Sepsis Clinical Trial
— SAUNAOfficial title:
Selective Antibiotics When Symptoms Develop Versus Universal Antibiotics for Preterm Neonates At-risk of Early-onset Bacterial Sepsis: a Multicentric, Randomized, Controlled, Non-inferiority Trial (the SAUNA Trial)
Preterm infants are born at less than 37 weeks of pregnancy. Sometimes a break or tear in the fluid filled bag that surrounds and protects the infant during pregnancy leads to an untimely birth. This state puts the infant at risk of serious condition called sepsis. Sepsis is a condition in which body responds inappropriately to an infection. Sepsis may progress to septic shock which can result in the loss of life. Doctors give antibiotics to treat sepsis. The goal of this research study is to find out: 1. Among neonates at risk of early-onset neonatal sepsis, whether a policy of administering antibiotics selectively to a subset of at-risk infants who later develop signs of sepsis is not inferior to administering antibiotics to all at-risk infants in the 1st week of life. 2. To find out if infants receiving selective antibiotics (as above) compared to those receiving antibiotics from birth (as above) require fewer antibiotic courses of 48 hours duration or more in the 1st week of life. 3. To find out whether infants receiving selective antibiotics (as above) compared to those receiving antibiotics from birth (as above) are significantly different with respect to a wide range of secondary outcomes (listed under "Outcomes").
| Status | Not yet recruiting |
| Enrollment | 1500 |
| Est. completion date | April 14, 2028 |
| Est. primary completion date | April 15, 2027 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 0 Hours to 4 Hours |
| Eligibility | Inclusion criteria: - Gestational age of 26 to 34 weeks - Chronological age 4 hours - Have any one or both of the following risk factors of EONS: - Prolonged rupture of membranes >18 hours - Pre-labour rupture of membranes [as all subjects will be preterm, this is effectively pPROM] - Are either asymptomatic or have no signs attributable to sepsis at 4 hours. This will be defined as absence of the following clinical signs or need for interventions mentioned below: 1. Apnea (Standard definition) requiring intervention at any time until enrolment. 2. Need for a fluid bolus or inotropic support at any time until enrolment. 3. Seizures or seizure-like activity at any time until enrolment. 4. Upper GI bleed in the absence of a history of ante-partum hemorrhage at any time until enrolment. 5. Pus from any site at any time until enrolment. 6. Need for CPAP >6 cms of water with FiO2 >35% at 6-8 hours OR need for CPAP £6 cms and FiO2 £35% but with increasing requirement of support** 7. Chest Xray (if performed) with radiological features of pneumonia. 8. Need for intubation and mechanical ventilation. 9. Temperature >37.5°C or <36°C, unexplained by environmental causes 10. Feed intolerance [bilious or bloodstained vomiting (or gastric residuals) or visibly distended abdomen or >50% of the previous feed volume as gastric residuals] 11. Lethargy or unarousability 12. Sclerema Exclusion Criteria: Subjects will be excluded if they have any 1 of the following: 1. Life-threatening congenital malformation 2. Severe perinatal asphyxia (Apgar score <5 at 10 minutes or cord pH <7.0) 3. Clinical chorioamnionitis# [see definition below] 4. Foul-smelling liquor 5. Multiple gestation 6. Received a dose of antibiotics 7. Positive amniotic fluid culture (if performed and available prior to randomization) 8. Treating neonatologist unwilling to enroll the patient in the trial on the grounds that the patient needs antibiotics. - |
| Country | Name | City | State |
|---|---|---|---|
| India | Post Graduate Institute of Medical Education and Research (PGIMER) | Chandigarh |
| Lead Sponsor | Collaborator |
|---|---|
| Indian Council of Medical Research | Government Medical College, Aurangabad, Government Medical College, Chandigarh, Indira Gandhi Institute of Child Health, Institute of Obstetrics and Gynecology, King Edward Memorial Hospital, Mumbai, King George's Medical University, Lady Hardinge Medical College, Pandit Bhagwat Dayal Sharma, PGIMS, Rohtak |
India,
Berardi A, Buffagni AM, Rossi C, Vaccina E, Cattelani C, Gambini L, Baccilieri F, Varioli F, Ferrari F. Serial physical examinations, a simple and reliable tool for managing neonates at risk for early-onset sepsis. World J Clin Pediatr. 2016 Nov 8;5(4):35 — View Citation
Berardi A, Fornaciari S, Rossi C, Patianna V, Bacchi Reggiani ML, Ferrari F, Neri I, Ferrari F. Safety of physical examination alone for managing well-appearing neonates >/= 35 weeks' gestation at risk for early-onset sepsis. J Matern Fetal Neonatal Med. — View Citation
Berardi A, Spada C, Reggiani MLB, Creti R, Baroni L, Capretti MG, Ciccia M, Fiorini V, Gambini L, Gargano G, Papa I, Piccinini G, Rizzo V, Sandri F, Lucaccioni L; GBS Prevention Working Group of Emilia-Romagna. Group B Streptococcus early-onset disease an — View Citation
Cantoni L, Ronfani L, Da Riol R, Demarini S; Perinatal Study Group of the Region Friuli-Venezia Giulia. Physical examination instead of laboratory tests for most infants born to mothers colonized with group B Streptococcus: support for the Centers for Dis — View Citation
Chan GJ, Lee AC, Baqui AH, Tan J, Black RE. Risk of early-onset neonatal infection with maternal infection or colonization: a global systematic review and meta-analysis. PLoS Med. 2013 Aug;10(8):e1001502. doi: 10.1371/journal.pmed.1001502. Epub 2013 Aug 2 — View Citation
Chaurasia S, Sivanandan S, Agarwal R, Ellis S, Sharland M, Sankar MJ. Neonatal sepsis in South Asia: huge burden and spiralling antimicrobial resistance. BMJ. 2019 Jan 22;364:k5314. doi: 10.1136/bmj.k5314. — View Citation
Chiruvolu A, Petrey B, Stanzo KC, Daoud Y. An Institutional Approach to the Management of Asymptomatic Chorioamnionitis-Exposed Infants Born >/=35 Weeks Gestation. Pediatr Qual Saf. 2019 Dec 5;4(6):e238. doi: 10.1097/pq9.0000000000000238. eCollection 2019 — View Citation
Investigators of the Delhi Neonatal Infection Study (DeNIS) collaboration. Characterisation and antimicrobial resistance of sepsis pathogens in neonates born in tertiary care centres in Delhi, India: a cohort study. Lancet Glob Health. 2016 Oct;4(10):e752 — View Citation
Joshi NS, Gupta A, Allan JM, Cohen RS, Aby JL, Weldon B, Kim JL, Benitz WE, Frymoyer A. Clinical Monitoring of Well-Appearing Infants Born to Mothers With Chorioamnionitis. Pediatrics. 2018 Apr;141(4):e20172056. doi: 10.1542/peds.2017-2056. — View Citation
Lawn JE, Blencowe H, Oza S, You D, Lee AC, Waiswa P, Lalli M, Bhutta Z, Barros AJ, Christian P, Mathers C, Cousens SN; Lancet Every Newborn Study Group. Every Newborn: progress, priorities, and potential beyond survival. Lancet. 2014 Jul 12;384(9938):189- — View Citation
Puopolo KM, Benitz WE, Zaoutis TE; COMMITTEE ON FETUS AND NEWBORN; COMMITTEE ON INFECTIOUS DISEASES. Management of Neonates Born at >/=35 0/7 Weeks' Gestation With Suspected or Proven Early-Onset Bacterial Sepsis. Pediatrics. 2018 Dec;142(6):e20182894. do — View Citation
Sankar MJ, Neogi SB, Sharma J, Chauhan M, Srivastava R, Prabhakar PK, Khera A, Kumar R, Zodpey S, Paul VK. State of newborn health in India. J Perinatol. 2016 Dec;36(s3):S3-S8. doi: 10.1038/jp.2016.183. — View Citation
Wolf RL, Olinsky A. Prolonged rupture of fetal membranes and neonatal infections. S Afr Med J. 1976 Apr 3;50(15):574-6. — View Citation
* Note: There are 13 references in all — Click here to view all references
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Composite of all-cause mortality and/or any episode of culture-positive sepsis and/or severe sepsis* within the 1st 7 days after randomization | Either mortality due to any cause and/or an episode of culture-positive sepsis and/or severe sepsis. These outcomes will be measured within the "1st 7 days after randomization", which for all practical purposes, is equivalent to the "1st 7 days of life" since participants will be randomized at about 4 hours of life. Hence, the duration expressed after randomization and of life will be used interchangeably for this outcome and other outcomes. | Within 1st 7 days after randomization | |
| Primary | Need for intravenous antibiotics for = 48 hours within the 1st 7 days after randomization | Requirement for intravenous antibiotic courses whose duration is = 48 hours with the onset of the course within the first 7 days after randomization. For all practical purposes, this would be equivalent to the 1st 7 days of life since participants will be randomized at about 4 hours of life. | Within 1st 7 days after randomization | |
| Secondary | All-cause Mortality within 1st 7 days after randomization | Mortality due to any cause | During 1st 7 days after randomization | |
| Secondary | Blood culture-positive sepsis of any severity within 1st 7 days after randomization | Blood culture proven septicemia | Within 1st 7 days after randomization | |
| Secondary | Episode of severe sepsis within 1st 7 days after randomization | Any episode of severe sepsis during 1st 7 days after randomization. Severe sepsis be defined as clinical signs of sepsis AND either a positive blood culture or laboratory evidence of sepsis (either CRP OR Procalcitonin above the age-appropriate cut-off value OR any two of the CBC parameters outside the age-appropriate ranges OR chest x-ray suggestive of pneumonia) AND one or more of the following indices of severity [Need for intubation and mechanical ventilation, Need for inotropes >10 mic/kg/min dopamine or >10 mic/kg/min dobutamine or adrenaline > 0.05 mic/kg/min, Need for exchange transfusion, Need for platelet concentrates or FFP, Meningitis (defined as either CSF culture positive or Gram stain positive or Cell count >25/microlitre or glucose <25 mg/dl or protein >180 mg/dl)] | Within 1st 7 days after randomization | |
| Secondary | Composite of mortality/blood culture positive sepsis/severe sepsis within 1st 72 hours after randomization | Either mortality and/or blood culture-positive sepsis and/or severe sepsis | Within first 72 hour after randomization | |
| Secondary | Individual components of composite outcome within 1st 72 hours after randomization | Separately mortality, blood culture-positive sepsis or severe sepsis | Within 1st 72 hours after randomization | |
| Secondary | Composite of mortality/blood culture positive sepsis/severe sepsis during hospital stay | Either mortality due to any cause and/or blood culture-positive sepsis and/or severe sepsis during hospital stay, with maximum duration of observation during hospital stay being capped at 100 days | During hospital stay upto 100 days after randomization | |
| Secondary | Individual components of composite outcome during hospital stay | Separately mortality, blood culture-positive sepsis or severe sepsis during hospital stay, with maximum duration of observation during hospital stay being capped at 100 days | During hospital stay upto 100 days after randomization | |
| Secondary | Necrotizing enterocolitis, stage II-III by modified Bell's staging criteria during hospital stay | Necrotizing enterocolitis stage II-III by modified Bell's staging criteria during hospital stay, with maximum duration of observation during hospital stay being capped at 100 days after randomization | During hospital stay upto 100 days after randomization | |
| Secondary | Composite of mortality/blood culture positive sepsis/severe sepsis during 1st 30 days after randomization | Either all-cause mortality and/or blood culture-positive sepsis and/or severe sepsis during the 1st 30 days after randomization | During 1st 30 days after randomization | |
| Secondary | Individual components of composite outcome during 1st 30 days | Separately, all-cause mortality, blood culture-positive sepsis or severe sepsis during the 1st 30 days after randomization | During 1st 30 days after randomization | |
| Secondary | Necrotizing enterocolitis, stage II-III by modified Bell's staging criteria | Necrotizing enterocolitis, stage II-III by modified Bell's staging criteria during the 1st 30 days after randomization | During 1st 30 days after randomization | |
| Secondary | Sepsis-related mortality within 1st 72 hours after randomization | Mortality due to sepsis within 1st 72 hours. The decision of the treating team will be recorded for attributing mortality to sepsis. | Within 1st 72 hours after randomization | |
| Secondary | Sepsis-related mortality within 7 day after randomization | Mortality due to sepsis within 7 days after randomization. The decision of the treating team will be recorded for attributing mortality to sepsis. | Within 7 days after randomization | |
| Secondary | Sepsis-related mortality during hospital stay after randomization | Mortality due to sepsis during hospital stay. The decision of the treating team will be recorded for attributing mortality to sepsis. | During hospital stay upto 100 days after randomization | |
| Secondary | Sepsis-related mortality during 1st 30 days after randomization | Mortality due to sepsis during 1st 30 days after randomization | During 1st 30 days after randomization | |
| Secondary | Clinical sepsis within 1st 72 hours after randomization | Episodes of clinical EONS (as per definition from a repertoire of clinical signs with normal lab parameters) within 1st 72 hours | Within 1st 72 hours after randomization | |
| Secondary | Clinical sepsis within 7 days after randomization | Episodes of clinical EONS (as per definition from a repertoire of clinical signs with normal lab parameters) within 7 days | Within 7 days after randomization | |
| Secondary | Clinical sepsis during hospital stay | Episodes of clinical EONS (as per definition from a repertoire of clinical signs with normal lab parameters) during hospital stay, with maximum duration of observation during hospital stay being capped at 100 days after randomization | During hospital stay upto 100 days | |
| Secondary | Clinical sepsis within 1st 30 days after randomization | Episodes of clinical EONS (as per definition from a repertoire of clinical signs with normal lab parameters) within 1st 30 days of life | During 1st 30 days after randomization | |
| Secondary | Episode of Probable EONS within 72 hours after randomization | Episode of Probable EONS [as per definition from a repertoire of clinical signs, AND with abnormal age-appropriate values of one or more of TLC, ANC, CRP, PCT, chest x-ray suggestive of pneumonia AND with sterile blood culture] | Within 72 hours after randomization | |
| Secondary | Episode of Probable EONS within 7 days after randomization | Episode of Probable EONS [as per definition from a repertoire of clinical signs, AND with abnormal age-appropriate values of one or more of TLC, ANC, CRP, PCT, chest x-ray suggestive of pneumonia AND with sterile blood culture] | Within 7 days after randomization | |
| Secondary | Episode of asymptomatic proven EONS within 72 hours after randomization | Episode of asymptomatic proven EONS [asymptomatic but baseline blood culture positive with non-contaminant organism] | Within 72 hours after randomization | |
| Secondary | Need for sepsis workup during 1st 72 hours after randomization | ["Sepsis workup" defined as one or more of CBC, CRP, Procalcitonin, blood culture] during 1st 72 hours of life | During 1st 72 hours after randomization | |
| Secondary | Need for sepsis workup during 1st 7 days after randomization | "Sepsis workup" defined as one or more of CBC, CRP, Procalcitonin, blood culture during 1st 7 days of life | During 1st 7 days after randomization | |
| Secondary | Need for sepsis workup during 1st 30 days after randomization | "Sepsis workup" defined as one or more of CBC, CRP, Procalcitonin, blood culture during 1st 30 days of life | During 1st 30 days after randomization | |
| Secondary | Need for sepsis workup during hospital stay | "Sepsis workup" defined as one or more of CBC, CRP, Procalcitonin, blood culture during hospital stay, with the period of observation during hospital stay being capped at 100 days | During hospital stay upto 100 days | |
| Secondary | Cumulative duration of antibiotic therapy during 1st 7 days after randomization | Cumulative duration of antibiotic therapy during the 1st 7 days, which may include the sum of the durations of multiple courses of antibiotics, either in continuation or discontinuous. If any course of antibiotics continues beyond the 1st 7 days after randomization, only that portion of the antibiotic course would be included until the 1st 7 days after randomization. | During 1st 7 days after randomization | |
| Secondary | Cumulative duration of antibiotic therapy during 1st 72 hrs after randomization | Cumulative measure of antibiotics therapy during the 1st 72 hours | During 1st 72 hours after randomization | |
| Secondary | Cumulative duration of antibiotic therapy during hospital stay | Cumulative measure of antibiotics therapy during hospital stay, with the period of observation during hospital stay capped at 100 days | During hospital stay upto 100 days after randomization | |
| Secondary | Duration of hospitalization | Full length of hospital stay, with the period capped at 100 days | Upto 100 days | |
| Secondary | Episodes of healthcare associated infection during hospital stay. | Defined as any episode of culture positive sepsis with onset after 72 hours of life or any episode of culture-positive sepsis if baseline blood culture was sterile, with the period of observation during hospital stay capped at 100 days | From after 72 hours until 100 days during hospital stay | |
| Secondary | Adverse effects until day 30 after randomization | Adverse effects will be recorded as per the Common Terminology Criteria for Adverse Events (CTCAE) version 5. | During 30 days after randomization | |
| Secondary | Serious adverse effects until day 30 after randomization | Serious adverse effects will be recorded as per the Common Terminology Criteria for Adverse Events (CTCAE) version 5. | During 30 days after randomization |
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