dēkhā'ēkō kuśalatālā'ī prasṭa garēkō cha.

Mahānāyaka rājēśa hamāla ‘ujyālō nēpāla’ calacitramā mantrīkō bhūmikāmā dēkhi'ēkā chan bhanē pā'ilaṭa vijaya lāmā prādhikaraṇa kāryakārī nirdēśakakō rupamā dēkhi'ēkā chan. Calacitramā vidyuta vikāsamā dēkhi'ēkā samasyā ra cāli'ēkā kadamaharulā'ī pani dēkhā'una khōjī'ēkō cha.

Śubha miḍiyā hōma prā.Lilē nirmāṇa garēkō yasa calacitramā abhiman'yu niravīkō kathā rahēkō cha. Sarōja ōlīkō nirdēśana rahēkō calacitramā rājēśa hamāla, vijaya lāmāsam̐gai gaurī malla, arjuna śrēṣṭha, namratā sāpakōṭā, nirmala śarmā, kēśava bhaṭṭarā'ī, rabi śarmā, vinōda rā'ī, viṣṇu buḍhāthōkīlagāyatakā kalākārakō abhinaya cha. Nēpāla ṭēlibhijanamā prasāraṇa bha'isakēkō calacitra ‘ujyālō nēpāla’ yuṭyubamā pani sārvajanika gari'ēkō cha.


Yemale seven recommendations, the team choosing candidates

SOLUKHUMBU. CPN (UML) held Solu dudhakunda municipality mayor nominee has recommended seven names. City Organization Committee meeting on Thursday for the upcoming local level elections anadami Sherpa, Dak ranapala, janbu Lama Dorji, Bachchunarayan best, viraudasa best, Kaji Shrestha and Santosh Magar recommended Publicity Department chief viraudasa Shrestha said.Meanwhile, the name of the district committee meeting failed to decide on the name of the state Assembly has decided to send hanged. The municipality deputy Rai fiction, mohanakumari Karki, suryakumari Sunuwar and yandi Lama Pradesh Assembly has recommended.Solu dudhakunda Municipality Mayor verse CPN (Maoist Center) has already nimatendupa Lama mayor candidate has already announced that the Nepalese kamgresalagayata other parties have not been able yet to select the candidates.CPN (UML) has been finalized so far, the district's nominee to head the three gaumpalikako. The party chief likhupike gaumpalikako postakumara Karki, Khumbu Sherpa and Dudhkoshi gaumpalikama sicne gaumpalikama nimadorji buddhikirana Rai has made major official candidate.Similarly, the CPN (Maoist Center) has Solu Sherpa nimatendupa dudhakunda municipality, Dudhkoshi gaumpalikama nab Rai, dudhakausika gaumpalikama asima Rai Bahadur Basnet and likhupike gaumpalikako chief has already announced major official candidate.Other local level, if one has not been able to decide on a candidate. Now the parties have reached the final stage candidate selection is described. Ward head of the local government and many aspirants as the head of the Nepali Congress and the CPN (UML) has been reported to have been difficult to choose a candidate.

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