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stem cells applications in hurler syndrome

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Stem cell applications in mucopolysaccharidosis type 1 ( hurler syndrome )
Mucopolysaccharidosis type I (MPS I) is a rare disease in which the body is missing or does not have enough of an enzyme needed to break down long chains of sugar molecules. This disorder was once divided into three separate syndromes: 1- Hurler syndrome (MPS I-H) 2-Hurler-Scheie syndrome (MPS I-H/S) 3-Scheie syndrome (MPS I-S) Symptoms: A-macrocephaly B-hydrocephalus C- heart valve abnormalities D- hepatosplenomegaly E- macroglossia F - dysostosis multiplex G- airway become narrow and this will lead to : 1-upper respiratory infection 2- sleep apnea A B C D E F
CAUSES: Mutations in the IDUA gene cause MPS I. The IDUA gene provides instructions for producing an enzyme that is involved in the breakdown of large sugar molecules called glycosaminoglycans (GAGs). Mutations in the IDUA gene reduce or completely eliminate the function of the IDUA enzyme. The lack of IDUA enzyme activity leads to the accumulation of GAGs within cells, specifically inside The lysosomes. Conditions that cause molecules to build up inside the lysosomes, including MPS I, are called lysosomal storage disorders. Children with this form of the disorder usually have a shortened lifespan, sometimes living only into late childhood.
Delivery of a-L-iduronidase may be achieved by either the exogenous administration of a- L-iduronidase or through the endogenous production of a-L-iduronidase following stable engraftment of cells producing enzyme within the affected individual. The first experience with hematopoietic stem cell transplantation (HSCT) as therapy for Hurler was reported by Hobbs, and since that time HSCT has been accepted as the standard of care for patients with MPS IH. Data from our institution as well as others indicate that there is an increased risk of pulmonary and cardiac complications after HSCT in patients with MPS IH.
NO STUDY TITLE STATUS 1 Stem Cell Transplantation for Hurler Completed 2 Stem Cell Transplant w/Laronidase for Hurler Completed 3 Laronidase (Aldurazyme TM) Enzyme Replacement Therapy With Hematopoietic Stem Cell Transplant for Hurler Syndrome Terminated 4 Gene Therapy With Modified Autologous Hematopoietic Stem Cells for the Treatment of Patients With Mucopolysaccharidosis Type I, Hurler Variant Active, not recruiting 5 Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Completed 6 Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Completed
Hematopoietic Stem Cell Transplantation for Hurler Syndrome, Maroteaux Lamy Syndrome (MPS VI), and Alpha Mannosidase Deficiency (Mannosidosis) OBJECTIVE: to determine the safety and engraftment of donor hematopoietic cells PATIENTS: NO: 41 AGE: <=18 years FEMALE : 23 MALE : 18 Region of Enrollment: United States Patients with Mucopolysaccharidosis, type I (e.g., Hurler syndrome) Cardiac: ejection fraction >40%; no decompensated congestive heart failure or uncontrolled arrhythmia Hepatic: total bilirubin <3x Upper limits of normal transaminases < 5.0 x Upper limits of normal Brain MRI of a child with moderate Hunter syndrome showing multiple patchy white matter lesions in the periventricular and subcortical areas. Age: 11 years.
Prior to transplantation, subjects will receive Busulfan intravenously (IV) via the Hickman line four times daily for 4 days. Cyclophosphamide intravenously via the Hickman line once a day for 4 days. Anti-Thymocyte Globulin IV via the Hickman line twice daily for three days before the transplant. These three drugs are being given to subjects to help the new marrow "take" and grow. On the day of transplantation, the donor's hematopoietic cells will be transfused via central venous catheter. After hematopoietic cell transplant, subjects will then receive two drugs, Cyclosporin and methylprednisolone or MMF are given to help prevent the complication of graft-versus-host disease and to decrease the chance that the new donor cells will be rejected.
Results Number of Patients Surviving on Study Number of Patients Who Failed Engraftment. Number of Patients Who Failed Engraftment. 1 patient of 41 failed engraftment Number of Patients With Grade III-IV Acute Graft-versus-host Disease (aGVHD). Based on variability in age, diagnosis and condition of these patients, the data on enzyme levels and neuropsych testing is extremely difficult to report.
Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Owing to few studies documenting long-term survival of these children treated with HSCT this study has been done. Patients : The diagnosis of HS was confirmed by an increase in urinary GAG excretion, a deficiency or absence of IDUA in peripheral blood leukocytes, and the clinical phenotype. 54 children with HS born. Of the 39 patients alive-andengrafted after first and second HSCT, six patients were followed-up at other centers and alive when we contacted their centers prior to submission of the review. Thirty-three patients were finally included for evaluation of disease-related cardiopulmonary burden.
RESULTS: 1- The outcome of the 54 children is illustrated in Fig. 1. Of the 18 patients with graft failure, 17 received a second HSCT while one was lost to continuing follow-up after returning to the referring overseas center. 2- Of the 14 deaths after HCST, 13 died of transplant related mortality and one died of disease-related heart failure. Four children died of graftversus-host disease and one died of EBV post- transplant lymphoproliferative disease (PTLD). 3-all deaths occurred within the first year after HSCT and there was no late death in our cohort. The overall survival at 20-years was 73.7% (95% confidence interval 60.3-83.5%).
Phase II Study of Combined Laronidase (AldurazymeTM) Enzyme Replacement Therapy (ERT) With Hematopoietic Stem Cell Transplantation (HSCT) for Hurler Syndrome (MPS IH) To investigate that weekly infusions of Laronidase ERT for 10-12 weeks prior to transplant and 8 weeks following transplant will result in a reduction of glycosaminoglycans (GAG) burden that is associated with decreased complications following transplant. Patients: NO: 25 AGE: <=18 years FEMALE : 11 MALE : 11 Region of Enrollment : United States, Minnesota
Results Number of Patients Alive at One Year Post Transplant (one year) Number of Patients Requiring Ventilator Support at One Year Post Transplant Patients With Grade III-IV Acute GVHD
Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Objective :To determine whether enzyme replacement therapy (ERT) with iduronidase in the peritransplant period affects outcome of hematopoietic stem cell transplantation (HSCT) for MPS IH. Patients : NO: 7 with MPS IH (All patients had null mutations in IDUA gene) Age :median age of 1.5 years Between 2004 and 2007, seven patients received allogeneic HSCT with ERT (Table 1). Outcomes were assessed at least 6 months after transplantation. Follow-up is reported through August 2007 (median 1.1 years).
For ERT, a-L-iduronidase (Laronidase; Genzyme Corporation, Cambridge, MA, USA) was administered weekly at a dose of 0.58 mg/kg per dose i.v. for 11–14 weeks prior to HSCT and for additional 8 weeks after HSCT. The goal of this dosing was to provide a source of exogenous a-L-iduronidase from the time of diagnosis until stable donor chimerism was achieved.
Results 1- Two patients developed skin GvHD. Patient 1 had stage 3 grade C GvHD and patient 4 had stage 2 grade B GvHD. 2- we have observed that MPS IH patients with a history of pulmonary disease including a history of pneumonia or reactive airway disease had worse outcomes than those who were free from pulmonary issues before HSCT 3- We reasoned that ERT before transplant could have a potential to decrease the GAG burden in the lung and other visceral tissues. As a result, regimen-related morbidity and mortality of HSCT could potentially be decreased. 4- Five out of seven MPS IH patients had two or more risk factors a finding that we have observed to be associated with significant morbidity and mortality in MPS IH patients treated with HSCT alone.
Four pretransplant risk factors (pneumonia, abnormal sleep study with apnea, reactive airway disease and need for supplemental oxygen) were assessed (Table 2). • Combination therapy results in low overall morbidity and normal a-L-iduronidase levels. • suggesting an overall decrease in GAG visceral burden. a-L-iduronidase leukocyte levels were measured following HSCT. As expected on the basis of robust donor engraftment in all patients, enzyme levels were within the normal range after HSCT.
Recommendations: • the effect of ERT and HSCT provides evidence that this combination therapy is safe, and does not negatively impact on donor stem cell engraftment and GvHD. • we have observed low morbidity after ERT þ HSCT combination therapy despite significant pulmonary risk factors present before HSCT. • our data indicate that despite the expected formation of anti-a-L- iduronidase antibodies, no evidence of immune-mediated graft rejection was observed in MPS IH patients receiving pre-HSCT ERT. • it is possible that ERT-mediated GAG clearance in the bone marrow niche could create a more permissive environment for donor engraftment31 when compared to patients who are recipients of HSCT alone. • our recommendation is to treat all severe MPS IH patients with ERT and HSCT to improve morbidity and mortality. • .
References • Lum, S. H., Stepien, K. M., Ghosh, A., Broomfield, A., Church, H., Mercer, J., ... & Wynn, R. (2017). Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Journal of inherited metabolic disease, 40(3), 455-460. • Tolar, J., Grewal, S. S., Bjoraker, K. J., Whitley, C. B., Shapiro, E. G., Charnas, L., & Orchard, P. J. (2008). Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Bone marrow transplantation, 41(6), 531-535. • Boelens JJ. Trends in haematopoietic cell transplantation for inborn errors of metabolism. J Inherit Metab Dis 2006; 29: 413–420. • Bijarnia S, Shaw P, Vimpani A, Smith R, Pacey V, O’Grady H, Christodoulou J, Sillence D (2009) Combined enzyme replacement and haematopoietic stem cell transplantation in Hurler syndrome. J Paediatr Child Health 45(7-8):469–472 • Tolar J, Grewal SS, Bjoraker KJ, Whitley CB, Shapiro EG, Charnas L, Orchard PJ (2008) Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Bone Marrow Transplant 41(6):531–535. • 9 Grewal SS, Krivit W, Defor TE, Shapiro EG, Orchard PJ, Abel SL et al. Outcome of second hematopoietic cell transplantation in Hurler syndrome. Bone Marrow Transplant 2002; 29: 491–496.

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stem cells applications in hurler syndrome

  • 1. Stem cell applications in mucopolysaccharidosis type 1 ( hurler syndrome )
  • 2. Mucopolysaccharidosis type I (MPS I) is a rare disease in which the body is missing or does not have enough of an enzyme needed to break down long chains of sugar molecules. This disorder was once divided into three separate syndromes: 1- Hurler syndrome (MPS I-H) 2-Hurler-Scheie syndrome (MPS I-H/S) 3-Scheie syndrome (MPS I-S) Symptoms: A-macrocephaly B-hydrocephalus C- heart valve abnormalities D- hepatosplenomegaly E- macroglossia F - dysostosis multiplex G- airway become narrow and this will lead to : 1-upper respiratory infection 2- sleep apnea A B C D E F
  • 3. CAUSES: Mutations in the IDUA gene cause MPS I. The IDUA gene provides instructions for producing an enzyme that is involved in the breakdown of large sugar molecules called glycosaminoglycans (GAGs). Mutations in the IDUA gene reduce or completely eliminate the function of the IDUA enzyme. The lack of IDUA enzyme activity leads to the accumulation of GAGs within cells, specifically inside The lysosomes. Conditions that cause molecules to build up inside the lysosomes, including MPS I, are called lysosomal storage disorders. Children with this form of the disorder usually have a shortened lifespan, sometimes living only into late childhood.
  • 4. Delivery of a-L-iduronidase may be achieved by either the exogenous administration of a- L-iduronidase or through the endogenous production of a-L-iduronidase following stable engraftment of cells producing enzyme within the affected individual. The first experience with hematopoietic stem cell transplantation (HSCT) as therapy for Hurler was reported by Hobbs, and since that time HSCT has been accepted as the standard of care for patients with MPS IH. Data from our institution as well as others indicate that there is an increased risk of pulmonary and cardiac complications after HSCT in patients with MPS IH.
  • 5. NO STUDY TITLE STATUS 1 Stem Cell Transplantation for Hurler Completed 2 Stem Cell Transplant w/Laronidase for Hurler Completed 3 Laronidase (Aldurazyme TM) Enzyme Replacement Therapy With Hematopoietic Stem Cell Transplant for Hurler Syndrome Terminated 4 Gene Therapy With Modified Autologous Hematopoietic Stem Cells for the Treatment of Patients With Mucopolysaccharidosis Type I, Hurler Variant Active, not recruiting 5 Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Completed 6 Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Completed
  • 6. Hematopoietic Stem Cell Transplantation for Hurler Syndrome, Maroteaux Lamy Syndrome (MPS VI), and Alpha Mannosidase Deficiency (Mannosidosis) OBJECTIVE: to determine the safety and engraftment of donor hematopoietic cells PATIENTS: NO: 41 AGE: <=18 years FEMALE : 23 MALE : 18 Region of Enrollment: United States Patients with Mucopolysaccharidosis, type I (e.g., Hurler syndrome) Cardiac: ejection fraction >40%; no decompensated congestive heart failure or uncontrolled arrhythmia Hepatic: total bilirubin <3x Upper limits of normal transaminases < 5.0 x Upper limits of normal Brain MRI of a child with moderate Hunter syndrome showing multiple patchy white matter lesions in the periventricular and subcortical areas. Age: 11 years.
  • 7. Prior to transplantation, subjects will receive Busulfan intravenously (IV) via the Hickman line four times daily for 4 days. Cyclophosphamide intravenously via the Hickman line once a day for 4 days. Anti-Thymocyte Globulin IV via the Hickman line twice daily for three days before the transplant. These three drugs are being given to subjects to help the new marrow "take" and grow. On the day of transplantation, the donor's hematopoietic cells will be transfused via central venous catheter. After hematopoietic cell transplant, subjects will then receive two drugs, Cyclosporin and methylprednisolone or MMF are given to help prevent the complication of graft-versus-host disease and to decrease the chance that the new donor cells will be rejected.
  • 8. Results Number of Patients Surviving on Study Number of Patients Who Failed Engraftment. Number of Patients Who Failed Engraftment. 1 patient of 41 failed engraftment Number of Patients With Grade III-IV Acute Graft-versus-host Disease (aGVHD). Based on variability in age, diagnosis and condition of these patients, the data on enzyme levels and neuropsych testing is extremely difficult to report.
  • 9. Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Owing to few studies documenting long-term survival of these children treated with HSCT this study has been done. Patients : The diagnosis of HS was confirmed by an increase in urinary GAG excretion, a deficiency or absence of IDUA in peripheral blood leukocytes, and the clinical phenotype. 54 children with HS born. Of the 39 patients alive-andengrafted after first and second HSCT, six patients were followed-up at other centers and alive when we contacted their centers prior to submission of the review. Thirty-three patients were finally included for evaluation of disease-related cardiopulmonary burden.
  • 10. RESULTS: 1- The outcome of the 54 children is illustrated in Fig. 1. Of the 18 patients with graft failure, 17 received a second HSCT while one was lost to continuing follow-up after returning to the referring overseas center. 2- Of the 14 deaths after HCST, 13 died of transplant related mortality and one died of disease-related heart failure. Four children died of graftversus-host disease and one died of EBV post- transplant lymphoproliferative disease (PTLD). 3-all deaths occurred within the first year after HSCT and there was no late death in our cohort. The overall survival at 20-years was 73.7% (95% confidence interval 60.3-83.5%).
  • 11. Phase II Study of Combined Laronidase (AldurazymeTM) Enzyme Replacement Therapy (ERT) With Hematopoietic Stem Cell Transplantation (HSCT) for Hurler Syndrome (MPS IH) To investigate that weekly infusions of Laronidase ERT for 10-12 weeks prior to transplant and 8 weeks following transplant will result in a reduction of glycosaminoglycans (GAG) burden that is associated with decreased complications following transplant. Patients: NO: 25 AGE: <=18 years FEMALE : 11 MALE : 11 Region of Enrollment : United States, Minnesota
  • 12. Results Number of Patients Alive at One Year Post Transplant (one year) Number of Patients Requiring Ventilator Support at One Year Post Transplant Patients With Grade III-IV Acute GVHD
  • 13. Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Objective :To determine whether enzyme replacement therapy (ERT) with iduronidase in the peritransplant period affects outcome of hematopoietic stem cell transplantation (HSCT) for MPS IH. Patients : NO: 7 with MPS IH (All patients had null mutations in IDUA gene) Age :median age of 1.5 years Between 2004 and 2007, seven patients received allogeneic HSCT with ERT (Table 1). Outcomes were assessed at least 6 months after transplantation. Follow-up is reported through August 2007 (median 1.1 years).
  • 14. For ERT, a-L-iduronidase (Laronidase; Genzyme Corporation, Cambridge, MA, USA) was administered weekly at a dose of 0.58 mg/kg per dose i.v. for 11–14 weeks prior to HSCT and for additional 8 weeks after HSCT. The goal of this dosing was to provide a source of exogenous a-L-iduronidase from the time of diagnosis until stable donor chimerism was achieved.
  • 15. Results 1- Two patients developed skin GvHD. Patient 1 had stage 3 grade C GvHD and patient 4 had stage 2 grade B GvHD. 2- we have observed that MPS IH patients with a history of pulmonary disease including a history of pneumonia or reactive airway disease had worse outcomes than those who were free from pulmonary issues before HSCT 3- We reasoned that ERT before transplant could have a potential to decrease the GAG burden in the lung and other visceral tissues. As a result, regimen-related morbidity and mortality of HSCT could potentially be decreased. 4- Five out of seven MPS IH patients had two or more risk factors a finding that we have observed to be associated with significant morbidity and mortality in MPS IH patients treated with HSCT alone.
  • 16. Four pretransplant risk factors (pneumonia, abnormal sleep study with apnea, reactive airway disease and need for supplemental oxygen) were assessed (Table 2). • Combination therapy results in low overall morbidity and normal a-L-iduronidase levels. • suggesting an overall decrease in GAG visceral burden. a-L-iduronidase leukocyte levels were measured following HSCT. As expected on the basis of robust donor engraftment in all patients, enzyme levels were within the normal range after HSCT.
  • 17. Recommendations: • the effect of ERT and HSCT provides evidence that this combination therapy is safe, and does not negatively impact on donor stem cell engraftment and GvHD. • we have observed low morbidity after ERT þ HSCT combination therapy despite significant pulmonary risk factors present before HSCT. • our data indicate that despite the expected formation of anti-a-L- iduronidase antibodies, no evidence of immune-mediated graft rejection was observed in MPS IH patients receiving pre-HSCT ERT. • it is possible that ERT-mediated GAG clearance in the bone marrow niche could create a more permissive environment for donor engraftment31 when compared to patients who are recipients of HSCT alone. • our recommendation is to treat all severe MPS IH patients with ERT and HSCT to improve morbidity and mortality. • .
  • 18. References • Lum, S. H., Stepien, K. M., Ghosh, A., Broomfield, A., Church, H., Mercer, J., ... & Wynn, R. (2017). Long term survival and cardiopulmonary outcome in children with Hurler syndrome after haematopoietic stem cell transplantation. Journal of inherited metabolic disease, 40(3), 455-460. • Tolar, J., Grewal, S. S., Bjoraker, K. J., Whitley, C. B., Shapiro, E. G., Charnas, L., & Orchard, P. J. (2008). Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Bone marrow transplantation, 41(6), 531-535. • Boelens JJ. Trends in haematopoietic cell transplantation for inborn errors of metabolism. J Inherit Metab Dis 2006; 29: 413–420. • Bijarnia S, Shaw P, Vimpani A, Smith R, Pacey V, O’Grady H, Christodoulou J, Sillence D (2009) Combined enzyme replacement and haematopoietic stem cell transplantation in Hurler syndrome. J Paediatr Child Health 45(7-8):469–472 • Tolar J, Grewal SS, Bjoraker KJ, Whitley CB, Shapiro EG, Charnas L, Orchard PJ (2008) Combination of enzyme replacement and hematopoietic stem cell transplantation as therapy for Hurler syndrome. Bone Marrow Transplant 41(6):531–535. • 9 Grewal SS, Krivit W, Defor TE, Shapiro EG, Orchard PJ, Abel SL et al. Outcome of second hematopoietic cell transplantation in Hurler syndrome. Bone Marrow Transplant 2002; 29: 491–496.