Hypothermia is not therapeutic in a neonatal piglet model of inflammation-sensitized hypoxia–ischemia

Martinello, Kathryn; Meehan, Christopher; Avdic-Belltheus, Adnan; Lingam, Ingran; Mutshiya, Tatenda; Yang, Qin; Akın, Mustafa Ali; Price, David L.; Sokolska, Magdalena; Bainbridge, Alan; Hristova, Mariya; Tachtsidis, Ilias; Tann, Cally J; Peebles, Donald; Hagberg, Henrik; Wolfs, Tim G. A. M.; Klein, Nigel; Kramer, Boris W.; Fleiss, Bobbi; Gressèns, Pierre; Golay, Xavier; Robertson, Nicola J.

doi:10.1038/s41390-021-01584-6

Cited by 14 publications

(41 citation statements)

References 83 publications

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“…Part of the lack of complete neuroprotection by TH may be due to heterogeneous etiologies of injury in the clinical setting, including HIE complicated by infection or chronic placental insufficiency [38,39]. In particular, TH has not been neuroprotective in preclinical models of HI sensitized with LPS [13,40,41]. The lack of significant neuroprotection conferred by TH in our ferret model is therefore not unexpected due to the use of LPS for inflammatory presensitization, though TH animals did demonstrate improved behavioral outcomes in some tests compared to other HIH-exposed animals.…”

Section: Discussionmentioning

confidence: 99%

“…Examining the mechanisms of Epo neuroprotection in this model are beyond the scope of this manuscript but will form the basis of future work. By comparison, although we have not studied response to these therapies without the presensitizing effect of LPS in the model, it is likely that the inclusion of LPS is the primary reason for a lack of neuroprotective effect of TH [13,40,41]. However, as more definitive evidence is accumulating regarding the lack of TH neuroprotection in lower income settings [5], perhaps due to more protracted or chronic perinatal insults, the model as used here may be particularly useful for examining therapies for use in scenarios where TH is not beneficial.…”

Section: Discussionmentioning

confidence: 99%

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Evaluating Neuroprotective Effects of Uridine, Erythropoietin, and Therapeutic Hypothermia in a Ferret Model of Inflammation-Sensitized Hypoxic-Ischemic Encephalopathy

Corry

White

Shearlock

et al. 2021

IJMS

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Perinatal hypoxic-ischemic (HI) brain injury, often in conjunction with an inflammatory insult, is the most common cause of death or disability in neonates. Therapeutic hypothermia (TH) is the standard of care for HI encephalopathy in term and near-term infants. However, TH may not always be available or efficacious, creating a need for novel or adjunctive neurotherapeutics. Using a near-term model of inflammation-sensitized HI brain injury in postnatal day (P) 17 ferrets, animals were randomized to either the control group (n = 43) or the HI-exposed groups: saline vehicle (Veh; n = 42), Ur (uridine monophosphate, n = 23), Epo (erythropoietin, n = 26), or TH (n = 24) to test their respective therapeutic effects. Motor development was assessed from P21 to P42 followed by analysis of cortical anatomy, ex vivo MRI, and neuropathology. HI animals took longer to complete the motor assessments compared to controls, which was exacerbated in the Ur group. Injury resulted in thinned white matter tracts and narrowed cortical sulci and gyri, which was mitigated in Epo-treated animals in addition to normalization of cortical neuropathology scores to control levels. TH and Epo treatment also resulted in region-specific improvements in diffusion parameters on ex vivo MRI; however, TH was not robustly neuroprotective in any behavioral or neuropathological outcome measures. Overall, Ur and TH did not provide meaningful neuroprotection after inflammation-sensitized HI brain injury in the ferret, and Ur appeared to worsen outcomes. By comparison, Epo appears to provide significant, though not complete, neuroprotection in this model.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Evaluating Neuroprotective Effects of Uridine, Erythropoietin, and Therapeutic Hypothermia in a Ferret Model of Inflammation-Sensitized Hypoxic-Ischemic Encephalopathy

Corry

White

Shearlock

et al. 2021

IJMS

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“…Meanwhile, some researchers proposed infection was the main cause of encephalopathy in African settings. More recent data from Africa [13,21] and South Asia suggest that the incidence of coexistent sepsis in Africa and South Asia is not higher than high-income countries [14] and coexistent sepsis cannot explain lack of hypothermic neuroprotection in LMIC.…”

Section: Ignoring Population Differences and Misleading Infection-ischemia Theorymentioning

confidence: 96%

Rise and Fall of Therapeutic Hypothermia in Low-Resource Settings: Lessons from the HELIX Trial

et al. 2021

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In the past decade, therapeutic hypothermia using a variety of low-cost devices has been widely implemented in India and other low-and middle-income countries (LMIC) without adequate evidence of either safety or efficacy. The recently reported data from the world’s largest cooling trial (HELIX - hypothermia for encephalopathy in low- and middle-income countries) in LMIC provides definitive evidence of harm of cooling therapy with increase in mortality (number to harm 9) and lack of neuroprotection. Although the HELIX participating centers were highly selected tertiary neonatal intensive care units in South Asia with facilities for invasive ventilation, cardiovascular support, and 3 Tesla magnetic resonance imaging (MRI), and the trial used state-of-the-art automated servo-controlled cooling devices, a therapy that is harmful under such optimal conditions cannot be safe in low-resource settings that cannot even afford servo-controlled cooling devices.The HELIX trial has set a new benchmark for conducting high quality randomized controlled trials in terms of research governance, consent, ethics, follow-up rates, and involvement of parents. The standard care for neonatal encephalopathy in LMIC should remain normothermia, with close attention to prevention of hyperthermia. There is no role for therapeutic hypothermia in LMIC as the efficacy of hypothermia is dependent on the population, and not merely on the level of neonatal intensive care facilities. Future research should explore timings and origins of brain injury and prevention of brain injury in LMIC, with a strong emphasis on academic research capacity building and patient and public engagement.

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“…Several animal studies have found that endotoxin-induced inflammation prior to hypoxia-ischemia severely exacerbates brain injury in newborns ( 24 – 31 ). In addition to the possible aggravation of brain damage, both animal ( 32 – 37 ) and clinical studies ( 38 – 41 ) have suggested that infections may affect both the efficacy and safety of therapeutic hypothermia.…”

Section: Introductionmentioning

confidence: 99%

Neurological Outcome Following Newborn Encephalopathy With and Without Perinatal Infection: A Systematic Review

et al. 2021

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Background: Studies have suggested that neurological outcome may differ in newborns with encephalopathy with and without perinatal infection. We aimed to systematically review this association.Methods: We conducted this systematic review according to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA). Studies were obtained from four databases including Pubmed, Embase, Web of Science, and The Cochrane Database. Newborns with encephalopathy with and without markers of perinatal infection were compared with regard to neurodevelopmental assessments, neurological disorders, and early biomarkers of brain damage. Risk of bias and quality of evidence were assessed by the Newcastle-Ottawa scale and Grading of Recommendations Assessment, Development and Evaluation (GRADE).Results: We screened 4,284 studies of which eight cohort studies and one case-control study met inclusion criteria. A narrative synthesis was composed due to heterogeneity between studies. Six studies were classified as having low risk of bias, while three studies were classified as having high risk of bias. Across all outcomes, the quality of evidence was very low. The neurological outcome was similar in newborns with encephalopathy with and without markers of perinatal infection.Conclusions: Further studies of higher quality are needed to clarify whether perinatal infection may affect neurological outcome following newborn encephalopathy.Systematic Review Registration:https://www.crd.york.ac.uk/prospero/, identifier CRD42020185717.

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Hypothermia is not therapeutic in a neonatal piglet model of inflammation-sensitized hypoxia–ischemia

Cited by 14 publications

References 83 publications

Evaluating Neuroprotective Effects of Uridine, Erythropoietin, and Therapeutic Hypothermia in a Ferret Model of Inflammation-Sensitized Hypoxic-Ischemic Encephalopathy

Evaluating Neuroprotective Effects of Uridine, Erythropoietin, and Therapeutic Hypothermia in a Ferret Model of Inflammation-Sensitized Hypoxic-Ischemic Encephalopathy

Rise and Fall of Therapeutic Hypothermia in Low-Resource Settings: Lessons from the HELIX Trial

Neurological Outcome Following Newborn Encephalopathy With and Without Perinatal Infection: A Systematic Review

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