Long-Term Risk of Infections After Treatment of Childhood Leukemia: A Population-Based Cohort Study Using Administrative Health Data

Pelland‐Marcotte, Marie‐Claude; Pole, Jason D.; Hwee, Jeremiah; Sutradhar, Rinku; Nathan, Paul C.; Sung, Lillian

doi:10.1200/jco.19.00570

Cited by 14 publications

(11 citation statements)

References 48 publications

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“…While the cellular immune response is reinforced by increased hematopoiesis following induction chemotherapy our data confirms substantial reduction in the humoral innate immune response in line with increased susceptibility to infection [36,37]. Importantly, elements of this post-apoptotic immunosuppressed humoral microenvironment, such as elevated adenosine, may play an essential role in the regeneration of the hematopoietic progenitor cell pool [38].…”

Section: Discussionsupporting

confidence: 65%

Multi-omic profiling of the leukemic microenvironment shows bone marrow interstitial fluid is distinct from peripheral blood plasma

Nierves

Guo

Chen

et al. 2022

Preprint

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The bone marrow is the place of hematopoiesis with a microenvironment that supports lifelong maintenance of stem cells and high proliferation. It is not surprising that this environment is also favourable for malignant cells emerging in the bone marrow or metastasizing to it. While the cellular composition of the bone marrow microenvironment has been extensively studied, the extracellular matrix and interstitial fluid components have received little attention. Since the sinusoids connect the bone marrow interstitial fluid to the circulation, it is often considered to have the same composition as peripheral blood plasma. Stark differences in the cellular composition of the bone marrow and peripheral blood with different secretory capacities would however suggest profound differences. In this study we set out to better define if and how the bone marrow interstitial fluid (BMIF) compares to the peripheral blood plasma (PBP) and how both are remodeled during chemotherapy. We applied a multi-omic strategy to quantify the metabolite, lipid and protein components as well as the proteolytic modification of proteins to gain a comprehensive understanding of the two compartments. We found that the bone marrow interstitial fluid is clearly distinct from peripheral blood plasma, both during active pediatric acute lymphoblastic leukemia and following induction chemotherapy. Either compartment was shaped differently by active leukemia, with the bone marrow interstitial fluid being rich in extracellular vesicle components and showing protease dysregulation while the peripheral blood plasma showed elevation of immune regulatory proteins. Following chemotherapy, the BMIF showed signs of cellular remodeling and impaired innate immune activation while the peripheral blood plasma was characterized by restored lipid homeostasis.

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Section: Discussionsupporting

confidence: 65%

Multi-omic profiling of the leukemic microenvironment shows bone marrow interstitial fluid is distinct from peripheral blood plasma

Nierves

Guo

Chen

et al. 2022

Preprint

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“…Similarly, DS is associated with immunodeficiency and a high susceptibility to infections, both at baseline and during leukemia treatment 6,30 . Interestingly, survivors of childhood cancer have recently been noted to be at increased risk of infection‐related death well after the completion of cancer treatment 31 . For both pulmonary and infectious complications, it is possible that baseline DS‐associated risks of infectious and pulmonary events are further increased among DS survivors, resulting in increased late mortality compared to both non‐DS survivors and DS controls.…”

Section: Discussionmentioning

confidence: 99%

Risks of late mortality and morbidity among survivors of childhood acute leukemia with Down syndrome: A population‐based cohort study

Gupta

Sutradhar

Pequeno

et al. 2021

Cancer

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Background Children with leukemia and Down syndrome (DS) are at higher risk of acute treatment toxicities than those without DS. Whether late toxicity risks are also elevated is unknown. Methods The authors identified all patients diagnosed with leukemia before the age of 18 years in Ontario, Canada between 1987 and 2013 and who survived greater than 5 years since their last pediatric cancer event. Survivors were divided into those with and without DS, matched by birth year, sex, leukemia type, and receipt of radiation. DS survivors were matched to individuals with DS without childhood cancer (DS controls) in a 1:10 ratio. Outcomes were identified through linkage to population‐based health services databases. Results DS survivors (n = 79) experienced inferior overall survival compared to non‐DS survivors (n = 231) (20‐year overall survival, 81.7% ± 6.8% vs 98.3% ± 1.2%; hazard ratio [HR], 12.8; P < .0001) and to DS controls (n = 790; 96.3% ± 1.2%; HR, 5.4 P < .0001). Pulmonary and infectious deaths were noted among DS survivors. There was no difference in the incidence of congestive heart failure between DS survivors and either control cohort, nor of hearing loss or dementia between DS survivors and DS controls. Conclusions DS survivors were at substantially higher risk of late mortality than non‐DS survivors or DS controls. This excess risk was not attributable to cardiac‐ or subsequent malignant neoplasm‐related late effects, historically main causes of premature death among non‐DS survivors. Chronic morbidities associated with DS were not increased compared to DS controls. DS‐specific surveillance guidelines may be warranted.

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“…Furthermore, in these individuals, increased T-cell activation and chronic inflammation was observed, suggesting a correlation between dysregulated microbial taxa and immune dysregulation [ 41 ]. The increased infection risk in survivors [ 73 ], a high prevalence of chronic health conditions [ 74 , 75 ] and an elevated risk of mortality and morbidity have been investigated [ 76 ]. Thus, microbial dysregulation due to the influences of chemotherapy and antibiotics during ALL treatment may have long-term effects on the development of other diseases, such as obesity or diabetes, in adult survivors of pediatric ALL [ 41 , 42 ].…”

Section: Microbiome In Allmentioning

confidence: 99%

The Microbiome in Childhood Acute Lymphoblastic Leukemia

Oldenburg

Rüchel

Gössling

2021

Cancers

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For almost 30 years, the term “holobiont” has referred to an ecological unit where a host (e.g., human) and all species living in or around it are considered together. The concept highlights the complex interactions between the host and the other species, which, if disturbed may lead to disease and premature aging. Specifically, the impact of microbiome alterations on the etiology of acute lymphoblastic leukemia (ALL) in children is not fully understood, but has been the focus of much research in recent years. In ALL patients, significant reductions in microbiome diversity are already observable at disease onset. It remains unclear whether such alterations at diagnosis are etiologically linked with leukemogenesis or simply due to immunological alteration preceding ALL onset. Regardless, all chemotherapeutic treatment regimens severely affect the microbiome, accompanied by severe side effects, including mucositis, systemic inflammation, and infection. In particular, dominance of Enterococcaceae is predictive of infections during chemotherapy. Long-term dysbiosis, like depletion of Faecalibacterium, has been observed in ALL survivors. Modulation of the microbiome (e.g., by fecal microbiota transplant, probiotics, or prebiotics) is currently being researched for potential protective effects. Herein, we review the latest microbiome studies in pediatric ALL patients.

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Long-Term Risk of Infections After Treatment of Childhood Leukemia: A Population-Based Cohort Study Using Administrative Health Data

Cited by 14 publications

References 48 publications

Multi-omic profiling of the leukemic microenvironment shows bone marrow interstitial fluid is distinct from peripheral blood plasma

Multi-omic profiling of the leukemic microenvironment shows bone marrow interstitial fluid is distinct from peripheral blood plasma

Risks of late mortality and morbidity among survivors of childhood acute leukemia with Down syndrome: A population‐based cohort study

The Microbiome in Childhood Acute Lymphoblastic Leukemia

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