Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants

Dale L. Phelps; Robert M. Ward; Rick L. Williams; Tracy L. Nolen; Kristi L. Watterberg; William Oh; Michael Goedecke; Richard A. Ehrenkranz; Timothy Fennell; Brenda B. Poindexter; C. Michael Cotten; Mikko Hallman; Ivan D. Frantz; Roger G. Faix; Kristin M. Zaterka-Baxter; Abhik Das; M. Bethany Ball; Conra Backstrom Lacy; Michele C. Walsh; Waldemar A. Carlo; Pablo J. Sánchez; Edward F. Bell; Seetha Shankaran; David P. Carlton; Patricia R. Chess; Rosemary D. Higgins

doi:10.1038/pr.2016.97

Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants

Dale L. Phelps, Robert M. Ward, Rick L. Williams, Tracy L. Nolen, Kristi L. Watterberg, William Oh, Michael Goedecke, Richard A. Ehrenkranz, Timothy Fennell, Brenda B. Poindexter, C. Michael Cotten, Mikko Hallman, Ivan D. Frantz, Roger G. Faix, Kristin M. Zaterka-Baxter, Abhik Das, M. Bethany Ball, Conra Backstrom Lacy, Michele C. Walsh, Waldemar A. CarloPablo J. Sánchez, Edward F. Bell, Seetha Shankaran, David P. Carlton, Patricia R. Chess, Rosemary D. Higgins

Pediatrics

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Background: Preterm infants with respiratory distress syndrome (RDS) given inositol had reduced bronchopulmonary dysplasia (BPD), death and severe retinopathy of prematurity (ROP). We assessed the safety and pharmacokinetics of daily inositol to select a dose providing serum levels previously associated with benefit, and to learn if accumulation occurred when administered throughout the normal period of retinal vascularization. Methods: Infants ≤ 29 wk GA (n = 122, 14 centers) were randomized and treated with placebo or inositol at 10, 40, or 80 mg/kg/d. Intravenous administration converted to enteral when feedings were established, and continued to the first of 10 wk, 34 wk postmenstrual age (PMA) or discharge. Serum collection employed a sparse sampling population pharmacokinetics design. Inositol urine losses and feeding intakes were measured. Safety was prospectively monitored. Results: At 80 mg/kg/d mean serum levels reached 140 mg/l, similar to Hallman's findings. Levels declined after 2 wk, converging in all groups by 6 wk. Analyses showed a mean volume of distribution 0.657 l/kg, clearance 0.058 l/kg/h, and half-life 7.90 h. Adverse events and comorbidities were fewer in the inositol groups, but not significantly so. Conclusion: Multiple dose inositol at 80 mg/kg/d was not associated with increased adverse events, achieves previously effective serum levels, and is appropriate for investigation in a phase III trial.

Original language	English (US)
Pages (from-to)	209-217
Number of pages	9
Journal	Pediatric Research
Volume	80
Issue number	2
DOIs	https://doi.org/10.1038/pr.2016.97
State	Published - Aug 1 2016

ASJC Scopus subject areas

Pediatrics, Perinatology, and Child Health

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10.1038/pr.2016.97

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Phelps, D. L., Ward, R. M., Williams, R. L., Nolen, T. L., Watterberg, K. L., Oh, W., Goedecke, M., Ehrenkranz, R. A., Fennell, T., Poindexter, B. B., Cotten, C. M., Hallman, M., Frantz, I. D., Faix, R. G., Zaterka-Baxter, K. M., Das, A., Ball, M. B., Lacy, C. B., Walsh, M. C., ... Higgins, R. D. (2016). Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants. Pediatric Research, 80(2), 209-217. https://doi.org/10.1038/pr.2016.97

Phelps, DL, Ward, RM, Williams, RL, Nolen, TL, Watterberg, KL, Oh, W, Goedecke, M, Ehrenkranz, RA, Fennell, T, Poindexter, BB, Cotten, CM, Hallman, M, Frantz, ID, Faix, RG, Zaterka-Baxter, KM, Das, A, Ball, MB, Lacy, CB, Walsh, MC, Carlo, WA, Sánchez, PJ, Bell, EF, Shankaran, S, Carlton, DP, Chess, PR & Higgins, RD 2016, 'Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants', Pediatric Research, vol. 80, no. 2, pp. 209-217. https://doi.org/10.1038/pr.2016.97

@article{e37c59521a624c9d81459b2bac51f47c,

title = "Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants",

abstract = "Background: Preterm infants with respiratory distress syndrome (RDS) given inositol had reduced bronchopulmonary dysplasia (BPD), death and severe retinopathy of prematurity (ROP). We assessed the safety and pharmacokinetics of daily inositol to select a dose providing serum levels previously associated with benefit, and to learn if accumulation occurred when administered throughout the normal period of retinal vascularization. Methods: Infants ≤ 29 wk GA (n = 122, 14 centers) were randomized and treated with placebo or inositol at 10, 40, or 80 mg/kg/d. Intravenous administration converted to enteral when feedings were established, and continued to the first of 10 wk, 34 wk postmenstrual age (PMA) or discharge. Serum collection employed a sparse sampling population pharmacokinetics design. Inositol urine losses and feeding intakes were measured. Safety was prospectively monitored. Results: At 80 mg/kg/d mean serum levels reached 140 mg/l, similar to Hallman's findings. Levels declined after 2 wk, converging in all groups by 6 wk. Analyses showed a mean volume of distribution 0.657 l/kg, clearance 0.058 l/kg/h, and half-life 7.90 h. Adverse events and comorbidities were fewer in the inositol groups, but not significantly so. Conclusion: Multiple dose inositol at 80 mg/kg/d was not associated with increased adverse events, achieves previously effective serum levels, and is appropriate for investigation in a phase III trial.",

author = "Phelps, {Dale L.} and Ward, {Robert M.} and Williams, {Rick L.} and Nolen, {Tracy L.} and Watterberg, {Kristi L.} and William Oh and Michael Goedecke and Ehrenkranz, {Richard A.} and Timothy Fennell and Poindexter, {Brenda B.} and Cotten, {C. Michael} and Mikko Hallman and Frantz, {Ivan D.} and Faix, {Roger G.} and Zaterka-Baxter, {Kristin M.} and Abhik Das and Ball, {M. Bethany} and Lacy, {Conra Backstrom} and Walsh, {Michele C.} and Carlo, {Waldemar A.} and S{\'a}nchez, {Pablo J.} and Bell, {Edward F.} and Seetha Shankaran and Carlton, {David P.} and Chess, {Patricia R.} and Higgins, {Rosemary D.}",

note = "Funding Information: The National Institutes of Health and the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) Neonatal Research Network and the Pediatric Pharmacology Research Units Network, with cofunding from the National Eye Institute provided grant support for this trial, with additional support from the National Center for Research Resources, and the National Center for Advancing Translational Sciences, Bethesda, MD, USA. The following NRNetwork Centers and Institutions (with grant numbers) participated in the Inositol Multidose Study: Alpert Medical School of Brown University and Women & Infants Hospital of Rhode Island (U10 HD27904); Case Western Reserve University, Rainbow Babies & Children's Hospital (U10 HD21364, M01 RR80); Duke University School of Medicine, University Hospital, and Durham Regional Hospital (U10 HD40492, M01 RR30); Emory University, Children's Healthcare of Atlanta, Grady Memorial Hospital, and Emory University Hospital Midtown (U10 HD27851, M01 RR39, and UL1 TR454); Indiana University, University Hospital, Methodist Hospital, Riley Hospital for Children at Indiana University Health, and Wishard Health Services (U10 HD27856, M01 RR750); Stanford University (U10 HD27880); Tufts Medical Center, Floating Hospital for Children (U10 HD53119, M01 RR54); University of Alabama at Birmingham Health System and Children's Hospital of Alabama (U10 HD34216, M01 RR32); University of Iowa (U10 HD53109, M01 RR59, UL1 TR442); University of New Mexico Health Sciences Center (U10 HD53089, M01 RR997); University of Rochester Medical Center, Golisano Children's Hospital (U10 HD40521, M01 RR44); University of Texas Southwestern Medical Center, Parkland Health & Hospital System, and Children's Medical Center Dallas (U10 HD40689, M01 RR633); University of Utah Medical Center, Intermountain Medical Center, LDS Hospital, and Primary Children's Medical Center (U10 HD53124, U10 HD45986, and M01 RR64); Wayne State University, Hutzel Women's Hospital and Children's Hospital of Michigan (U10 HD21385, U10 HD37261); Yale University, Yale-New Haven Children's Hospital (U10 HD27871, UL1 RR24139, M01 RR125). Publisher Copyright: {\textcopyright} 2016 International Pediatric Research Foundation, Inc.",

year = "2016",

month = aug,

day = "1",

doi = "10.1038/pr.2016.97",

language = "English (US)",

volume = "80",

pages = "209--217",

journal = "Pediatric Research",

issn = "0031-3998",

publisher = "Lippincott Williams and Wilkins",

number = "2",

}

TY - JOUR

T1 - Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants

AU - Phelps, Dale L.

AU - Ward, Robert M.

AU - Williams, Rick L.

AU - Nolen, Tracy L.

AU - Watterberg, Kristi L.

AU - Oh, William

AU - Goedecke, Michael

AU - Ehrenkranz, Richard A.

AU - Fennell, Timothy

AU - Poindexter, Brenda B.

AU - Cotten, C. Michael

AU - Hallman, Mikko

AU - Frantz, Ivan D.

AU - Faix, Roger G.

AU - Zaterka-Baxter, Kristin M.

AU - Das, Abhik

AU - Ball, M. Bethany

AU - Lacy, Conra Backstrom

AU - Walsh, Michele C.

AU - Carlo, Waldemar A.

AU - Sánchez, Pablo J.

AU - Bell, Edward F.

AU - Shankaran, Seetha

AU - Carlton, David P.

AU - Chess, Patricia R.

AU - Higgins, Rosemary D.

N1 - Funding Information: The National Institutes of Health and the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) Neonatal Research Network and the Pediatric Pharmacology Research Units Network, with cofunding from the National Eye Institute provided grant support for this trial, with additional support from the National Center for Research Resources, and the National Center for Advancing Translational Sciences, Bethesda, MD, USA. The following NRNetwork Centers and Institutions (with grant numbers) participated in the Inositol Multidose Study: Alpert Medical School of Brown University and Women & Infants Hospital of Rhode Island (U10 HD27904); Case Western Reserve University, Rainbow Babies & Children's Hospital (U10 HD21364, M01 RR80); Duke University School of Medicine, University Hospital, and Durham Regional Hospital (U10 HD40492, M01 RR30); Emory University, Children's Healthcare of Atlanta, Grady Memorial Hospital, and Emory University Hospital Midtown (U10 HD27851, M01 RR39, and UL1 TR454); Indiana University, University Hospital, Methodist Hospital, Riley Hospital for Children at Indiana University Health, and Wishard Health Services (U10 HD27856, M01 RR750); Stanford University (U10 HD27880); Tufts Medical Center, Floating Hospital for Children (U10 HD53119, M01 RR54); University of Alabama at Birmingham Health System and Children's Hospital of Alabama (U10 HD34216, M01 RR32); University of Iowa (U10 HD53109, M01 RR59, UL1 TR442); University of New Mexico Health Sciences Center (U10 HD53089, M01 RR997); University of Rochester Medical Center, Golisano Children's Hospital (U10 HD40521, M01 RR44); University of Texas Southwestern Medical Center, Parkland Health & Hospital System, and Children's Medical Center Dallas (U10 HD40689, M01 RR633); University of Utah Medical Center, Intermountain Medical Center, LDS Hospital, and Primary Children's Medical Center (U10 HD53124, U10 HD45986, and M01 RR64); Wayne State University, Hutzel Women's Hospital and Children's Hospital of Michigan (U10 HD21385, U10 HD37261); Yale University, Yale-New Haven Children's Hospital (U10 HD27871, UL1 RR24139, M01 RR125). Publisher Copyright: © 2016 International Pediatric Research Foundation, Inc.

PY - 2016/8/1

Y1 - 2016/8/1

N2 - Background: Preterm infants with respiratory distress syndrome (RDS) given inositol had reduced bronchopulmonary dysplasia (BPD), death and severe retinopathy of prematurity (ROP). We assessed the safety and pharmacokinetics of daily inositol to select a dose providing serum levels previously associated with benefit, and to learn if accumulation occurred when administered throughout the normal period of retinal vascularization. Methods: Infants ≤ 29 wk GA (n = 122, 14 centers) were randomized and treated with placebo or inositol at 10, 40, or 80 mg/kg/d. Intravenous administration converted to enteral when feedings were established, and continued to the first of 10 wk, 34 wk postmenstrual age (PMA) or discharge. Serum collection employed a sparse sampling population pharmacokinetics design. Inositol urine losses and feeding intakes were measured. Safety was prospectively monitored. Results: At 80 mg/kg/d mean serum levels reached 140 mg/l, similar to Hallman's findings. Levels declined after 2 wk, converging in all groups by 6 wk. Analyses showed a mean volume of distribution 0.657 l/kg, clearance 0.058 l/kg/h, and half-life 7.90 h. Adverse events and comorbidities were fewer in the inositol groups, but not significantly so. Conclusion: Multiple dose inositol at 80 mg/kg/d was not associated with increased adverse events, achieves previously effective serum levels, and is appropriate for investigation in a phase III trial.

AB - Background: Preterm infants with respiratory distress syndrome (RDS) given inositol had reduced bronchopulmonary dysplasia (BPD), death and severe retinopathy of prematurity (ROP). We assessed the safety and pharmacokinetics of daily inositol to select a dose providing serum levels previously associated with benefit, and to learn if accumulation occurred when administered throughout the normal period of retinal vascularization. Methods: Infants ≤ 29 wk GA (n = 122, 14 centers) were randomized and treated with placebo or inositol at 10, 40, or 80 mg/kg/d. Intravenous administration converted to enteral when feedings were established, and continued to the first of 10 wk, 34 wk postmenstrual age (PMA) or discharge. Serum collection employed a sparse sampling population pharmacokinetics design. Inositol urine losses and feeding intakes were measured. Safety was prospectively monitored. Results: At 80 mg/kg/d mean serum levels reached 140 mg/l, similar to Hallman's findings. Levels declined after 2 wk, converging in all groups by 6 wk. Analyses showed a mean volume of distribution 0.657 l/kg, clearance 0.058 l/kg/h, and half-life 7.90 h. Adverse events and comorbidities were fewer in the inositol groups, but not significantly so. Conclusion: Multiple dose inositol at 80 mg/kg/d was not associated with increased adverse events, achieves previously effective serum levels, and is appropriate for investigation in a phase III trial.

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Safety and pharmacokinetics of multiple dose myo-inositol in preterm infants

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