6 research outputs found
Mechanics of silage compaction
- Author
- Publication venue
- Iowa State University Digital Repository
- Publication date
- 01/01/1967
- Field of study
Get PDFDeveloping and testing accelerated partner therapy for partner notification for people with genital Chlamydia trachomatis diagnosed in primary care: a pilot randomised controlled trial
- Author
- Althaus
- Andrew Copas
- Anne M Johnson
- Bailey
- Cassell
- Catherine H Mercer
- Centers for Disease Control and Prevention
- Chen
- Claudia S Estcourt
- Cowan
- Estcourt
- Estcourt
- Ferreira
- Greta Rait
- Götz
- Jackie A Cassell
- Kazeem Aderogba
- Laura Tickle
- Lorna J Sutcliffe
- Louise J Jackson
- Low
- Low
- McCarney
- McNulty
- McNulty
- McNulty
- Mercer
- Mercer
- Mercer
- Merle Symonds
- Miller
- Pamela Muniina
- Roberts
- Sarah Creighton
- Shackleton
- Tracy E Roberts
- Turner
- Publication venue
- 'BMJ'
- Publication date
- 01/01/2015
- Field of study
Get PDFBackground
Accelerated partner therapy (APT) is a promising partner notification (PN) intervention in specialist sexual health clinic attenders. To address its applicability in primary care, we undertook a pilot randomised controlled trial (RCT) of two APT models in community settings.
Methods
Three-arm pilot RCT of two adjunct APT interventions: APTHotline (telephone assessment of partner(s) plus standard PN) and APTPharmacy (community pharmacist assessment of partner(s) plus routine PN), versus standard PN alone (patient referral). Index patients were women diagnosed with genital chlamydia in 12 general practices and three community contraception and sexual health (CASH) services in London and south coast of England, randomised between 1 September 2011 and 31 July 2013.
Results
199 women described 339 male partners, of whom 313 were reported by the index as contactable. The proportions of contactable partners considered treated within 6â
weeks of index diagnosis were APTHotline 39/111 (35%), APTPharmacy 46/100 (46%), standard patient referral 46/102 (45%). Among treated partners, 8/39 (21%) in APTHotline arm were treated via hotline and 14/46 (30%) in APTPharmacy arm were treated via pharmacy.
Conclusions
The two novel primary care APT models were acceptable, feasible, compliant with regulations and capable of achieving acceptable outcomes within a pilot RCT but intervention uptake was low. Although addition of these interventions to standard PN did not result in a difference between arms, overall PN uptake was higher than previously reported in similar settings, probably as a result of introducing a formal evaluation. Recruitment to an individually randomised trial proved challenging and full evaluation will likely require service-level randomisation
Guidelines for the use of flow cytometry and cell sorting in immunological studies
- Author
- A. Graham Pockley
- Aalderen
- Abate
- Abdelrahman
- Acosta-Rodriguez
- Agematsu
- Agematsu
- Aghaeepour
- Aghaeepour
- Aghaeepour
- Aghaeepour
- Aghaeepour
- Aichele
- Akkaya
- Akondy
- Alan M. Stall
- Alanio
- Alder
- Alessandro Moretta
- Alexander Scheffold
- Alfadda
- Alfonso Blanco
- Alice Yue
- Alix-PanabiĂšres
- Alsayed
- Altman
- Amini
- Amir el
- Amit
- Amy Lovett-Racke
- Ana Cumano
- Anat Shemer
- Anderson
- Anderson
- Anding
- Andrea Cavani
- Andrea Cossarizza
- Andrea Gori
- Andreas Diefenbach
- Andreas Dolf
- Andreas GrĂŒtzkau
- Andreas Radbruch
- Andrew Filby
- Angelo
- Anis Larbi
- Anita Dreher
- Anja E. Hauser
- Anna Iannone
- Anna Rubartelli
- Anna-Katharina Simon
- Anne Cooke
- Annette Oxenius
- Annika Wiedemann
- Anselmo
- Antonio Cosma
- Appay
- Appay
- Appert-Collin
- Arai
- Ari Waisman
- Armstrong
- Asbury
- Assenmacher
- Attila Tarnok
- Auffray
- Autréaux
- Avey
- Avramidou
- Axel Ronald Schulz
- Baba
- Bacher
- Bacher
- Bacher
- Bacher
- Bacher
- Baecher-Allan
- Baehner
- Baerbel Keller
- Baerlocher
- Bagwell
- Bailey
- Bain
- Bajno
- Bakker
- Balazs
- Bandura
- Bar-On
- Barber
- Barry Moran
- Bart Everts
- Bartek Rajwa
- Bashashati
- Basiji
- BassĂže
- Basu
- Baumgart
- Baumgart
- Baxter
- Beate Ruckert
- Beatriz JĂĄvega
- Becher
- Becker
- Behbehani
- Behbehani
- Belaaouaj
- Bendall
- Bendall
- Benjamini
- Berhanu
- Bernardo
- Bernink
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- Betts
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- Bianco
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- Biasi
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- Bimba F. Hoyer
- Binder
- Birgit Sawitzki
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- Bo Huang
- Bocsi
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- Boehm
- Bogunovic
- Boya
- Boyd
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- Boyum
- Boyum
- Boyum
- Bradbury
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- Braud
- Breitfeld
- Brinkman
- Britta Engelhardt
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- Burkhard Becher
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- Chattopadhyay
- Chattopadhyay
- Chattopadhyay
- Chattopadhyay
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- Chen
- Chen
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- Christoph Goettlinger
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- Cristiano Scotta
- Crosland-Taylor
- Cua
- Cuervo
- Cupedo
- D'Silva
- Daisy Philips
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- Mario Clerici
- Mark Dessing
- Marlous van der Braber
- Marquardt
- Martin BĂŒscher
- Martin Herrmann
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- Wolfgang M. Bauer
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- Wong
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- Wood
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- Wu
- Wynn
- Wysocki
- Wölfl
- Wölfl
- Xiao
- Xu
- Xuetao Cao
- Yamamoto
- Yamanaka
- Yang
- Yanling Liu
- Yeo
- Yi Zhao
- Yilmaz
- Yona
- Young
- Yousuke Takahama
- Yu
- Yu
- Yu
- Yvonne Samstag
- Yåñez
- Zaunders
- Zawada
- Zhang
- Zheng
- ZhiGang Tian
- Zhou
- Zhou
- Zhou
- Zhou
- Zielinski
- Zigmond
- Zimmermann
- Zimmermann
- Zivanovic
- Zuba-Surman
- Zunder
- Zunder
- Publication venue
- 'Wiley'
- Publication date
- 01/01/2017
- Field of study
Get PDFInternational audienceThe classical model of hematopoiesis established in the mouse postulates that lymphoid cells originate from a founder population of common lymphoid progenitors. Here, using a modeling approach in humanized mice, we showed that human lymphoid development stemmed from distinct populations of CD127(-) and CD127(+) early lymphoid progenitors (ELPs). Combining molecular analyses with in vitro and in vivo functional assays, we demonstrated that CD127(-) and CD127(+) ELPs emerged independently from lympho-mono-dendritic progenitors, responded differently to Notch1 signals, underwent divergent modes of lineage restriction, and displayed both common and specific differentiation potentials. Whereas CD127(-) ELPs comprised precursors of T cells, marginal zone B cells, and natural killer (NK) and innate lymphoid cells (ILCs), CD127(+) ELPs supported production of all NK cell, ILC, and B cell populations but lacked T potential. On the basis of these results, we propose a "two-family" model of human lymphoid development that differs from the prevailing model of hematopoiesis
Enhanced infection prophylaxis reduces mortality in severely immunosuppressed HIV-infected adults and older children initiating antiretroviral therapy in Kenya, Malawi, Uganda and Zimbabwe: the REALITY trial
- Author
- Abach J
- Abdallah J
- Abdallah S
- Abdallah S
- Aberle-Grasse J
- Abimiku A
- Abishev A
- Abongomera G
- Aboud M
- Aboud M
- Abramovitz D
- Abrams E
- Abrams E
- Abrams E
- Abrams E
- Abravaya K
- Abreu L
- Achra A
- Adera F
- Adetokunboh O
- Adeyemi O
- Adeyemi O
- Adipo T
- Affolabi D
- Agegnehu D
- Agius P
- Agolory S
- Agot K
- Agot K
- Agovi A-A
- Aguiar P
- Aguilar-Martinez J
- Agutu C
- Ahmed M
- Ahmed R
- Ahmed S
- Ahmed S
- Ahmed S
- Aizire J
- Ajibola G
- Ajok S
- Albert-Hope C
- Alejos B
- Alexander G
- Alicea C
- Allen H
- Allen M
- Allen S
- Allen S
- Allen S
- Alloui C
- Altice F
- Altice F
- Amara R
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Get PDFMeeting abstract FRAB0101LB from 21st International AIDS Conference 18â22 July 2016, Durban, South Africa.
Introduction: Mortality from infections is high in the first 6 months of antiretroviral therapy (ART) among HIVâinfected adults and children with advanced disease in subâSaharan Africa. Whether an enhanced package of infection prophylaxis at ART initiation would reduce mortality is unknown.
Methods:
The REALITY 2Ă2Ă2 factorial openâlabel trial (ISRCTN43622374) randomized ARTânaĂŻve HIVâinfected adults and children >5 years with CD4 <100 cells/mm3. This randomization compared initiating ART with enhanced prophylaxis (continuous cotrimoxazole plus 12 weeks isoniazid/pyridoxine (antiâtuberculosis) and fluconazole (antiâcryptococcal/candida), 5 days azithromycin (antiâbacterial/protozoal) and singleâdose albendazole (antiâhelminth)), versus standardâofâcare cotrimoxazole. Isoniazid/pyridoxine/cotrimoxazole was formulated as a scored fixedâdose combination. Two other randomizations investigated 12âweek adjunctive raltegravir or supplementary food. The primary endpoint was 24âweek mortality.
Results:
1805 eligible adults (n = 1733; 96.0%) and children/adolescents (n = 72; 4.0%) (median 36 years; 53.2% male) were randomized to enhanced (n = 906) or standard prophylaxis (n = 899) and followed for 48 weeks (3.8% lossâtoâfollowâup). Median baseline CD4 was 36 cells/mm3 (IQR: 16â62) but 47.3% were WHO Stage 1/2. 80 (8.9%) enhanced versus 108(12.2%) standard prophylaxis died before 24 weeks (adjusted hazard ratio (aHR) = 0.73 (95% CI: 0.54â0.97) p = 0.03; Figure 1) and 98(11.0%) versus 127(14.4%) respectively died before 48 weeks (aHR = 0.75 (0.58â0.98) p = 0.04), with no evidence of interaction with the two other randomizations (p > 0.8). Enhanced prophylaxis significantly reduced incidence of tuberculosis (p = 0.02), cryptococcal disease (p = 0.01), oral/oesophageal candidiasis (p = 0.02), deaths of unknown cause (p = 0.02) and (marginally) hospitalisations (p = 0.06) but not presumed severe bacterial infections (p = 0.38). Serious and grade 4 adverse events were marginally less common with enhanced prophylaxis (p = 0.06). CD4 increases and VL suppression were similar between groups (p > 0.2).
Conclusions:
Enhanced infection prophylaxis at ART initiation reduces early mortality by 25% among HIVâinfected adults and children with advanced disease. The pill burden did not adversely affect VL suppression. Policy makers should consider adopting and implementing this lowâcost broad infection prevention package which could save 3.3 lives for every 100 individuals treated
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- Ng Johnny
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- Nguyen-Hong-Nheim
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- Patel D. I.
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- Publication venue
- 'UCLA American Indian Studies Center'
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