Your search keyword '"K. Sathiyanarayanan"' showing total 29 results

1. Active versus passive case finding for tuberculosis in marginalised and vulnerable populations in India: comparison of treatment outcomes

Author

Hemant Deepak Shewade, Vivek Gupta, Srinath Satyanarayana, Sunil Kumar, Prabhat Pandey, U. N. Bajpai, Jaya Prasad Tripathy, Soundappan Kathirvel, Sripriya Pandurangan, Subrat Mohanty, Vaibhav Haribhau Ghule, Karuna D. Sagili, Banuru Muralidhara Prasad, Priyanka Singh, Kamlesh Singh, Gurukartick Jayaraman, P. Rajeswaran, Moumita Biswas, Gayadhar Mallick, Ali Jafar Naqvi, Ashwin Kumar Bharadwaj, K. Sathiyanarayanan, Aniruddha Pathak, Nisha Mohan, Raghuram Rao, Ajay M. V. Kumar, and Sarabjit Singh Chadha

Subjects

tuberculosis/therapy, systematic screening, vulnerable populations, treatment outcome, community-based active case finding, Public aspects of medicine, RA1-1270

Abstract

Background: Community-based active case finding (ACF) for tuberculosis (TB) implemented among marginalised and vulnerable populations in 285 districts of India resulted in reduction of diagnosis delay and prevalence of catastrophic costs due to TB diagnosis. We were interested to know whether this translated into improved treatment outcomes. Globally, there is limited published literature from marginalised and vulnerable populations on the independent effect of community-based ACF on treatment outcomes when compared to passive case finding (PCF). Objectives: To determine the relative differences in unfavourable treatment outcomes (death, loss-to-follow-up, failure, not evaluated) of ACF and PCF-diagnosed people. Methods: Cohort study involving record reviews and interviews in 18 randomly selected districts. We enrolled all ACF-diagnosed people with new smear-positive pulmonary TB, registered under the national TB programme between March 2016 and February 2017, and an equal number of randomly selected PCF-diagnosed people in the same settings. We used log binomial models to adjust for confounders. Results: Of 572 enrolled, 275 belonged to the ACF and 297 to the PCF group. The proportion of unfavourable outcomes were 10.2% (95% CI: 7.1%, 14.3%) in the ACF and 12.5% (95% CI: 9.2%, 16.7%) in the PCF group (p = 0.468). The association between ACF and unfavourable outcomes remained non-significant after adjusting for confounders available from records [aRR: 0.83 (95% CI: 0.56, 1.21)]. Due to patient non-availability at their residence, interviews were conducted for 465 (81.3%). In the 465 cohort too, there was no association after adjusting for confounders from records and interviews [aRR: 1.05 (95% CI: 0.62, 1.77)]. Conclusion: We did not find significant differences in the treatment outcomes. Due to the wide CIs, studies with larger sample sizes are urgently required. Studies are required to understand how to translate the benefits of ACF to improved treatment outcomes.

Published

2019

2. Active case finding among marginalised and vulnerable populations reduces catastrophic costs due to tuberculosis diagnosis

Author

Hemant Deepak Shewade, Vivek Gupta, Srinath Satyanarayana, Atul Kharate, K.N. Sahai, Lakshmi Murali, Sanjeev Kamble, Madhav Deshpande, Naresh Kumar, Sunil Kumar, Prabhat Pandey, U.N. Bajpai, Jaya Prasad Tripathy, Soundappan Kathirvel, Sripriya Pandurangan, Subrat Mohanty, Vaibhav Haribhau Ghule, Karuna D. Sagili, Banuru Muralidhara Prasad, Sudhi Nath, Priyanka Singh, Kamlesh Singh, Ramesh Singh, Gurukartick Jayaraman, P. Rajeswaran, Binod Kumar Srivastava, Moumita Biswas, Gayadhar Mallick, Om Prakash Bera, A. James Jeyakumar Jaisingh, Ali Jafar Naqvi, Prafulla Verma, Mohammed Salauddin Ansari, Prafulla C. Mishra, G. Sumesh, Sanjeeb Barik, Vijesh Mathew, Manas Ranjan Singh Lohar, Chandrashekhar S. Gaurkhede, Ganesh Parate, Sharifa Yasin Bale, Ishwar Koli, Ashwin Kumar Bharadwaj, G. Venkatraman, K. Sathiyanarayanan, Jinesh Lal, Ashwini Kumar Sharma, Raghuram Rao, Ajay M.V. Kumar, and Sarabjit Singh Chadha

Subjects

tuberculosis/prevention and control, systematic screening, vulnerable populations, health care costs, health equity, Public aspects of medicine, RA1-1270

Abstract

Background: There is limited evidence on whether active case finding (ACF) among marginalised and vulnerable populations mitigates the financial burden during tuberculosis (TB) diagnosis. Objectives: To determine the effect of ACF among marginalised and vulnerable populations on prevalence and inequity of catastrophic costs due to TB diagnosis among TB-affected households when compared with passive case finding (PCF). Methods: In 18 randomly sampled ACF districts in India, during March 2016 to February 2017, we enrolled all new sputum-smear-positive TB patients detected through ACF and an equal number of randomly selected patients detected through PCF. Direct (medical and non-medical) and indirect costs due to TB diagnosis were collected through patient interviews at their residence. We defined costs due to TB diagnosis as ‘catastrophic’ if the total costs (direct and indirect) due to TB diagnosis exceeded 20% of annual pre-TB household income. We used concentration curves and indices to assess the extent of inequity. Results: When compared with patients detected through PCF (n = 231), ACF patients (n = 234) incurred lower median total costs (US$ 4.6 and 20.4, p

Published

2018

3. 1-Methoxy-4-({[(4-methoxyphenyl)sulfanyl](phenyl)methyl}sulfanyl)benzene

Author

R. S. Rathore, M. Sathishkumar, Hongqi Li, G. Ramachandran, and K. Sathiyanarayanan

Subjects

Crystallography, QD901-999

Abstract

The title compound, C21H20O2S2, forms a propeller-shaped structure with the tetrahedral C atom as the central hub and methoxybenzene and phenyl residues as radiating blades. Short C—H...π contacts are observed.

Published

2012

4. 1,1′-[(2-Bromophenyl)methylene]dipyrrolidin-2-one

Author

K. Sathiyanarayanan, R. S. Rathore, V. Satheesh, Hong-Qi Li, and G. Ramachandran

Subjects

Crystallography, QD901-999

Abstract

In the title compound, C15H17BrN2O2, both pyrrolidinone rings adopt envelope conformations. The crystal packing is characterized by short C—Br...O=C interactions [Br...O = 3.1730 (13) Å], leading to supramolecular dimers. Intermolecular C—H...O and C—H...π interactions are also observed.

Published

2012

5. 3-(7,8,13,14-Tetrahydrodibenzo[a,i]phenanthridin-5-yl)benzene-1,2-diol

Author

N. S. Karthikeyan, G. Ramachandran, K. Sathiyanarayanan, P. Raghavaiah, and R. S. Rathore

Subjects

Crystallography, QD901-999

Abstract

In the title compound, C27H21NO2, the half-chair conformation of the alicyclic rings gives rise to a slightly folded structure of the central tricyclic tetrahydrophenanthridine unit. Tandem intramolecular O—H...N and O—H...O hydrogen bonds give rise to adjacent S(6) and S(5) rings, respectively, which dictate the conformation of the 5-aryl substituent. In the crystal structure, an intermolecular C—H...O contact generates chains parallel to [101]. Short O—H...π and C—H...π contacts are also observed.

Published

2010

6. (7E)-5-Benzyl-7-(2-chlorobenzylidene)-3-(2-chlorophenyl)-2-phenyl-3,3a,4,5,6,7-hexahydro-2H-pyrazolo[4,3-c]pyridine

Author

N. S. Karthikeyan, B. Uma Mahesh, K. Sathiyanarayanan, P. Raghavaiah, and R. S. Rathore

Subjects

Crystallography, QD901-999

Abstract

In the title 2H-pyrazolo[4,3-c]pyridine derivative, C32H27Cl2N3, the dihydropyrazole ring adopts an envelope conformation and the piperidine fused ring a twisted-chair conformation. Two short intramolecular C—H...Cl contacts are observed. The crystal packing is characterized by dimeric C—Cl...π interactions involving the 5-benzyl ring, with Cl...centroid and closest atomic Cl...π distances of 3.778 (2) and 3.366 (4) Å, respectively.

Published

2010

7. (3E,5E)-3,5-Bis(4-allyloxybenzylidene)-1-benzylpiperidin-4-one

Author

R. S. Rathore, H. Ghosh, P. G. Aravindan, N. S. Karthikeyan, and K. Sathiyanarayanan

Subjects

Crystallography, QD901-999

Abstract

In the title compound C32H31NO3, the allyloxy groups on either side of the piperidin-4-one ring are conformationally disordered. The contribution of major and minor components of the allyloxy group at the 3rd position of the ring are 0.576 (4) and 0.424 (4), respectively, and those at the 5th position are 0.885 (3) and 0.115 (3), respectively. The six-membered piperidin-4-one ring adopts a sofa conformation with the benzyl group occupying an equatorial position and the olefinic double bonds possessing an E configuration. Flanking phenyl substituents are stretched out on either side of the six-membered ring. π–π interactions with a centroid–centroid distance of 3.885 (1) Å give rise to molecular dimers and short C—H...π contacts lead to chains along the c axis.

Published

2009

8. (3E,5E)-1-Benzyl-3,5-bis(2-fluorobenzylidene)piperidin-4-one

Author

R. S. Rathore, N. S. Karthikeyan, K. Sathiyanarayanan, and P. G. Aravindan

Subjects

Crystallography, QD901-999

Abstract

The inversion-related molecules of the title compound, C26H21F2NO, associate into closed dimeric subunits via co-operative C—H...π interactions. Two non-classical C—H...O and one C—H...N intramolecular hydrogen bonds are also found in the crystal structure. The piperidin-4-one ring adopts a sofa conforamtion with the 1-benzyl group in the equatorial position, and the equiplanar fluorophenyl substituents in the 3- and 5-positions stretched out on either side. The 1-benzyl group is disposed towards the substituent in the 6th position of the piperidin-4-one ring. The 3,5-diene units possess E configurations.

Published

2009

9. (3E,5E)-1-Benzyl-3,5-dibenzylidenepiperidin-4-one

Author

N. S. Karthikeyan, K. Sathiyanarayanan, P. G. Aravindan, and R. S. Rathore

Subjects

Crystallography, QD901-999

Abstract

In the title compound, C26H23NO, C—H...O hydrogen bonds generate a ribbon structure along the a axis. These ribbons further assemble into a one-dimensional sheet parallel to the ac plane via C—H...π interactions. The piperidin-4-one ring adopts a sofa conformation with the 1-benzyl group in the equatorial position, and the 3- and 5-phenyl substituents stretched out on either side. The benzylidene units adopt E configurations and the 1-benzyl group is disposed towards the 3- substituent of the piperidin-4-one ring.

Published

2009

10. 2,3-Bis[(2-methylphenoxy)methyl]buta-1,3-diene

Author

K. Sathiyanarayanan, A. George Fernand, V. Dhanasekaran, and R. S. Rathore

Subjects

Crystallography, QD901-999

Abstract

The molecule of the title compound, C20H22O2, a symmetrically 2-methylphenol-substituted divinyl analog, exhibits crystallographically imposed C2 symmetry. The molecular structure is essentially planar. The structure is stabilized by a short intermolecular C—H...O contact. Cooperative C—H...π interactions generate an infinite one-dimensional chain of molecules along the a axis.

Published

2008

11. 2,3-Bis(phenoxymethyl)buta-1,3-diene

Author

K. Sathiyanarayanan, A. George Fernand, V. Dhanasekaran, and R. S. Rathore

Subjects

Crystallography, QD901-999

Abstract

The molecule of the title compound, C18H18O2, a symmetrically phenol-substituted divinyl analog, exhibits crystallographically imposed C2 symmetry. The phenolic and divinyl planar groups intersect each other orthogonally, with a dihedral angle of 82.7 (1)°. The structure is stabilized by a short intramolecular C—H...O contact. The molecules are held together by C—H...π interactions, forming a sheet structure parallel to the (201) plane.

Published

2008

12. Are we missing ‘previously treated’ smear-positive pulmonary tuberculosis under programme settings in India? A cross-sectional study [version 2; peer review: 1 approved, 2 approved with reservations]

Author

Hemant Deepak Shewade, Vivek Gupta, Srinath Satyanarayana, Atul Kharate, Lakshmi Murali, Madhav Deshpande, Naresh Kumar, Prabhat Pandey, U N Bajpai, Jaya Prasad Tripathy, Soundappan Kathirvel, Sripriya Pandurangan, Subrat Mohanty, Vaibhav Haribhau Ghule, Karuna D Sagili, Banuru Muralidhara Prasad, Sudhi Nath, Priyanka Singh, Kamlesh Singh, Gurukartick Jayaraman, P Rajeswaran, Binod Kumar Srivastava, Moumita Biswas, Gayadhar Mallick, Om Prakash Bera, A James Jeyakumar Jaisingh, Ali Jafar Naqvi, Prafulla Verma, Mohammed Salauddin Ansari, Prafulla C Mishra, G Sumesh, Sanjeeb Barik, Vijesh Mathew, Manas Ranjan Singh Lohar, Chandrashekhar S Gaurkhede, Ganesh Parate, Sharifa Yasin Bale, Ishwar Koli, Ashwin Kumar Bharadwaj, G Venkatraman, K Sathiyanarayanan, Jinesh Lal, Ashwini Kumar Sharma, Ajay MV Kumar, and Sarabjit S Chadha

Subjects

lcsh:R, lcsh:Medicine, lcsh:Q, lcsh:Science

Abstract

Background: In 2007, a field observation from India reported 11% misclassification among ‘new’ patients registered under the revised national tuberculosis (TB) control programme. Ten years down the line, it is important to know what proportion of newly registered patients has a past history of TB treatment for at least one month (henceforth called ‘misclassification’). Methods: A study was conducted among new smear-positive pulmonary TB patients registered between March 2016 and February 2017 in 18 randomly selected districts to determine the effectiveness of an active case-finding strategy in marginalised and vulnerable populations. We included all patients detected through active case-finding. An equal number of randomly selected patients registered through passive case-finding from marginalised and vulnerable populations in the same districts were included. Before enrolment, we enquired about any history of previous TB treatment through interviews. Results: Of 629 patients, we interviewed 521, of whom, 11% (n=56) had past history of TB treatment (public or private) for at least a month: 13% (34/268) among the active case-finding group and 9% (22/253) among the passive case-finding group (p=0.18). No factors were found to be significantly associated with misclassification. Conclusion: Around one in every ten patients registered as ‘new’ had previous history of TB treatment. Corrective measures need to be implemented, followed by monitoring of any change in the proportion of ‘previously treated’ patients among all registered patients treated under the programme at national level.

Published

2019

13. Three dimensional conformal radiation therapy in prostate adenocarcinoma: Survival and rectal toxicity

Author

V Kannan, S. Sagde, V. K. Sathiyanarayanan, Vivek Anand, Asha Kapadia, V. Srinivas, and Sachin Almel

Subjects

Male, Prostate adenocarcinoma, medicine.medical_specialty, Conformal radiation therapy, Adenocarcinoma, Conformal Radiation, lcsh:RC254-282, Prostate cancer, Prostate, Doses collection, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Stage (cooking), Pelvis, Aged, Radiotherapy, business.industry, Radiotherapy Planning, Computer-Assisted, Rectal toxicity, Rectum, Prostatic Neoplasms, Radiotherapy Dosage, General Medicine, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Surgery, medicine.anatomical_structure, Oncology, Radiology, business, Progressive disease

Abstract

Technological advances in radiation beam planning and linear accelerator based radiation delivery have led to the development of three dimensional conformal radiation therapy (3D-CRT). The 3D-CRT clinical treatment in our hospital was started in September 1998 and till December 2002, 51 patients with M0 stage prostate carcinoma were treated. Treatment method consisted of pelvis and leg immobilization, planning CT scan, marking of planning target volume and organs at risk and 3D beam plan using multileaf collimated beam shaping through beam′s eye view display. Network controlled 3D conformal radiation therapy was delivered with portal image verification. The median 3D-CRT dose was 72 Gy. Of the 51 patients, 35 were followed-up till December 2002 (minimum follow-up 2 years) in whom 32 were disease free and 3 had progressive disease. Eleven patients died, 8 of progressive disease, one due to second malignancy and two of intercurrent illness. Five patients were lost for follow up during 0 - 29 months period, after 3D-CRT. The acute rectal reaction (RTOG criteria) in 51 patients was grade 0 in 4, grade I in 31 and grade II in 16. None had greater than grade II rectal toxicity. The late rectal toxicity in 49 patients who had a minimum 6 months follow-up was grade 0 in 41, grade I in 3 and grade II in 5. Our experience suggests that a dose of 72 Gy by 3D-CRT can be safely delivered to the prostate and gastrointestinal tolerance during treatment and follow-up period was excellent.

Published

2005

14. Statistical descriptors to measure the effectiveness of hydrogen bonding groups and an example of ether oxygenElectronic supplementary information (ESI) available. ESI contains data for different types of HB groups. See DOI: 10.1039/c1ce05034f.

Author

R. S. Rathore, Y. Alekhya, A. K. Kondapi, and K. Sathiyanarayanan

Subjects

HYDROGEN bonding, ETHER (Anesthetic), OXYGEN, NUMERICAL analysis, PARAMETER estimation, CARBONYL compounds, NITROGEN compounds

Abstract

To quantify the effectiveness of hydrogen-bonding donors and acceptors for forming interactions, we here introduce the concept of statistical competitiveness, defined in terms of three numerical parameters namely, absolute, relative and exclusive statistical competitiveness. The concept can be applied to evaluate the effectiveness of a donor or acceptor in any chemical context. We have evaluated the efficacy of ether oxygen for hydrogen-bonding with respect to carbonyl oxygen and nitrogen acceptors. The quantification in terms of statistical parameters reveals a striking result that the population of hydrogen-bonding groups predominately dictates their effectiveness irrespective of their acidic or basic strengths. The quantification of the competitiveness serves to estimate better the outcome of crystal structure prediction and engineering methodologies, and molecular docking. [ABSTRACT FROM AUTHOR]

Published

2011

15. Patient characteristics, health seeking and delays among new sputum smear positive TB patients identified through active case finding when compared to passive case finding in India.

Author

Hemant Deepak Shewade, Vivek Gupta, Srinath Satyanarayana, Prabhat Pandey, U N Bajpai, Jaya Prasad Tripathy, Soundappan Kathirvel, Sripriya Pandurangan, Subrat Mohanty, Vaibhav Haribhau Ghule, Karuna D Sagili, Banuru Muralidhara Prasad, Sudhi Nath, Priyanka Singh, Kamlesh Singh, Ramesh Singh, Gurukartick Jayaraman, P Rajeswaran, Binod Kumar Srivastava, Moumita Biswas, Gayadhar Mallick, Om Prakash Bera, K N Sahai, Lakshmi Murali, Sanjeev Kamble, Madhav Deshpande, Naresh Kumar, Sunil Kumar, A James Jeyakumar Jaisingh, Ali Jafar Naqvi, Prafulla Verma, Mohammed Salauddin Ansari, Prafulla C Mishra, G Sumesh, Sanjeeb Barik, Vijesh Mathew, Manas Ranjan Singh Lohar, Chandrashekhar S Gaurkhede, Ganesh Parate, Sharifa Yasin Bale, Ishwar Koli, Ashwin Kumar Bharadwaj, G Venkatraman, K Sathiyanarayanan, Jinesh Lal, Ashwini Kumar Sharma, Raghuram Rao, Ajay M V Kumar, and Sarabjit Singh Chadha

Subjects

Medicine, Science

Abstract

BackgroundAxshya SAMVAD is an active tuberculosis (TB) case finding (ACF) strategy under project Axshya (Axshya meaning 'free of TB' and SAMVAD meaning 'conversation') among marginalized and vulnerable populations in 285 districts of India.ObjectivesTo compare patient characteristics, health seeking, delays in diagnosis and treatment initiation among new sputum smear positive TB patients detected through ACF and passive case finding (PCF) under the national TB programme in marginalized and vulnerable populations between March 2016 and February 2017.MethodsThis observational analytic study was conducted in 18 randomly sampled Axshya districts. We enrolled all TB patients detected through ACF and an equal number of randomly selected patients detected through PCF in the same settings. Data on patient characteristics, health seeking and delays were collected through record review and patient interviews (at their residence). Delays included patient level delay (from eligibility for sputum examination to first contact with any health care provider (HCP)), health system level diagnosis delay (from contact with first HCP to TB diagnosis) and treatment initiation delays (from diagnosis to treatment initiation). Total delay was the sum of patient level, health system level diagnosis delay and treatment initiation delays.ResultsWe included 234 ACF-diagnosed and 231 PCF-diagnosed patients. When compared to PCF, ACF patients were relatively older (≥65 years, 14% versus 8%, p = 0.041), had no formal education (57% versus 36%, pConclusionAxshya SAMVAD linked the most impoverished communities to TB care and resulted in reduction of health system level diagnosis delay.

Published

2019

16. Are we missing 'previously treated' smear-positive pulmonary tuberculosis under programme settings in India? A cross-sectional study.

Author

Shewade HD, Gupta V, Satyanarayana S, Kharate A, Murali L, Deshpande M, Kumar N, Pandey P, Bajpai UN, Tripathy JP, Kathirvel S, Pandurangan S, Mohanty S, Ghule VH, Sagili KD, Prasad BM, Nath S, Singh P, Singh K, Jayaraman G, Rajeswaran P, Srivastava BK, Biswas M, Mallick G, Bera OP, Jaisingh AJJ, Naqvi AJ, Verma P, Ansari MS, Mishra PC, Sumesh G, Barik S, Mathew V, Lohar MRS, Gaurkhede CS, Parate G, Bale SY, Koli I, Bharadwaj AK, Venkatraman G, Sathiyanarayanan K, Lal J, Sharma AK, Kumar AM, and Chadha SS

Subjects

Adolescent, Adult, Aged, Cross-Sectional Studies, Female, Humans, India, Male, Middle Aged, Young Adult, Tuberculosis, Pulmonary diagnosis, Tuberculosis, Pulmonary drug therapy

Abstract

Background: In 2007, a field observation from India reported 11% misclassification among 'new' patients registered under the revised national tuberculosis (TB) control programme. Ten years down the line, it is important to know what proportion of newly registered patients has a past history of TB treatment for at least one month (henceforth called 'misclassification'). Methods: A study was conducted among new smear-positive pulmonary TB patients registered between March 2016 and February 2017 in 18 randomly selected districts to determine the effectiveness of an active case-finding strategy in marginalised and vulnerable populations. We included all patients detected through active case-finding. An equal number of randomly selected patients registered through passive case-finding from marginalised and vulnerable populations in the same districts were included. Before enrolment, we enquired about any history of previous TB treatment through interviews. Results: Of 629 patients, we interviewed 521, of whom, 11% (n=56) had past history of TB treatment (public or private) for at least a month: 13% (34/268) among the active case-finding group and 9% (22/253) among the passive case-finding group (p=0.18). No factors were found to be significantly associated with misclassification. Conclusion: Around one in every ten patients registered as 'new' had previous history of TB treatment. Corrective measures need to be implemented, followed by monitoring of any change in the proportion of 'previously treated' patients among all registered patients treated under the programme at national level., Competing Interests: No competing interests were disclosed.

Published

2019

17. Patient characteristics, health seeking and delays among new sputum smear positive TB patients identified through active case finding when compared to passive case finding in India.

Author

Shewade HD, Gupta V, Satyanarayana S, Pandey P, Bajpai UN, Tripathy JP, Kathirvel S, Pandurangan S, Mohanty S, Ghule VH, Sagili KD, Prasad BM, Nath S, Singh P, Singh K, Singh R, Jayaraman G, Rajeswaran P, Srivastava BK, Biswas M, Mallick G, Bera OP, Sahai KN, Murali L, Kamble S, Deshpande M, Kumar N, Kumar S, Jaisingh AJJ, Naqvi AJ, Verma P, Ansari MS, Mishra PC, Sumesh G, Barik S, Mathew V, Lohar MRS, Gaurkhede CS, Parate G, Bale SY, Koli I, Bharadwaj AK, Venkatraman G, Sathiyanarayanan K, Lal J, Sharma AK, Rao R, Kumar AMV, and Chadha SS

Subjects

Adolescent, Adult, Aged, Delayed Diagnosis, Female, Humans, India, Male, Mass Screening, Middle Aged, National Health Programs, Patient Acceptance of Health Care, Sputum microbiology, Time-to-Treatment, Tuberculosis, Pulmonary microbiology, Tuberculosis, Pulmonary therapy, Vulnerable Populations, Young Adult, Tuberculosis, Pulmonary diagnosis

Abstract

Background: Axshya SAMVAD is an active tuberculosis (TB) case finding (ACF) strategy under project Axshya (Axshya meaning 'free of TB' and SAMVAD meaning 'conversation') among marginalized and vulnerable populations in 285 districts of India., Objectives: To compare patient characteristics, health seeking, delays in diagnosis and treatment initiation among new sputum smear positive TB patients detected through ACF and passive case finding (PCF) under the national TB programme in marginalized and vulnerable populations between March 2016 and February 2017., Methods: This observational analytic study was conducted in 18 randomly sampled Axshya districts. We enrolled all TB patients detected through ACF and an equal number of randomly selected patients detected through PCF in the same settings. Data on patient characteristics, health seeking and delays were collected through record review and patient interviews (at their residence). Delays included patient level delay (from eligibility for sputum examination to first contact with any health care provider (HCP)), health system level diagnosis delay (from contact with first HCP to TB diagnosis) and treatment initiation delays (from diagnosis to treatment initiation). Total delay was the sum of patient level, health system level diagnosis delay and treatment initiation delays., Results: We included 234 ACF-diagnosed and 231 PCF-diagnosed patients. When compared to PCF, ACF patients were relatively older (≥65 years, 14% versus 8%, p = 0.041), had no formal education (57% versus 36%, p<0.001), had lower monthly income per capita (median 13.1 versus 15.7 USD, p = 0.014), were more likely from rural areas (92% versus 81%, p<0.002) and residing far away from the sputum microscopy centres (more than 15 km, 24% versus 18%, p = 0.126). Fewer patients had history of significant loss of weight (68% versus 78%, p = 0.011) and sputum grade of 3+ (15% versus 21%, p = 0.060). Compared to PCF, HCP visits among ACF patients was significantly lower (median one versus two HCPs, p<0.001). ACF patients had significantly lower health system level diagnosis delay (median five versus 19 days, p = 0.008) and the association remained significant after adjusting for potential confounders. Patient level and total delays were not significantly different., Conclusion: Axshya SAMVAD linked the most impoverished communities to TB care and resulted in reduction of health system level diagnosis delay., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

18. Active versus passive case finding for tuberculosis in marginalised and vulnerable populations in India: comparison of treatment outcomes.

Author

Shewade HD, Gupta V, Satyanarayana S, Kumar S, Pandey P, Bajpai UN, Tripathy JP, Kathirvel S, Pandurangan S, Mohanty S, Ghule VH, Sagili KD, Prasad BM, Singh P, Singh K, Jayaraman G, Rajeswaran P, Biswas M, Mallick G, Naqvi AJ, Bharadwaj AK, Sathiyanarayanan K, Pathak A, Mohan N, Rao R, Kumar AMV, and Chadha SS

Subjects

Adolescent, Adult, Aged, Cohort Studies, Female, Humans, India epidemiology, Interviews as Topic, Male, Mass Screening methods, Middle Aged, Prevalence, Qualitative Research, Treatment Outcome, Tuberculosis, Pulmonary diagnosis, Young Adult, Tuberculosis, Pulmonary drug therapy, Tuberculosis, Pulmonary epidemiology, Vulnerable Populations

Abstract

Background : Community-based active case finding (ACF) for tuberculosis (TB) implemented among marginalised and vulnerable populations in 285 districts of India resulted in reduction of diagnosis delay and prevalence of catastrophic costs due to TB diagnosis. We were interested to know whether this translated into improved treatment outcomes. Globally, there is limited published literature from marginalised and vulnerable populations on the independent effect of community-based ACF on treatment outcomes when compared to passive case finding (PCF). Objectives : To determine the relative differences in unfavourable treatment outcomes (death, loss-to-follow-up, failure, not evaluated) of ACF and PCF-diagnosed people. Methods : Cohort study involving record reviews and interviews in 18 randomly selected districts. We enrolled all ACF-diagnosed people with new smear-positive pulmonary TB, registered under the national TB programme between March 2016 and February 2017, and an equal number of randomly selected PCF-diagnosed people in the same settings. We used log binomial models to adjust for confounders. Results : Of 572 enrolled, 275 belonged to the ACF and 297 to the PCF group. The proportion of unfavourable outcomes were 10.2% (95% CI: 7.1%, 14.3%) in the ACF and 12.5% (95% CI: 9.2%, 16.7%) in the PCF group (p = 0.468). The association between ACF and unfavourable outcomes remained non-significant after adjusting for confounders available from records [aRR: 0.83 (95% CI: 0.56, 1.21)]. Due to patient non-availability at their residence, interviews were conducted for 465 (81.3%). In the 465 cohort too, there was no association after adjusting for confounders from records and interviews [aRR: 1.05 (95% CI: 0.62, 1.77)]. Conclusion : We did not find significant differences in the treatment outcomes. Due to the wide CIs, studies with larger sample sizes are urgently required. Studies are required to understand how to translate the benefits of ACF to improved treatment outcomes.

Published

2019

19. Active case finding among marginalised and vulnerable populations reduces catastrophic costs due to tuberculosis diagnosis.

Author

Shewade HD, Gupta V, Satyanarayana S, Kharate A, Sahai KN, Murali L, Kamble S, Deshpande M, Kumar N, Kumar S, Pandey P, Bajpai UN, Tripathy JP, Kathirvel S, Pandurangan S, Mohanty S, Ghule VH, Sagili KD, Prasad BM, Nath S, Singh P, Singh K, Singh R, Jayaraman G, Rajeswaran P, Srivastava BK, Biswas M, Mallick G, Bera OP, Jaisingh AJJ, Naqvi AJ, Verma P, Ansari MS, Mishra PC, Sumesh G, Barik S, Mathew V, Lohar MRS, Gaurkhede CS, Parate G, Bale SY, Koli I, Bharadwaj AK, Venkatraman G, Sathiyanarayanan K, Lal J, Sharma AK, Rao R, Kumar AMV, and Chadha SS

Subjects

Adolescent, Adult, Aged, Female, Health Expenditures, Humans, India epidemiology, Male, Middle Aged, Prevalence, Socioeconomic Factors, Tuberculosis epidemiology, Young Adult, Mass Screening economics, Tuberculosis diagnosis, Tuberculosis economics, Vulnerable Populations

Abstract

Background: There is limited evidence on whether active case finding (ACF) among marginalised and vulnerable populations mitigates the financial burden during tuberculosis (TB) diagnosis., Objectives: To determine the effect of ACF among marginalised and vulnerable populations on prevalence and inequity of catastrophic costs due to TB diagnosis among TB-affected households when compared with passive case finding (PCF)., Methods: In 18 randomly sampled ACF districts in India, during March 2016 to February 2017, we enrolled all new sputum-smear-positive TB patients detected through ACF and an equal number of randomly selected patients detected through PCF. Direct (medical and non-medical) and indirect costs due to TB diagnosis were collected through patient interviews at their residence. We defined costs due to TB diagnosis as 'catastrophic' if the total costs (direct and indirect) due to TB diagnosis exceeded 20% of annual pre-TB household income. We used concentration curves and indices to assess the extent of inequity., Results: When compared with patients detected through PCF (n = 231), ACF patients (n = 234) incurred lower median total costs (US$ 4.6 and 20.4, p < 0.001). The prevalence of catastrophic costs in ACF and PCF was 10.3 and 11.5% respectively. Adjusted analysis showed that patients detected through ACF had a 32% lower prevalence of catastrophic costs relative to PCF [adjusted prevalence ratio (95% CI): 0.68 (0.69, 0.97)]. The concentration indices (95% CI) for total costs in both ACF [-0.15 (-0.32, 0.11)] and PCF [-0.06 (-0.20, 0.08)] were not significantly different from the line of equality and each other. The concentration indices (95% CI) for catastrophic costs in both ACF [-0.60 (-0.81, -0.39)] and PCF [-0.58 (-0.78, -0.38)] were not significantly different from each other: however, both the curves had a significant distribution among the poorest quintiles., Conclusion: ACF among marginalised and vulnerable populations reduced total costs and prevalence of catastrophic costs due to TB diagnosis, but could not address inequity.

Published

2018

20. 1,1'-[(2-Bromo-phen-yl)-methyl-ene]-dipyrrolidin-2-one.

Author

Li HQ, Ramachandran G, Satheesh V, Sathiyanarayanan K, and Rathore RS

Abstract

In the title compound, C(15)H(17)BrN(2)O(2), both pyrrolidinone rings adopt envelope conformations. The crystal packing is characterized by short C-Br⋯O=C inter-actions [Br⋯O = 3.1730 (13) Å], leading to supra-molecular dimers. Inter-molecular C-H⋯O and C-H⋯π inter-actions are also observed.

Published

2012

21. 1-Meth-oxy-4-({[(4-meth-oxy-phen-yl)-sulfan-yl](phen-yl)meth-yl}sulfan-yl)benzene.

Author

Li H, Ramachandran G, Sathishkumar M, Sathiyanarayanan K, and Rathore RS

Abstract

The title compound, C(21)H(20)O(2)S(2), forms a propeller-shaped structure with the tetra-hedral C atom as the central hub and meth-oxy-benzene and phenyl residues as radiating blades. Short C-H⋯π contacts are observed.

Published

2012

22. (7E)-5-Benzyl-7-(2-chloro-benzyl-idene)-3-(2-chloro-phen-yl)-2-phenyl-3,3a,4,5,6,7-hexa-hydro-2H-pyrazolo-[4,3-c]pyridine.

Author

Karthikeyan NS, Mahesh BU, Sathiyanarayanan K, Raghavaiah P, and Rathore RS

Abstract

In the title 2H-pyrazolo-[4,3-c]pyridine derivative, C(32)H(27)Cl(2)N(3), the dihydro-pyrazole ring adopts an envelope conformation and the piperidine fused ring a twisted-chair conformation. Two short intra-molecular C-H⋯Cl contacts are observed. The crystal packing is characterized by dimeric C-Cl⋯π inter-actions involving the 5-benzyl ring, with Cl⋯centroid and closest atomic Cl⋯π distances of 3.778 (2) and 3.366 (4) Å, respectively.

Published

2010

23. 3-(7,8,13,14-Tetra-hydrodi-benzo-[a,i]phen-an-thridin-5-yl)benzene-1,2-diol.

Author

Karthikeyan NS, Ramachandran G, Sathiyanarayanan K, Raghavaiah P, and Rathore RS

Abstract

In the title compound, C(27)H(21)NO(2), the half-chair conformation of the alicyclic rings gives rise to a slightly folded structure of the central tricyclic tetra-hydrophenanthridine unit. Tandem intra-molecular O-H⋯N and O-H⋯O hydrogen bonds give rise to adjacent S(6) and S(5) rings, respectively, which dictate the conformation of the 5-aryl substituent. In the crystal structure, an inter-molecular C-H⋯O contact generates chains parallel to [101]. Short O-H⋯π and C-H⋯π contacts are also observed.

Published

2010

24. (3E,5E)-3,5-Bis(4-allyl-oxybenzyl-idene)-1-benzyl-piperidin-4-one.

Author

Karthikeyan NS, Sathiyanarayanan K, Aravindan PG, Ghosh H, and Rathore RS

Abstract

In the title compound C(32)H(31)NO(3), the all-yloxy groups on either side of the piperidin-4-one ring are conformationally disordered. The contribution of major and minor components of the allyloxy group at the 3rd position of the ring are 0.576 (4) and 0.424 (4), respectively, and those at the 5th position are 0.885 (3) and 0.115 (3), respectively. The six-membered piperidin-4-one ring adopts a sofa conformation with the benzyl group occupying an equatorial position and the olefinic double bonds possessing an E configuration. Flanking phenyl substituents are stretched out on either side of the six-membered ring. π-π inter-actions with a centroid-centroid distance of 3.885 (1) Å give rise to mol-ecular dimers and short C-H⋯π contacts lead to chains along the c axis.

Published

2009

25. (3E,5E)-1-Benzyl-3,5-dibenzyl-idenepiperidin-4-one.

Author

Karthikeyan NS, Sathiyanarayanan K, Aravindan PG, and Rathore RS

Abstract

In the title compound, C(26)H(23)NO, C-H⋯O hydrogen bonds generate a ribbon structure along the a axis. These ribbons further assemble into a one-dimensional sheet parallel to the ac plane via C-H⋯π inter-actions. The piperidin-4-one ring adopts a sofa conformation with the 1-benzyl group in the equatorial position, and the 3- and 5-phenyl substituents stretched out on either side. The benzyl-idene units adopt E configurations and the 1-benzyl group is disposed towards the 3- substituent of the piperidin-4-one ring.

Published

2009

26. (3E,5E)-1-Benzyl-3,5-bis-(2-fluoro-benzyl-idene)piperidin-4-one.

Author

Rathore RS, Karthikeyan NS, Sathiyanarayanan K, and Aravindan PG

Abstract

The inversion-related mol-ecules of the title compound, C(26)H(21)F(2)NO, associate into closed dimeric subunits via co-operative C-H⋯π inter-actions. Two non-classical C-H⋯O and one C-H⋯N intra-molecular hydrogen bonds are also found in the crystal structure. The piperidin-4-one ring adopts a sofa conforamtion with the 1-benzyl group in the equatorial position, and the equiplanar fluoro-phenyl substituents in the 3- and 5-positions stretched out on either side. The 1-benzyl group is disposed towards the substituent in the 6th position of the piperidin-4-one ring. The 3,5-diene units possess E configurations.

Published

2009

27. 2,3-Bis(phenoxy-meth-yl)buta-1,3-diene.

Author

Sathiyanarayanan K, George Fernand A, Dhanasekaran V, and Rathore RS

Abstract

The mol-ecule of the title compound, C(18)H(18)O(2), a symmetrically phenol-substituted divinyl analog, exhibits crystallographically imposed C(2) symmetry. The phenolic and divinyl planar groups inter-sect each other orthogonally, with a dihedral angle of 82.7 (1)°. The structure is stabilized by a short intra-molecular C-H⋯O contact. The mol-ecules are held together by C-H⋯π inter-actions, forming a sheet structure parallel to the (201) plane.

Published

2007

28. 2,3-Bis[(2-methyl-phen-oxy)meth-yl]buta-1,3-diene.

Author

Sathiyanarayanan K, George Fernand A, Dhanasekaran V, and Rathore RS

Abstract

The mol-ecule of the title compound, C(20)H(22)O(2), a symmetrically 2-methyl-phenol-substituted divinyl analog, exhibits crystallographically imposed C(2) symmetry. The mol-ecular structure is essentially planar. The structure is stabilized by a short inter-molecular C-H⋯O contact. Cooperative C-H⋯π inter-actions generate an infinite one-dimensional chain of mol-ecules along the a axis.

Published

2007

29. An improved method for defluoridation.

Author

Muthu GI, Vinodhini V, Padmapriya G, Sathiyanarayanan K, and Sabumon PC

Subjects

Alum Compounds chemistry, Environmental Monitoring, Fluorides analysis, India, Fluorides isolation & purification, Water Purification methods

Abstract

Fluoride is a naturally occurring toxic mineral present in drinking water and the root cause of many diseases and disorders. Present international drinking water standard set by World Health Organisation (WHO) for fluoride is 1.5 ppm. In order to find the wide spread concentration of fluoride in drinking water of fluoride contaminated aquifer, 30 bore well water samples have been collected from different villages of Natrampalli Union which comes under Tiruvannamalai Circle, Tamil Nadu, India. In the present work, an attempt to remove fluoride by the use of coagulant, Poly Aluminium Chloride (PAC) was made and is compared with the most common existing technique "Nalgonda Technique" where there was a reversible reaction. The coagulant used in Nalgonda technique is Alum [(Al2SO4)3]. Results of the present work show that Poly Aluminium Chloride (PAC) can be an effective coagulant for the removal of fluoride from water with a higher removal efficiency of about 75 - 85% in less detention time and also observed that the fluoride removal was dependent on initial fluoride concentration and dose of coagulants.

Published

2003