Membrane Stabilization by Modified Steroid Offers a Potential Therapy for Muscular Dystrophy Due to Dysferlin Deficit

Sen Chandra Sreetama; Goutam Chandra; Jack H. Van der Meulen; Mohammad Mahad Ahmad; Peter Suzuki; Shivaprasad Bhuvanendran; Kanneboyina Nagaraju; Eric P. Hoffman; Jyoti K. Jaiswal

doi:10.1016/j.ymthe.2018.07.021

Membrane Stabilization by Modified Steroid Offers a Potential Therapy for Muscular Dystrophy Due to Dysferlin Deficit

Sen Chandra Sreetama
, Goutam Chandra
, Jack H. Van der Meulen
, Mohammad Mahad Ahmad
, Peter Suzuki
, Shivaprasad Bhuvanendran
, Kanneboyina Nagaraju
, Eric P. Hoffman
, Jyoti K. Jaiswal

Binghamton University

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

52 Scopus citations

Abstract

Mutations of the DYSF gene leading to reduced dysferlin protein level causes limb girdle muscular dystrophy type 2B (LGMD2B). Dysferlin facilitates sarcolemmal membrane repair in healthy myofibers, thus its deficit compromises myofiber repair and leads to chronic muscle inflammation. An experimental therapeutic approach for LGMD2B is to protect damage or improve repair of myofiber sarcolemma. Here, we compared the effects of prednisolone and vamorolone (a dissociative steroid; VBP15) on dysferlin-deficient myofiber repair. Vamorolone, but not prednisolone, stabilized dysferlin-deficient muscle cell membrane and improved repair of dysferlin-deficient mouse (B6A/J) myofibers injured by focal sarcolemmal damage, eccentric contraction-induced injury or injury due to spontaneous in vivo activity. Vamorolone decreased sarcolemmal lipid mobility, increased muscle strength, and decreased late-stage myofiber loss due to adipogenic infiltration. In contrast, the conventional glucocorticoid prednisolone failed to stabilize dysferlin deficient muscle cell membrane or improve repair of dysferlinopathic patient myoblasts and mouse myofibers. Instead, prednisolone treatment increased muscle weakness and myofiber atrophy in B6A/J mice—findings that correlate with reports of prednisolone worsening symptoms of LGMD2B patients. Our findings showing improved cellular and pre-clinical efficacy of vamorolone compared to prednisolone and better safety profile of vamorolone indicates the suitability of vamorolone for clinical trials in LGMD2B. Glucocorticoids are ineffective at treating muscular dystrophy (LGMD2B) caused by mutations in dysferlin gene, which causes poor muscle cell membrane repair. Sreetama et al. show that glucocorticoids can destabilize the dysferlin-deficient muscle cell membrane and further compromise their repair. A novel dissociative steroid in clinical trial reverses this effect and demonstrates therapeutic benefits in pre-clinical studies.

Original language	English
Pages (from-to)	2231-2242
Number of pages	12
Journal	Molecular Therapy
Volume	26
Issue number	9
DOIs	https://doi.org/10.1016/j.ymthe.2018.07.021
State	Published - Sep 5 2018

Keywords

LGMD2B
VBP15
dysferlinopathy
glucocorticoid
inflammation
membrane lipids
membrane repair
muscle injury
steroid

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10.1016/j.ymthe.2018.07.021

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title = "Membrane Stabilization by Modified Steroid Offers a Potential Therapy for Muscular Dystrophy Due to Dysferlin Deficit",

abstract = "Mutations of the DYSF gene leading to reduced dysferlin protein level causes limb girdle muscular dystrophy type 2B (LGMD2B). Dysferlin facilitates sarcolemmal membrane repair in healthy myofibers, thus its deficit compromises myofiber repair and leads to chronic muscle inflammation. An experimental therapeutic approach for LGMD2B is to protect damage or improve repair of myofiber sarcolemma. Here, we compared the effects of prednisolone and vamorolone (a dissociative steroid; VBP15) on dysferlin-deficient myofiber repair. Vamorolone, but not prednisolone, stabilized dysferlin-deficient muscle cell membrane and improved repair of dysferlin-deficient mouse (B6A/J) myofibers injured by focal sarcolemmal damage, eccentric contraction-induced injury or injury due to spontaneous in vivo activity. Vamorolone decreased sarcolemmal lipid mobility, increased muscle strength, and decreased late-stage myofiber loss due to adipogenic infiltration. In contrast, the conventional glucocorticoid prednisolone failed to stabilize dysferlin deficient muscle cell membrane or improve repair of dysferlinopathic patient myoblasts and mouse myofibers. Instead, prednisolone treatment increased muscle weakness and myofiber atrophy in B6A/J mice—findings that correlate with reports of prednisolone worsening symptoms of LGMD2B patients. Our findings showing improved cellular and pre-clinical efficacy of vamorolone compared to prednisolone and better safety profile of vamorolone indicates the suitability of vamorolone for clinical trials in LGMD2B. Glucocorticoids are ineffective at treating muscular dystrophy (LGMD2B) caused by mutations in dysferlin gene, which causes poor muscle cell membrane repair. Sreetama et al. show that glucocorticoids can destabilize the dysferlin-deficient muscle cell membrane and further compromise their repair. A novel dissociative steroid in clinical trial reverses this effect and demonstrates therapeutic benefits in pre-clinical studies.",

keywords = "LGMD2B, VBP15, dysferlinopathy, glucocorticoid, inflammation, membrane lipids, membrane repair, muscle injury, steroid",

author = "Sreetama, \{Sen Chandra\} and Goutam Chandra and \{Van der Meulen\}, \{Jack H.\} and Ahmad, \{Mohammad Mahad\} and Peter Suzuki and Shivaprasad Bhuvanendran and Kanneboyina Nagaraju and Hoffman, \{Eric P.\} and Jaiswal, \{Jyoti K.\}",

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doi = "10.1016/j.ymthe.2018.07.021",

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T1 - Membrane Stabilization by Modified Steroid Offers a Potential Therapy for Muscular Dystrophy Due to Dysferlin Deficit

AU - Sreetama, Sen Chandra

AU - Chandra, Goutam

AU - Van der Meulen, Jack H.

AU - Ahmad, Mohammad Mahad

AU - Suzuki, Peter

AU - Bhuvanendran, Shivaprasad

AU - Nagaraju, Kanneboyina

AU - Hoffman, Eric P.

AU - Jaiswal, Jyoti K.

PY - 2018/9/5

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N2 - Mutations of the DYSF gene leading to reduced dysferlin protein level causes limb girdle muscular dystrophy type 2B (LGMD2B). Dysferlin facilitates sarcolemmal membrane repair in healthy myofibers, thus its deficit compromises myofiber repair and leads to chronic muscle inflammation. An experimental therapeutic approach for LGMD2B is to protect damage or improve repair of myofiber sarcolemma. Here, we compared the effects of prednisolone and vamorolone (a dissociative steroid; VBP15) on dysferlin-deficient myofiber repair. Vamorolone, but not prednisolone, stabilized dysferlin-deficient muscle cell membrane and improved repair of dysferlin-deficient mouse (B6A/J) myofibers injured by focal sarcolemmal damage, eccentric contraction-induced injury or injury due to spontaneous in vivo activity. Vamorolone decreased sarcolemmal lipid mobility, increased muscle strength, and decreased late-stage myofiber loss due to adipogenic infiltration. In contrast, the conventional glucocorticoid prednisolone failed to stabilize dysferlin deficient muscle cell membrane or improve repair of dysferlinopathic patient myoblasts and mouse myofibers. Instead, prednisolone treatment increased muscle weakness and myofiber atrophy in B6A/J mice—findings that correlate with reports of prednisolone worsening symptoms of LGMD2B patients. Our findings showing improved cellular and pre-clinical efficacy of vamorolone compared to prednisolone and better safety profile of vamorolone indicates the suitability of vamorolone for clinical trials in LGMD2B. Glucocorticoids are ineffective at treating muscular dystrophy (LGMD2B) caused by mutations in dysferlin gene, which causes poor muscle cell membrane repair. Sreetama et al. show that glucocorticoids can destabilize the dysferlin-deficient muscle cell membrane and further compromise their repair. A novel dissociative steroid in clinical trial reverses this effect and demonstrates therapeutic benefits in pre-clinical studies.

AB - Mutations of the DYSF gene leading to reduced dysferlin protein level causes limb girdle muscular dystrophy type 2B (LGMD2B). Dysferlin facilitates sarcolemmal membrane repair in healthy myofibers, thus its deficit compromises myofiber repair and leads to chronic muscle inflammation. An experimental therapeutic approach for LGMD2B is to protect damage or improve repair of myofiber sarcolemma. Here, we compared the effects of prednisolone and vamorolone (a dissociative steroid; VBP15) on dysferlin-deficient myofiber repair. Vamorolone, but not prednisolone, stabilized dysferlin-deficient muscle cell membrane and improved repair of dysferlin-deficient mouse (B6A/J) myofibers injured by focal sarcolemmal damage, eccentric contraction-induced injury or injury due to spontaneous in vivo activity. Vamorolone decreased sarcolemmal lipid mobility, increased muscle strength, and decreased late-stage myofiber loss due to adipogenic infiltration. In contrast, the conventional glucocorticoid prednisolone failed to stabilize dysferlin deficient muscle cell membrane or improve repair of dysferlinopathic patient myoblasts and mouse myofibers. Instead, prednisolone treatment increased muscle weakness and myofiber atrophy in B6A/J mice—findings that correlate with reports of prednisolone worsening symptoms of LGMD2B patients. Our findings showing improved cellular and pre-clinical efficacy of vamorolone compared to prednisolone and better safety profile of vamorolone indicates the suitability of vamorolone for clinical trials in LGMD2B. Glucocorticoids are ineffective at treating muscular dystrophy (LGMD2B) caused by mutations in dysferlin gene, which causes poor muscle cell membrane repair. Sreetama et al. show that glucocorticoids can destabilize the dysferlin-deficient muscle cell membrane and further compromise their repair. A novel dissociative steroid in clinical trial reverses this effect and demonstrates therapeutic benefits in pre-clinical studies.

KW - LGMD2B

KW - VBP15

KW - dysferlinopathy

KW - glucocorticoid

KW - inflammation

KW - membrane lipids

KW - membrane repair

KW - muscle injury

KW - steroid

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DO - 10.1016/j.ymthe.2018.07.021

M3 - Article

C2 - 30166241

SN - 1525-0016

VL - 26

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JO - Molecular Therapy

JF - Molecular Therapy

IS - 9

ER -

Membrane Stabilization by Modified Steroid Offers a Potential Therapy for Muscular Dystrophy Due to Dysferlin Deficit

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Keywords

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