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161. Rethinking how development assistance for health can catalyse progress on primary health care.

作者: Tobias Kasper.;Gavin Yamey.;Sinead Dwyer.;Kaci Kennedy McDade.;Jon Lidén.;Cora Lüdemann.;Mohamed Mustafa Diab.;Osondu Ogbuoji.;Prashant Poodla.;Christina Schrade.;Andrea Thoumi.;Armand Zimmerman.;Yibeltal Assefa.;Luke N Allen.;Paulin Basinga.;Patricia J Garcia.;Debra Jackson.;Henry Mwanyika.;Rachel Nugent.;Anthony Ofosu.;Salman Rawaf.;K Srinath Reddy.;Dykki Settle.;Beth Tritter.;Christoph Benn.
来源: Lancet. 2023年402卷10418期2253-2264页
Global campaigns to control HIV, tuberculosis, malaria, and vaccine-preventable illnesses showed that large-scale impact can be achieved by using additional international financing to support selected, evidence-based, high-impact investment areas and to catalyse domestic resource mobilisation. Building on this paradigm, we make the case for targeting additional international funding for selected high-impact investments in primary health care. We have identified and costed a set of concrete, evidence-based investments that donors could support, which would be expected to have major impacts at an affordable cost. These investments are in: (1) individuals and communities empowered to engage in health decision making, (2) a new model of people-centred primary care, and (3) next generation community health workers. These three areas would be supported by strengthening two cross-cutting elements of national systems. The first is the digital tools and data that support facility, district, and national managers to improve processes, quality of care, and accountability across primary health care. The second is the educational, training, and supervisory systems needed to improve the quality of care. We estimate that with an additional international investment of between US$1·87 billion in a low-investment scenario and $3·85 billion in a high-investment scenario annually over the next 3 years, the international community could support the scale-up of this evidence-based package of investments in the 59 low-income and middle-income countries that are eligible for external financing from the World Bank Group's International Development Association.

162. The Lancet Commission on medicine, Nazism, and the Holocaust: historical evidence, implications for today, teaching for tomorrow.

作者: Herwig Czech.;Sabine Hildebrandt.;Shmuel P Reis.;Tessa Chelouche.;Matthew Fox.;Esteban González-López.;Etienne Lepicard.;Astrid Ley.;Miriam Offer.;Avi Ohry.;Maike Rotzoll.;Carola Sachse.;Sari J Siegel.;Michal Šimůnek.;Amir Teicher.;Kamila Uzarczyk.;Anna von Villiez.;Hedy S Wald.;Matthew K Wynia.;Volker Roelcke.
来源: Lancet. 2023年402卷10415期1867-1940页

163. Multiple sclerosis.

作者: Dejan Jakimovski.;Stefan Bittner.;Robert Zivadinov.;Sarah A Morrow.;Ralph Hb Benedict.;Frauke Zipp.;Bianca Weinstock-Guttman.
来源: Lancet. 2024年403卷10422期183-202页
Multiple sclerosis remains one of the most common causes of neurological disability in the young adult population (aged 18-40 years). Novel pathophysiological findings underline the importance of the interaction between genetics and environment. Improvements in diagnostic criteria, harmonised guidelines for MRI, and globalised treatment recommendations have led to more accurate diagnosis and an earlier start of effective immunomodulatory treatment than previously. Understanding and capturing the long prodromal multiple sclerosis period would further improve diagnostic abilities and thus treatment initiation, eventually improving long-term disease outcomes. The large portfolio of currently available medications paved the way for personalised therapeutic strategies that will balance safety and effectiveness. Incorporation of cognitive interventions, lifestyle recommendations, and management of non-neurological comorbidities could further improve quality of life and outcomes. Future challenges include the development of medications that successfully target the neurodegenerative aspect of the disease and creation of sensitive imaging and fluid biomarkers that can effectively predict and monitor disease changes.

164. Malaria.

作者: Jeanne Rini Poespoprodjo.;Nicholas M Douglas.;Daniel Ansong.;Steven Kho.;Nicholas M Anstey.
来源: Lancet. 2023年402卷10419期2328-2345页
Malaria is resurging in many African and South American countries, exacerbated by COVID-19-related health service disruption. In 2021, there were an estimated 247 million malaria cases and 619 000 deaths in 84 endemic countries. Plasmodium falciparum strains partly resistant to artemisinins are entrenched in the Greater Mekong region and have emerged in Africa, while Anopheles mosquito vectors continue to evolve physiological and behavioural resistance to insecticides. Elimination of Plasmodium vivax malaria is hindered by impractical and potentially toxic antirelapse regimens. Parasitological diagnosis and treatment with oral or parenteral artemisinin-based therapy is the mainstay of patient management. Timely blood transfusion, renal replacement therapy, and restrictive fluid therapy can improve survival in severe malaria. Rigorous use of intermittent preventive treatment in pregnancy and infancy and seasonal chemoprevention, potentially combined with pre-erythrocytic vaccines endorsed by WHO in 2021 and 2023, can substantially reduce malaria morbidity. Improved surveillance, better access to effective treatment, more labour-efficient vector control, continued drug development, targeted mass drug administration, and sustained political commitment are required to achieve targets for malaria reduction by the end of this decade.

165. β blockers switched to first-line therapy in hypertension.

作者: Franz H Messerli.;Sripal Bangalore.;John M Mandrola.
来源: Lancet. 2023年402卷10414期1802-1804页
In their recent guidelines, the European Society of Hypertension upgraded β blockers, putting them on equal footing with thiazide diuretics, renin-angiotensin system blockers (eg, angiotensin-converting enzyme inhibitors and angiotensin receptor blockers), and calcium channel blockers. The reason offered for upgrading β blockers was the observation that they are often used for many other clinical conditions commonly encountered with hypertension. This upgrade would allow for the treatment of two conditions with a single drug (a so-called twofer). In most current national and international hypertension guidelines, β blockers are only considered to be an alternative when there are specific indications. Compared with the other first-line antihypertensive drug classes, β blockers are significantly less effective in preventing stroke and cardiovascular mortality. To relegate β blockers to an inferiority status as previous guidelines have done was based on the evidence in aggregate, and still stands. No new evidence supports the switch of β blockers back to first-line therapy. We are concerned that this move might lead to widespread harm because of inferior stroke protection.

166. Health and inclusive labour force participation.

作者: Alex Burdorf.;Rita C P Fernandes.;Suzan J W Robroek.
来源: Lancet. 2023年402卷10410期1382-1392页
The future of work is rapidly changing, with higher flexibility of the labour market and increasing informal employment in many countries worldwide. There is also an increased pressure to extend working careers until older age. We introduce the concept of working life expectancy as a useful metric, capturing the expected numer of years in paid employment across the working age individuals, in particular among different groups. We describe factors that determine working life expectancy. Macro-level factors focus on the socioeconomic and political context that influences labour force participation, primarily policies and legislation in specific countries. At the meso level, employment contracts and working conditions are important. The micro level shows that individual characteristics, such as education, gender, and age, influence working careers. There are three important groups with a disadvantaged position in the labour market-workers with chronic diseases, workers with impairing disabilities, and workers aged 50 years or more. Within each of these disadvantaged groups, macro-level, meso-level, and micro-level factors that influence entering and exiting paid employment are discussed. To assure that paid employment is available for everyone of working age and that work contributes to better health, specific challenges need to be addressed at the macro, meso, and micro levels. To reach inclusive labour force participation, national policies, company practices, and workplace improvements need to be aligned to ensure safe and healthy workplaces that contribute to the health and wellbeing of workers and their communities.

167. Work-related causes of mental health conditions and interventions for their improvement in workplaces.

作者: Reiner Rugulies.;Birgit Aust.;Birgit A Greiner.;Ella Arensman.;Norito Kawakami.;Anthony D LaMontagne.;Ida E H Madsen.
来源: Lancet. 2023年402卷10410期1368-1381页
Mental health problems and disorders are common among working people and are costly for the affected individuals, employers, and whole of society. This discussion paper provides an overview of the current state of knowledge on the relationship between work and mental health to inform research, policy, and practice. We synthesise available evidence, examining both the role of working conditions in the development of mental disorders, and what can be done to protect and promote mental health in the workplace. We show that exposure to some working conditions is associated with an increased risk of the onset of depressive disorders, the most studied mental disorders. The causality of the association, however, is still debated. Causal inference should be supported by more research with stronger linkage to theory, better exposure assessment, better understanding of biopsychosocial mechanisms, use of innovative analytical methods, a life-course perspective, and better understanding of the role of context, including the role of societal structures in the development of mental disorders. There is growing evidence for the effectiveness of interventions to protect and promote mental health and wellbeing in the workplace; however, there is a disproportionate focus on interventions directed towards individual workers and illnesses, compared with interventions for improving working conditions and enhancing mental health. Moreover, research on work and mental health is mainly done in high-income countries, and often does not address workers in lower socioeconomic positions. Flexible and innovative approaches tailored to local conditions are needed in implementation research on workplace mental health to complement experimental studies. Improvements in translating workplace mental health research to policy and practice, such as through workplace-oriented concrete guidance for interventions, and by national policies and programmes focusing on the people most in need, could capitalise on the growing interest in workplace mental health, possibly yielding important mental health gains in working populations.

168. Work as a social determinant of health in high-income countries: past, present, and future.

作者: John Frank.;Cameron Mustard.;Peter Smith.;Arjumand Siddiqi.;Yawen Cheng.;Alex Burdorf.;Reiner Rugulies.
来源: Lancet. 2023年402卷10410期1357-1367页
This paper, the first in a three-part Series on work and health, provides a narrative review of research into work as a social determinant of health over the past 25 years, the key emerging challenges in this field, and the implications of these challenges for future research. By use of a conceptual framework for work as a social determinant of health, we identified six emerging challenges: (1) the influence of technology on the nature of work in high-income countries, culminating in the sudden shift to telework during the COVID-19 pandemic; (2) the intersectionality of work with gender, sexual orientation, age, race, ethnicity, migrant status, and socioeconomic status as codeterminants of health disparities; (3) the arrival in many Organisation for Economic Co-operation and Development countries of large migrant labour workforces, who are often subject to adverse working conditions and social exclusion; (4) the development of precarious employment as a feature of many national labour markets; (5) the phenomenon of working long and irregular hours with potential health consequences; and (6) the looming threat of climate change's effects on work. We conclude that profound changes in the nature and availability of work over the past few decades have led to widespread new psychosocial and physical exposures that are associated with adverse health outcomes and contribute to increasing disparities in health. These new exposures at work will require novel and creative methods of data collection for monitoring of their potential health impacts to protect the workforce, and for new research into better means of occupational health promotion and protection. There is also an urgent need for a better integration of occupational health within public health, medicine, the life sciences, and the social sciences, with the work environment explicitly conceptualised as a major social determinant of health.

169. The forgotten girls: the state of evidence for health interventions for pregnant adolescents and their newborns in low-income and middle-income countries.

作者: Farnaz Sabet.;Audrey Prost.;Sadaf Rahmanian.;Heba Al Qudah.;Mauro Nogueira Cardoso.;John B Carlin.;Susan M Sawyer.;George C Patton.
来源: Lancet. 2023年402卷10412期1580-1596页
Every year, an estimated 21 million girls aged 15-19 years become pregnant in low-income and middle-income countries (LMICs). Policy responses have focused on reducing the adolescent birth rate whereas efforts to support pregnant adolescents have developed more slowly. We did a systematic review of interventions addressing any health-related outcome for pregnant adolescents and their newborn babies in LMICs and mapped its results to a framework describing high-quality health systems for pregnant adolescents. Although we identified some promising interventions, such as micronutrient supplementation, conditional cash transfers, and well facilitated group care, most studies were at high risk of bias and there were substantial gaps in evidence. These included major gaps in delivery, abortion, and postnatal care, and mental health, violence, and substance misuse-related outcomes. We recommend that the fields of adolescent, maternal, and sexual and reproductive health collaborate to develop more adolescent-inclusive maternal health care and research, and specific interventions for pregnant adolescents. We outline steps to develop high-quality, evidence-based care for the millions of pregnant adolescents and their newborns who currently do not receive this.

170. Polymyalgia rheumatica.

作者: Georgina Espígol-Frigolé.;Christian Dejaco.;Sarah L Mackie.;Carlo Salvarani.;Eric L Matteson.;Maria C Cid.
来源: Lancet. 2023年402卷10411期1459-1472页
Polymyalgia rheumatica is an inflammatory disease producing pain and stiffness, mainly in the shoulders and pelvic girdle, in people older than 50 years. Elevation of acute phase reactants is common due to the inflammatory nature of the disease. Since there are no specific diagnostic tests, diagnosis requires the exclusion of other diseases with similar presentations. Imaging has helped to identify the pathological substrate of polymyalgia rheumatica and it is increasingly used to support clinical diagnosis or to detect coexistent giant cell arteritis. Although polymyalgia rheumatica does not clearly impair survival or organ function, it can have a detrimental effect on quality of life. Glucocorticoids at 12·5-25·0 mg prednisone per day are effective in inducing remission in most individuals but, when tapered, relapses occur in 40-60% of those affected and side-effects are common. Assessment of disease activity can be difficult because pain related to common comorbidities such as osteoarthritis and tendinopathies, can return when glucocorticoids are reduced, and acute phase reactants are increased less during flares in individuals undergoing treatment or might increase for other reasons. The role of imaging in assessing disease activity is not yet completely defined. In the search for more efficient and safer therapies, tocilizumab and sarilumab have shown efficacy in randomised controlled trials and additional targeted therapies are emerging. However, judicious risk-benefit balance is essential in applying therapeutic innovations to people with polymyalgia rheumatica.

171. Life at The Lancet: a collection of memories.

作者: Dorothy Bonn.;David Sharp.;Robin Fox.;Stephanie Clark.;Pia Pini.;James Butcher.
来源: Lancet. 2023年402卷10409期1294-1298页

172. The Lancet 1823-2023: the best science for better lives.

作者: Martin Gorsky.;Agnes Arnold-Forster.
来源: Lancet. 2023年402卷10409期1284-1293页
The Lancet celebrates its 200th anniversary in 2023. In this survey of the journal's history, we explore how it has contributed to shaping medicine both in the UK and internationally, and how it has demonstrated a commitment to "The best science for better lives". For two centuries, the journal has published pioneering articles on key developments in medical science and the organisation of health care. We explore the campaigning and advocacy work of the journal through several indicative areas where science and policy meet, balancing national and global themes over the 19th and 20th centuries. Themes include the raising of professional standards; environmental health in urbanising Britain; the transformation of surgery; the emergence of tropical medicine; the science and politics of vaccination; the advance towards universal health coverage; and the transition from international to global health. In the imperial era, both the journal's research reports and editorial stance were sometimes inflected with colonial attitudes, although it consistently presented medicine as an international endeavour. The Lancet's blend of science and advocacy demonstrates a track record of campaigning for medicine in the cause of social betterment.

173. Women, power, and cancer: a Lancet Commission.

作者: Ophira Ginsburg.;Verna Vanderpuye.;Ann Marie Beddoe.;Nirmala Bhoo-Pathy.;Freddie Bray.;Carlo Caduff.;Narjust Florez.;Ibtihal Fadhil.;Nazik Hammad.;Shirin Heidari.;Ishu Kataria.;Somesh Kumar.;Erica Liebermann.;Jennifer Moodley.;Miriam Mutebi.;Deborah Mukherji.;Rachel Nugent.;Winnie K W So.;Enrique Soto-Perez-de-Celis.;Karla Unger-Saldaña.;Gavin Allman.;Jenna Bhimani.;María T Bourlon.;Michelle A B Eala.;Peter S Hovmand.;Yek-Ching Kong.;Sonia Menon.;Carolyn D Taylor.;Isabelle Soerjomataram.
来源: Lancet. 2023年402卷10417期2113-2166页

174. CAR T-cell therapy in autoimmune diseases.

作者: Georg Schett.;Andreas Mackensen.;Dimitrios Mougiakakos.
来源: Lancet. 2023年402卷10416期2034-2044页
Despite the tremendous progress in the clinical management of autoimmune diseases, many patients do not respond to the currently used treatments. Autoreactive B cells play a key role in the pathogenesis of autoimmune diseases, such as systemic lupus erythematosus, rheumatoid arthritis, and multiple sclerosis. B-cell-depleting monoclonal antibodies, such as rituximab, have poor therapeutic efficacy in autoimmune diseases, mainly due to the persistence of autoreactive B cells in lymphatic organs and inflamed tissues. The adoptive transfer of T cells engineered to target tumour cells via chimeric antigen receptors (CARs) has emerged as an effective treatment modality in B-cell malignancies. In the last 2 years treatment with autologous CAR T cells directed against the CD19 antigen has been introduced in therapy of autoimmune disease. CD19 CAR T cells induced a rapid and sustained depletion of circulating B cells, as well as in a complete clinical and serological remission of refractory systemic lupus erythematosus and dermatomyositis. In this paper, we discuss the evolving strategies for targeting autoreactive B cells via CAR T cells, which might be used for targeted therapy in autoimmune diseases.

175. Glaucoma: now and beyond.

作者: Hari Jayaram.;Miriam Kolko.;David S Friedman.;Gus Gazzard.
来源: Lancet. 2023年402卷10414期1788-1801页
The glaucomas are a group of conditions leading to irreversible sight loss and characterised by progressive loss of retinal ganglion cells. Although not always elevated, intraocular pressure is the only modifiable risk factor demonstrated by large clinical trials. It remains the leading cause of irreversible blindness, but timely treatment to lower intraocular pressure is effective at slowing the rate of vision loss from glaucoma. Methods for lowering intraocular pressure include laser treatments, topical medications, and surgery. Although modern surgical innovations aim to be less invasive, many have been introduced with little supporting evidence from randomised controlled trials. Many cases remain undiagnosed until the advanced stages of disease due to the limitations of screening and poor access to opportunistic case finding. Future research aims to generate evidence for intraocular pressure-independent neuroprotective treatments, personalised treatment through genetic risk profiling, and exploration of potential advanced cellular and gene therapies.

176. Hepatitis C.

作者: Marianne Martinello.;Sunil S Solomon.;Norah A Terrault.;Gregory J Dore.
来源: Lancet. 2023年402卷10407期1085-1096页
Hepatitis C virus (HCV) is a hepatotropic RNA virus that can cause acute and chronic hepatitis, with progressive liver damage resulting in cirrhosis, decompensated liver disease, and hepatocellular carcinoma. In 2016, WHO called for the elimination of HCV infection as a public health threat by 2030. Despite some progress, an estimated 57 million people were living with HCV infection in 2020, and 300 000 HCV-related deaths occur per year. The development of direct-acting antiviral therapy has revolutionised clinical care and generated impetus for elimination, but simplified and broadened HCV screening, enhanced linkage to care, and higher coverage of treatment and primary prevention strategies are urgently required.

177. Primary brain tumours in adults.

作者: Martin J van den Bent.;Marjolein Geurts.;Pim J French.;Marion Smits.;David Capper.;Jacoline E C Bromberg.;Susan M Chang.
来源: Lancet. 2023年402卷10412期1564-1579页
The most frequent adult-type primary CNS tumours are diffuse gliomas, but a large variety of rarer CNS tumour types exists. The classification of these tumours is increasingly based on molecular diagnostics, which is reflected in the extensive molecular foundation of the recent WHO 2021 classification of CNS tumours. Resection as extensive as is safely possible is the cornerstone of treatment in most gliomas, and is now also recommended early in the treatment of patients with radiological evidence of histologically low-grade tumours. For the adult-type diffuse glioma, standard of care is a combination of radiotherapy and chemotherapy. Although treatment with curative intent is not available, combined modality treatment has resulted in long-term survival (>10-20 years) for some patients with isocitrate dehydrogenase (IDH) mutant tumours. Other rarer tumours require tailored approaches, best delivered in specialised centres. Targeted treatments based on molecular alterations still only play a minor role in the treatment landscape of adult-type diffuse glioma, and today are mainly limited to patients with tumours with BRAFV600E (ie, Val600Glu) mutations. Immunotherapy for CNS tumours is still in its infancy, and so far, trials with checkpoint inhibitors and vaccination studies have not shown improvement in patient outcomes in glioblastoma. Current research is focused on improving our understanding of the immunosuppressive tumour environment, the molecular heterogeneity of tumours, and the role of tumour microtube network connections between cells in the tumour microenvironment. These factors all appear to play a role in treatment resistance, and indicate that novel approaches are needed to further improve outcomes of patients with CNS tumours.

178. Dilated cardiomyopathy: causes, mechanisms, and current and future treatment approaches.

作者: Stephane Heymans.;Neal K Lakdawala.;Carsten Tschöpe.;Karin Klingel.
来源: Lancet. 2023年402卷10406期998-1011页
Dilated cardiomyopathy is conventionally defined as the presence of left ventricular or biventricular dilatation or systolic dysfunction in the absence of abnormal loading conditions (eg, primary valve disease) or significant coronary artery disease sufficient to cause ventricular remodelling. This definition has been recognised as overly restrictive, as left ventricular hypokinesis without dilation could be the initial presentation of dilated cardiomyopathy. The causes of dilated cardiomyopathy comprise genetic (primary dilated cardiomyopathy) or acquired factors (secondary dilated cardiomyopathy). Acquired factors include infections, toxins, cancer treatment, endocrinopathies, pregnancy, tachyarrhythmias, and immune-mediated diseases. 5-15% of patients with acquired dilated cardiomyopathy harbour a likely pathogenic or pathogenic gene variant (ie, gene mutation). Therefore, the diagnostic tests and therapeutic approach should always consider both genetic and acquired factors. This Seminar will focus on the current multidimensional diagnostic and therapeutic approach and discuss the underlying pathophysiology that could drive future treatments aiming to repair or replace the existing gene mutation, or target the specific inflammatory, metabolic, or pro-fibrotic drivers of genetic or acquired dilated cardiomyopathy.

179. Scientific advances and the end of tuberculosis: a report from the Lancet Commission on Tuberculosis.

作者: Michael Reid.;Yvan Jean Patrick Agbassi.;Nimalan Arinaminpathy.;Alyssa Bercasio.;Anurag Bhargava.;Madhavi Bhargava.;Amy Bloom.;Adithya Cattamanchi.;Richard Chaisson.;Daniel Chin.;Gavin Churchyard.;Helen Cox.;Claudia M Denkinger.;Lucica Ditiu.;David Dowdy.;Mark Dybul.;Anthony Fauci.;Endalkachew Fedaku.;Mustapha Gidado.;Mark Harrington.;Janika Hauser.;Petra Heitkamp.;Nick Herbert.;Ani Herna Sari.;Philip Hopewell.;Emily Kendall.;Aamir Khan.;Andrew Kim.;Irene Koek.;Sergiy Kondratyuk.;Nalini Krishnan.;Chu-Chang Ku.;Erica Lessem.;Erin V McConnell.;Payam Nahid.;Matt Oliver.;Madhukar Pai.;Mario Raviglione.;Theresa Ryckman.;Marco Schäferhoff.;Sachin Silva.;Peter Small.;Guy Stallworthy.;Zelalem Temesgen.;Kitty van Weezenbeek.;Anna Vassall.;Gustavo E Velásquez.;Nandita Venkatesan.;Gavin Yamey.;Armand Zimmerman.;Dean Jamison.;Soumya Swaminathan.;Eric Goosby.
来源: Lancet. 2023年402卷10411期1473-1498页

180. CFTR modulator therapy: transforming the landscape of clinical care in cystic fibrosis.

作者: Jennifer L Taylor-Cousar.;Paul D Robinson.;Michal Shteinberg.;Damian G Downey.
来源: Lancet. 2023年402卷10408期1171-1184页
Following discovery of the cystic fibrosis transmembrane conductance regulator (CFTR) gene in 1989 and subsequent elucidation of the varied CFTR protein abnormalities that result, a new era of cystic fibrosis management has emerged-one in which scientific principles translated from the bench to the bedside have enabled us to potentially treat the basic defect in the majority of children and adults with cystic fibrosis, with a resultant burgeoning adult cystic fibrosis population. However, the long-term effects of these therapies on the multiple manifestations of cystic fibrosis are still under investigation. Understanding the effects of modulators in populations excluded from clinical trials is also crucial. Furthermore, establishing appropriate disease measures to assess efficacy in the youngest potential trial participants and in those whose post-modulator lung function is in the typical range for people without chronic lung disease is essential for continued drug development. Finally, recognising that a health outcome gap has been created for some people and widened for others who are not eligible for, cannot tolerate, or do not have access to modulators is important.
共有 4075 条符合本次的查询结果, 用时 2.7928198 秒