Over 110 yr ago, the first description of a West Indian student with sickle cell disease (SCD) was reported by Dr Herrick in Chicago, USA, opening the way to deciphering the disease from its molecular basis to its complex systemic and multicellular pathophysiology1. SCD is characterized by a single mutation in the gene encoding for β-globin chain of haemoglobin which, in the homozygous state, results in a cascade of events starting with the polymerization of the mutated haemoglobin (HbS) when deoxygenated. Multiple downstream and interrelated biological processes contribute to the clinical expression of SCD, among which chronic inflammation, hypercoagulability, ischaemic injury, functional nitric oxide deficiency, endothelial, platelet and leucocyte activation and oxidative stress play important roles. Painful vaso-occlusion, chronic haemolytic anaemia, susceptibility to infections and systemic vasculopathy are among the main clinical consequences of the disease2. Patients with SCD experience considerable morbidity from both acute and chronic complications that lead to end-organ damage and reduced life expectancy. In addition, disease-related complications starting in infancy significantly impair physical, mental and psychosocial aspects of health-related quality of life3.
Today, SCD is the most common severe monogenic disorder in the world, with a high prevalence in sub-Saharan Africa, parts of Mediterranean, India and in the Middle East4. In South Asia, the highest prevalence of the disease is in India, where over 20 million patients with SCD live. SCD prevalence in India has been quantified through various approaches, including village-level prevalence surveys as well as State-wide screening programmes5, focussing on groups with a high prevalence of the βS allele. Screening generally relies on Hb solubility test at the point of care, but this test does not distinguish sickle cell trait (HbAS) from SCD and therefore requires further testing2. Pilot projects of new-born screening programmes for SCD in the States of Gujarat, Maharashtra and Chhattisgarh resulted in figures of HbAS prevalence ranging from two to 40 per cent2. The highest frequency of the βs allele is found across Central India (up to 10%), from South-Eastern Gujarat to South-Western Odisha4. Altogether, India has been ranked the country with the second highest numbers of predicted SCD births, with 42,016 [interquartile range (IQR): 35,347-50,919] newborns estimated to have been born with sickle cell anaemia in 20104.
SCD is characterized by considerable variability in clinical severity. This variability can partly be explained by genetic modifiers, including factors that affect HbF level and co-inheritance of α-thalassaemia. The Arab–India haplotype is associated with high HbF levels and found in an area extending from the eastern coast of Saudi Arabia and East Africa to India2. It is usually associated with a milder phenotype than that associated with the four African haplotypes (Benin, Bantu, Cameroon and Senegal haplotypes) and is prevalent in the tribal populations in India6. Early descriptions of SCD in India were focussed on these tribal populations and hence, SCD in India was initially thought to be milder than in other countries5,6. However, the latter data suggest that the severity of the disease can be compared to that in African countries. In a study of 833 paediatric SCD patients in Nagpur, common SCD-related complications, including acute pain, severe anaemia, stroke, splenic sequestration, acute chest syndrome and meningitis, were more frequent6 than in the Cooperative Study of SCD, which prospectively investigated the natural history of SCD in the United States between 1978 and 19887.
Early, simple, cost-effective measures can change the prognosis of SCD in childhood but are challenging in low-income, high-burden settings. Neonatal screening for early diagnosis, penicillin prophylaxis and immunization to control the infectious risk along with parents and medical community education have dramatically decreased SCD-related childhood mortality in high-income countries, where more than 90 per cent of children with SCD survive to adulthood8. Such measures are however, not widely implemented, particularly in low-income countries, where 50-80 per cent of children with SCD die before reaching five years of age9. In places without new-born screening programmes, the initial diagnosis of SCD typically occurs at approximately 21 months of age2. The initial presentation is often a fatal infection or acute anaemia, resulting from an acute splenic sequestration crisis. In a study performed in Gujarat, India, around 20 per cent of children with SCD died by two years of age and 30 per cent children from tribal areas died before they reached adulthood10. In India, there is important regional variation in the implementation of follow up strategies including penicillin prophylaxis, immunization against pneumococcus and comprehensive care. Additional basic health measures include access to safe transfusion and opioids for pain relief. Both are needed for SCD patients who suffer, among other complications, from recurrent painful vaso-occlusive episodes and exacerbation of chronic anaemia.
Blood transfusion is established as an important treatment in some acute situations, such as severe anaemia and acute chest syndrome, and also to prevent some chronic complications, such as cerebrovascular disease. The availability of blood transfusion varies widely across South Asia, as only a few patients have access to a safe and reliable supply of blood. There are State-run blood transfusion services in Sri Lanka, Bhutan and the Maldives, but most blood is supplied by charitable and private blood banks in Bangladesh, India and Pakistan. As per a modelling study, India is estimated to have the biggest unmet need for blood units in the world11, with important implications for the treatment of SCD. Making reliable blood transfusion services available would improve the standard of care for patients with SCD and facilitate the development of curative treatments, including gene therapy and bone marrow transplantation.
Hydroxyurea (HU) was the first licensed disease-modifying therapy for SCD. Clinical studies were first undertaken more than 30 yr ago in the USA and Europe and have shown convincing and consistent evidence of benefit, both for acute (reduced incidence of acute pain, acute chest syndrome and blood transfusion) and chronic complications (reduced risk of progressive cerebrovascular disease, improved hypoxia and prolonged survival)2. In low-income countries in malaria-endemic sub-Saharan Africa, the safety and efficacy of HU have also been demonstrated12. In India, prospective trials of HU therapy, mostly using a fixed low-dose (10 mg/kg/day) regimen, demonstrated a significant reduction in vaso-occlusive crises and transfusion requirements13. A dose-dependent effect was also shown in sub-Saharan Africa, opening the prospect of additional benefits of higher dose in other settings, like India14. Randomized studies in India are still needed to replicate these results given the many genetic and environmental differences that may influence outcomes15.
Irrespective of the question of optimal dosage, HU is underutilized both in low- and high-resource countries because of healthcare infrastructure deficiencies, poor compliance and fear of toxicity. In a review by Jain and Mohanty6, poor compliance with HU in India was attributed to physician’s concerns of potential long-term neoplastic effects and lack of experience of primary attending physician with HU therapy. HU-related carcinogenicity, teratogenicity and reduced fertility have not been confirmed by follow up studies, and no report of increased risk of neoplasia has emerged16. In particular, worries about the toxic effect on spermatogenesis may have triggered patients to decline HU17. Recent reassuring data on fertility have shown that the effect on spermatogenesis is reversible, including when HU is given to pre-pubertal boys18. Altogether, the benefit/risk ratio of HU in SCD argues very strongly for its wider use. Strong evidence-based guidelines in India could reassure primary attending physicians and increase the knowledge on the beneficial effect of HU in SCD.
Beyond sickle haemoglobin polymerization, the unravelling of many aspects of SCD pathophysiology, such as the increased adhesion of red cells to the vascular endothelium or platelet activation, has resulted in an increasing number of pre-clinical and clinical drug trials registered every year. Many products that target one or more of the mechanisms of the disease process are currently in phase II or phase III trials19. Most of these trials are multicentric and international but face the challenge of low enrolment, resulting in early termination. The recent completion of large, multicentre, multinational clinical trials has resulted in the marketing in high-income countries of new drugs for the treatment of SCD such as P-selectin blockers, L-glutamine and voxelotor19. These drugs are however, available to date at unaffordable costs for patients living outside high-income countries and currently seem to have a limited efficacy. Given the complexity of SCD and the wide range of possible complications, a tailored multidrug approach will probably be the best option for SCD patients, posing again the question of drug access in low- and middle-income countries in the future.
The only curative therapy in SCD so far is the replacement of the genetic defect in the haematopoietic stem cells (HSCs). This can be achieved either through allogeneic HSC transplant from an HLA-matched sibling (with or without myeloablative conditioning), through HSC transplant using a haplo-identical donor or through auto-HSC transplant using gene therapy. Although HSC transplant may be performed in high-burden, low-income areas18, the accessibility of curative therapies still needs to be addressed. In the short term, improving the availability of proven therapies, such as penicillin prophylaxis and HU, is the quickest and easily achievable way to increase the life expectancy of patients with SCD and, importantly, quality of life.
Irrespective of the genetic influence on disease expression, evidence suggests that poverty and low socio-economic status may result in adverse outcomes in the disease20. Environmental factors, home environment, nutrition and access to care influence the severity of the disease. In India, SCD is particularly prevalent in Scheduled Tribe and Scheduled Caste populations, which constitute the most socio-economically disadvantaged communities in the country5. When the COVID-19 pandemic has been tackled, in India and elsewhere, addressing the survival and quality of life of the many patients with SCD will be a priority.
Footnotes
Conflicts of Interest: None.
References
- 1.Savitt TL, Goldberg MF. Herrick's 1910 case report of sickle cell anemia. The rest of the story. JAMA. 1989;261:266–71. [PubMed] [Google Scholar]
- 2.Kato GJ, Piel FB, Reid CD, Gaston MH, Ohene-Frempong K, Krishnamurti L, et al. Sickle cell disease. Nat Rev Dis Primers. 2018;4:18010. doi: 10.1038/nrdp.2018.10. [DOI] [PubMed] [Google Scholar]
- 3.Panepinto JA. Health-related quality of life in patients with hemoglobinopathies. Hematology Am Soc Hematol Educ Program. 2012;2012:284–9. doi: 10.1182/asheducation-2012.1.284. [DOI] [PubMed] [Google Scholar]
- 4.Piel FB, Patil AP, Howes RE, Nyangiri OA, Gething PW, Dewi M, et al. Global epidemiology of sickle haemoglobin in neonates:A contemporary geostatistical model-based map and population estimates. Lancet. 2013;381:142–51. doi: 10.1016/S0140-6736(12)61229-X. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 5.Hockham C, Bhatt S, Colah R, Mukherjee MB, Penman BS, Gupta S, et al. The spatial epidemiology of sickle-cell anaemia in India. Sci Rep. 2018;8:17685. doi: 10.1038/s41598-018-36077-w. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 6.Jain D, Mohanty D. Clinical manifestations of sickle cell disease in India:Misconceptions and reality. Curr Opin Hematol. 2018;25:171–6. doi: 10.1097/MOH.0000000000000422. [DOI] [PubMed] [Google Scholar]
- 7.Jain D, Arjunan A, Sarathi V, Jain H, Bhandarwar A, Vuga M, et al. Clinical events in a large prospective cohort of children with sickle cell disease in Nagpur, India:Evidence against a milder clinical phenotype in India. Pediatr Blood Cancer. 2016;63:1814–21. doi: 10.1002/pbc.26085. [DOI] [PubMed] [Google Scholar]
- 8.Quinn CT, Rogers ZR, McCavit TL, Buchanan GR. Improved survival of children and adolescents with sickle cell disease. Blood. 2010;115:3447–52. doi: 10.1182/blood-2009-07-233700. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 9.Grosse SD, Odame I, Atrash HK, Amendah DD, Piel FB, Williams TN. Sickle cell disease in Africa:A neglected cause of early childhood mortality. Am J Prev Med. 2011;41(6 Suppl 4):S398–405. doi: 10.1016/j.amepre.2011.09.013. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 10.Saxena D, Yasobant S, Golechha M. Situational analysis of sickle cell disease in Gujarat, India. Indian J Community Med. 2017;42:218–21. doi: 10.4103/ijcm.IJCM_284_16. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 11.Roberts N, James S, Delaney M, Fitzmaurice C. The global need and availability of blood products:A modelling study. Lancet Haematol. 2019;6:e606–15. doi: 10.1016/S2352-3026(19)30200-5. [DOI] [PubMed] [Google Scholar]
- 12.Opoka RO, Ndugwa CM, Latham TS, Lane A, Hume HA, Kasirye P, et al. Novel use of Hydroxyurea in an African Region with Malaria (NOHARM):A trial for children with sickle cell anemia. Blood. 2017;130:2585–93. doi: 10.1182/blood-2017-06-788935. [DOI] [PubMed] [Google Scholar]
- 13.Darshana T, Rees D, Premawardhena A. Hydroxyurea and blood transfusion therapy for sickle cell disease in South Asia:Inconsistent treatment of a neglected disease. Orphanet J Rare Dis. 2021;16:148. doi: 10.1186/s13023-021-01781-w. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 14.John CC, Opoka RO, Latham TS, Hume HA, Nabaggala C, Kasirye P, et al. Hydroxyurea dose escalation for sickle cell anemia in Sub-Saharan Africa. N Engl J Med. 2020;382:2524–33. doi: 10.1056/NEJMoa2000146. [DOI] [PubMed] [Google Scholar]
- 15.Power-Hays A, Ware RE. Effective use of hydroxyurea for sickle cell anemia in low-resource countries. Curr Opin Hematol. 2020;27:172–80. doi: 10.1097/MOH.0000000000000582. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 16.Voskaridou E, Christoulas D, Bilalis A, Plata E, Varvagiannis K, Stamatopoulos G, et al. The effect of prolonged administration of hydroxyurea on morbidity and mortality in adult patients with sickle cell syndromes:results of a 17-year, single-center trial (LaSHS) Blood. 2010;115:2354–63. doi: 10.1182/blood-2009-05-221333. [DOI] [PubMed] [Google Scholar]
- 17.Sahoo LK, Kullu BK, Patel S, Patel NK, Rout P, Purohit P, et al. Study of seminal fluid parameters and fertility of male sickle cell disease patients and potential impact of hydroxyurea treatment. J Assoc Physicians India. 2017;65:22–5. [PubMed] [Google Scholar]
- 18.Joseph L, Jean C, Manceau S, Chalas C, Arnaud C, Kamdem A, et al. Effect of hydroxyurea exposure before puberty on sperm parameters in males with sickle cell disease. Blood. 2021;137:826–9. doi: 10.1182/blood.2020006270. [DOI] [PubMed] [Google Scholar]
- 19.Salinas Cisneros G, Thein SL. Research in sickle cell disease:From bedside to bench to bedside. Hemasphere. 2021;5:e584. doi: 10.1097/HS9.0000000000000584. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 20.Tewari S, Brousse V, Piel FB, Menzel S, Rees DC. Environmental determinants of severity in sickle cell disease. Haematologica. 2015;100:1108–16. doi: 10.3324/haematol.2014.120030. [DOI] [PMC free article] [PubMed] [Google Scholar]