Robert Kokou Dowou
57220119787
Publications - 2
Global burden of cancer in children and adolescents aged 0–19 years, 1990–2023: a systematic analysis for the Global Burden of Disease Study 2023
Jasvinder Singh Bhatti
Sayeh Ezzikouri
Ali Hasanpour- Dehkordi
Takeshi Fukumoto
Seyyed Shamsadin Athari
Hala Rashad Elhabashy
Aleksandr Y. Aravkin
Paul Narh Doku
Dariush Haghmorad
Theophilus I. Emeto
Adeniyi Francis Fagbamigbe
Nermin Ghith
Anis Ahmad Chaudhary
Mahwish Arooj
Hamidreza Hasani
Robert Kaba Alhassan
Salahdein Aburuz
Lucas Guimarães Abreu
Saeid Anvari
Muhammad Sohail Afzal
Jonathan M. Kocarnik
Mosab Arafat
Morenike Oluwatoyin Folayan
Hanadi Al Hamad
Ayesha Fahim
Mohammad Farahmand
Lisa M. Force
Adewale Oluwaseun Fadaka
Nadia M. Hamdy
Demelash Areda
Veer Bala Gupta
Maha Moh'd Wahbi Atout
Natalie Pritchett
Souad Bouaoud
Ayman Ahmed
Aso Mohammad Darwesh
Cem Bilgin
Dong Woo Choi
Wafa A. Aldhaleei
Awais Altaf
Ferrán Catalá-López
Danish Ahmad
Bashir Dabo
Rakhi Dandona
Mohammed Albashtawy
Mohamed Abouzid
Omotayo Francis Fagbule
Shirin Barati
Soham Bandyopadhyay
Ahmed Y. Azzam
Abdulfatai Aremu
Teferi Gebru Gebremeskel
Arvin Haj-Mirzaian
Catherine Bisignano
Aragaw Tesfaw Desale
Benedetta Armocida
Hasan Aalruz
Kayleigh Bhangdia
Isaac Sunday Chukwu
Md Kamrul Hasan
Promit Ananyo Chakraborty
Louise Penberthy
Maryam Bemanalizadeh
Robert Kokou Dowou
Giulia Carreras
Xiaochen Dai
Maysaa El Sayed Zaki
Johannes Haubold
Mohammad Asghari-Jafarabadi
Fatemeh Afrashteh
John Dube
Ali Hasanpour- Dehkordi
Shahkaar Aziz
Logan M. Glasstetter
Genanew K. Getahun
Sri Harsha Boppana
Alistair Acheson
Chiranjib Chakraborty
Saroja Devi Geetha
Razieh Bahreini
Yohannes Habtegiorgis Abate
Sabah Al-Marwani
Mohammad Farahmand
Mohammad Mahdi Bastan
Samuel Demissie Darcho
Thao Huynh Phuong Do
Miglas Welay Gebregergis
Lee Deitesfeld
Abdel Rahman E'mar
Mohammed Elshaer
Lemessa Assefa A. Ayana
Chadi Eltaha
Awoke Derbie Habteyohannes
Abid Ali
Safwat Aly
Nguyen Hoang Anh
Andrew Crist
Miranda L. May
Maha Moh d.Wahbi Atout
Hasan Aalruz
Syed Anees Ahmed
Demelash Areda
Mohammad Farahmand
Lalit Dandona
Karem H. Alzoubi
Yasser Bustanji
Publication Name: Lancet
Publication Date: 2026-04-04
Volume: 407
Issue: 10536
Page Range: 1360-1373
Description:
Background Information on childhood cancer burden is crucial for effective cancer policy planning. Unfortunately, observed paediatric cancer data are not available in every country, and previous global burden estimates have not discretely reported several common cancers of childhood. We aimed to inform efforts to address childhood cancer burden globally by analysing results from the Global Burden of Diseases, Injuries, and Risk Factors Study (GBD) 2023, which now include nine additional cancer causes compared with previous GBD analyses. Methods GBD 2023 data sources for cancer estimation included population-based cancer registries, vital registration systems, and verbal autopsies. For childhood cancers (defined as those occurring at ages 0–19 years), mortality was estimated using cancer-specific ensemble models and incidence was estimated using mortality estimates and modelled mortality-to-incidence ratios (MIRs). Years of life lost (YLLs) were estimated by multiplying age-specific cancer deaths by the standard life expectancy at the age of death. Prevalence was estimated using survival estimates modelled from MIRs and multiplied by sequelae-specific disability weights to estimate years lived with disability (YLDs). Disability-adjusted life-years (DALYs) were estimated as the sum of YLLs and YLDs. Estimates are presented globally and by geographical and resource groupings, and all estimates are presented with 95% uncertainty intervals (UIs). Findings Globally, in 2023, there were an estimated 377 000 incident childhood cancer cases (95% UI 288 000–489 000), 144 000 deaths (131 000–162 000), and 11·7 million (10·7–13·2) DALYs due to childhood cancer. Deaths due to childhood cancer decreased by 27·0% (15·5–36·1) globally, from 197 000 (173 000–218 000) in 1990, but increased in the WHO African region by 55·6% (25·5–92·4), from 31 500 (24 900–38 500) to 49 000 (42 600–58 200) between 1990 and 2023. In 2023, age-standardised YLLs due to childhood cancer were inversely correlated with country-level Socio-demographic Index. Childhood cancer was the eighth-leading cause of childhood deaths and the ninth-leading cause of DALYs among all cancers in 2023. The percentage of DALYs due to uncategorised childhood cancers was reduced from 26·5% (26·5–26·5) in GBD 2017 to 10·5% (8·1–13·1) with the addition of the nine new cancer causes. Target cancers for the WHO Global Initiative for Childhood Cancer (GICC) comprised 47·3% (42·2–52·0) of global childhood cancer deaths in 2023. Interpretation Global childhood cancer burden remains a substantial contributor to global childhood disease and cancer burden and is disproportionately weighted towards resource-limited settings. The estimation of additional cancer types relevant in childhood provides a step towards alignment with WHO GICC targets. Efforts to decrease global childhood cancer burden should focus on addressing the inequities in burden worldwide and support comprehensive improvements along the childhood cancer diagnosis and care continuum. Funding St Jude Children's Research Hospital, Gates Foundation, and St Baldrick's Foundation.
Open Access: Yes
Global burden of metabolic dysfunction-associated steatotic liver disease, 1990–2023, and projections to 2050: a systematic analysis for the Global Burden of Disease Study 2023
Jasvinder Singh Bhatti
Usha Adiga
Stephen E. Congly
Neeraj Bhala
Karolina Akinosoglou
Saleh A. Alqahtani
Seyyed Shamsadin Athari
Juan Pablo Arab
Aleksandr Y. Aravkin
Bruce B. Duncan
Archith Boloor
Catalina Liliana Andrei
Ahmed Abu-Zaid
Fadwa Naji Alhalaiqa
Oyewole Christopher Durojaiye
Ferry Efendi
Anis Ahmad Chaudhary
Sushil Dohare
Ajeet Singh Bhadoria
Vijay Kumar Chattu
Floriane Ausloos
Muhammad Sohail Afzal
Isaac Yeboah Addo
Ashish D. Badiye
Tahira Ashraf
Yogesh Bahurupi
Luis Antonio Diaz
Nasir Abbas
Anton A. Artamonov
Hubert Amu
Sheikh Mohammad Alif
Charles Oluwaseun Adetunji
Demelash Areda
Wirawan Adikusuma
Shady Abohashem
Maha Moh'd Wahbi Atout
Awais Altaf
Deanna Anderlini
Zahid A. Butt
Walid A. Al-Zyoud
Ismael Campos-Nonato
Omid Dadras
Foolad Eghbali
Jalal Arabloo
Narasimha M. Beeraka
Nelson Alvis-Guzman
Omar Ali Mohammed Al Zaabi
Fariba Dorostkar
Diana Fernanda Bejarano Ramirez
Hasan Aalruz
Amadou Barrow
Isaac Sunday Chukwu
Rajaa M. Al-Raddadi
Robert Kokou Dowou
Richard Gyan Aboagye
Xiaochen Dai
Arkadeep Dhali
Najim Z. Alshahrani
Menayit Tamrat Dresse
Mohammed Ahmed Akkaif
Patrick R. Ching
Pankaj Bhardwaj
Fatemeh Chichagi
Shahkaar Aziz
Bryan Chong
Shewatatek Melaku Asefa
Felix Busch
Mainak Bardhan
Ajay Nagesh Bhat
Pojsakorn Danpanichkul
Amani Alansari
Joshua Chadwick
Yaser Mohammed Al-Worafi
Filippos Anagnostakis
Behrad Eftekhari
Soeun Kim
Amol S. Dhane
Khushboo Bisht
Jiyeon Oh
Mohammad Mahdi Bastan
Melak Gedamu Beyene
Ashel Chelsea Dsouza
Sandip Chakraborty
Abiye Assefa Berihun
Abdel Rahman E’mar
Mohammad Daud Ali
Shahid Bashir
Jae Il Shin
Huyen Phuc Do
Hasan Aalruz
Syed Anees Ahmed
Haroon Ahmed
Abisola Esther Abdulmalik
Omar Al Ta'ani
Maha Moh'd Wahbi Atout
Salah Al Awaidy
Luis Alberto Cámera
Giovanni Addolorato
Márcia Carvalho
Mohammad Khursheed Alam
Yasser Bustanji
Jaffar A. Al-Tawfiq
Publication Name: Lancet Gastroenterology and Hepatology
Publication Date: 2026-06-01
Volume: 11
Issue: 6
Page Range: 463-494
Description:
Background: Metabolic dysfunction-associated steatotic liver disease (MASLD), previously known as non-alcoholic fatty liver disease, is one of the most prevalent liver diseases globally, contributing to both economic and health-related challenges. We aimed to evaluate the global, regional, and national burden of MASLD from 1990 to 2023, quantify the contribution of identified modifiable risk factors, and project future prevalence up to the year 2050. Methods: Estimates of MASLD prevalence and disability-adjusted life-years (DALYs) were produced by age, sex, region, Socio-demographic Index (SDI), and Healthcare Access and Quality (HAQ) index across 204 countries and territories from 1990 to 2023 as part of the Global Burden of Diseases, Injuries, and Risk Factors Study (GBD) 2023. The MASLD burden attributable to three risk factors (smoking, high BMI, and high fasting plasma glucose) was assessed as part of the GBD comparative risk assessment. As a secondary analysis, we used these estimates to forecast MASLD prevalence up to 2050 using fasting plasma glucose and mean BMI as predictors. Furthermore, to examine the relative contributions of population ageing, population growth, and changes in MASLD prevalence rate to the forecasted changes in case counts from 2023 to 2050, we conducted a decomposition analysis. Findings: In 2023, approximately 1·3 billion (95% uncertainty interval [UI] 1·2 to 1·4) individuals were estimated to be living with MASLD (ie, 16·1% of the global population), with an age-standardised prevalence rate of 14 429·3 (95% UI 13 268·3 to 15 990·6) per 100 000 population, representing a percentage increase of 142·7% (95% UI 139·2 to 146·7) in crude numbers from 1990 (0·5 billion [0·5 to 0·6]) and of 28·6% (27·8 to 29·5) in the rate (11 217·2 [10 276·8 to 12 467·0] per 100 000 in 1990). An estimated 3·6 million (2·8 to 4·5) total DALYs were attributable to MASLD worldwide in 2023, corresponding to an age-standardised DALY rate of 39·6 (31·2 to 49·9) per 100 000 population. Despite a 116·3% (93·3 to 139·4) increase in crude DALYs (from 1·7 million [1·3 to 2·1] in 1990), its age-standardised estimate remained consistent (1·8% [–8·6 to 12·8]) from 1990 (38·9 [30·1 to 49·8] per 100 000) to 2023. There was substantial variation in age-standardised estimates across regions. North Africa and the Middle East had the highest prevalence rate (29 246·1 [26 848·3 to 32 048·7] per 100 000) and Andean Latin America showed the highest DALY rate (152·3 [114·1 to 194·7] per 100 000). By contrast, the high-income Asia Pacific region had the lowest prevalence rate (8653·5 [7923·7 to 9592·8] per 100 000) and east Asia had the lowest DALY rate (16·3 [13·5 to 19·9] per 100 000) among all GBD regions. North Africa and the Middle East showed disproportionately higher prevalence rates relative to other regions with similar SDIs. Lower SDIs and HAQs were associated with higher age-standardised DALY rates. The age-standardised prevalence rate was consistently higher in males (15 616·4 [14 349·2 to 17 263·3] per 100 000 people in 2023) than in females (13 245·2 [12 132·0 to 14 692·6] per 100 000 people), and peaked at age 80–84 years in both sexes. The number of MASLD prevalent cases was the highest in younger adults, peaking at age 35–39 years for males and age 55–59 years for females. Among the risk factors for MASLD, high fasting plasma glucose presented the largest contribution to the age-standardised DALY rate of total MASLD in 2023 (2·2 [95% UI 1·6 to 3·1] per 100 000 people), followed by high BMI (1·4 [0·6 to 2·4] per 100 000 people) and smoking (1·0 [0·3 to 1·8] per 100 000 people). Our forecasting model estimates that 1·8 billion (95% UI 1·6 to 2·0) individuals are likely to have MASLD by 2050, representing a 42·0% increase from 2023. The age-standardised prevalence rate is expected to increase to 15 774·9 (95% UI 14 613·9 to 17 336·2) per 100 000 people in 2050, representing an average annual percentage change of 0·3% (95% UI 0·3–0·3). According to our decomposition analysis, this change will be primarily due to population growth, particularly in sub-Saharan Africa and North Africa and Middle East, and less by population ageing or epidemiological change. Interpretation: With a global prevalence of 16·1% and approximately 1·3 billion people already living with MASLD in 2023, the condition has and will continue to have substantial health and economic impacts worldwide. An inverse association between the HAQ Index and age-standardised DALY rates suggests that countries with lower health-care access and quality might be less well positioned to manage the growing MASLD burden, underscoring the need for strengthened health-system capacity in these settings. Funding: Gates Foundation.
Open Access: Yes