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TSC and LAM: Current Treatment Options and Clinical Trials

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TSC and LAM: Current Treatment Options and Clinical Trials Stephen Ruoss, MD Division of Pulmonary and Critical Care Medicine Stanford University School of Medicine – PowerPoint PPT presentation

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Title: TSC and LAM: Current Treatment Options and Clinical Trials


1
TSC and LAM Current Treatment Options and
Clinical Trials
  • Stephen Ruoss, MD
  • Division of Pulmonary and Critical Care Medicine
  • Stanford University School of Medicine

2
Outline
  • LAM disease and clinical background
  • Evolution of therapies for LAM
  • Future directions

3
Normal lung
4
CT image normal lung
5
CT images LAM
6
CT image TSC-LAM
7
Lymphangioleiomyomatosis (LAM)
  • systemic disease
  • multiple-organ involvement
  • progressive, cystic lung disease in women
  • associated with inappropriate activation of
    mammalian target of rapamycin (mTOR) signaling,
    which regulates cellular growth and lymphatic
    vessel development.
  • genetically mutant cells (LAM cells) that
    circulate in affected people are involved in
    organ injury

8
LAM sporadic vs. TSC-associated
Sporadic LAM TSC-LAM
Est. worldwide prevalence 35,000 (?) Est. worldwide TSC prevalence 200,000 (?)
Almost exclusively females LAM in 30-40 of females 10 of males
Only TSC2 mutations (after birth?) TSC1 and TSC2 mutations (germline)
50 have kidney angiomyolipomas 70-80 have kidney angiomyolipomas
gt 50 have respiratory symptoms lt 10 have respiratory symptoms
gt 60 have pneumothorax Pneumothorax rare
Chylothorax in 33 Chylothorax rare
9
Genes Involved in LAM
Chromosome 9
Chromosome 16
TSC1 gene
TSC2 gene
  • Cellular control
  • Cellular size
  • Cellular growth
  • Intracellular trafficking
  • Cell migration
  • Tumor suppression

HAMARTIN
TUBERIN
10
Genes Involved in LAM and TSC
1. TSC germline mutations of the TSC1 or TSC2
genes
altered TUBERIN and/or HAMARTIN
  • loss-of-function mutations, which can alter
  • Cellular size
  • Cellular growth
  • Intracellular trafficking
  • Cell migration
  • Tumor suppression

2. Sporadic LAM secondary mutations of TSC2
(only in LAM cells)
altered TUBERIN
11
Intracellular signaling pathways in LAM
insulin receptor
VEGFR3 (for VEGF-D)
PDGFR
(cell membrane)
P
P
IRS
PI3K
PDK1
estrogen receptor
Akt
TSC1
TSC2
Rheb
rictor
mTOR
raptor
mTOR
pS6
4EBP1
S6K
Lymphangiogenesis cell growth
Cell growth, movement
eIF4E
12
Intracellular signaling pathways in LAM
insulin receptor
VEGFR3 (for VEGF-D)
PDGFR
(cell membrane)
P
P
IRS
PI3K
PDK1
TSC mutations
estrogen receptor
Akt
TSC1
TSC2
Rheb
rictor
mTOR
raptor
mTOR
pS6
4EBP1
S6K
Lymphangiogenesis cell growth
Cell growth, movement
eIF4E
13
Intracellular signaling pathways in LAM
insulin receptor
VEGFR3 (for VEGF-D)
PDGFR
(cell membrane)
P
P
IRS
PI3K
PDK1
TSC mutations
estrogen receptor
Akt
TSC1
TSC2
Rheb
rictor
mTOR
raptor
mTOR
pS6
4EBP1
S6K
Lymphangiogenesis cell growth
Cell growth, movement
eIF4E
14
Cellular drug targets for LAM
insulin receptor
VEGFR3 (for VEGF-D)
PDGFR
(cell membrane)
P
P
IRS
PI3K
PDK1
anti-VEGF-D antibodies
TSC mutations
aromatase inhibitor
estrogen receptor
Akt
rapamycin (sirolimus)
TSC1
TSC2
statins
Rheb
rictor
metformin
mTOR
raptor
mTOR
pS6
4EBP1
S6K
Lymphangiogenesis cell growth
Cell growth, movement
eIF4E
15
Sirolimus studies LAM and TSC
NEJM 358(2) Jan 10, 2008
  • Therapy produced
  • AML volume reduction
  • Suggestion of improved lung function (small
    subject numbers)

16
Sirolimus studies LAM and TSC
  • Therapy produced
  • improved lung function
  • increasing use of this therapy in LAM patients

17
Disease-specific therapy LAM
18
Current Therapy Developments
19
MIDAS Trial Multicenter International
Durability and Safety of Sirolimus in LAM Trial
  • Purpose to determine if sirolimus (or
    everolimus) delays LAM progression
  • Eligibility Diagnosis of LAM, and are either
    currently taking sirolimus or everolimus, or
    being considered for therapy in the future
  • Methods
  • Annual visit to collect pulm. function results,
    quality-of-life questionnaire data, medications,
    clinical status data
  • more data will be collected if you attend your
    LAM clinic more frequently
  • No changes to your usual care/medications
  • Target 300 participants in U.S. followed for at
    least 2 yrs.
  • Cincinnati only site enrolling right now
    Stanford to follow

20
Other Current LAM Trials
  • SAIL Safety Study of Sirolimus and
    Hydroxychloroquine in Women with LAM (E. Henske,
    Harvard Univ.)
  • SOS Safety Study of Simvastatin (V. Krymskaya,
    U. Penn.)
  • SLAM-2 Preliminary clinical study of
    Saracatinib in Subjects with LAM (T. Eissa,
    Baylor Univ.)
  • GWAS LAM Genome Wide Association Study (D.
    Kwiatkowski, Harvard Univ.)

21
Future directions
  • Better understanding of the origins, biology, and
    control of LAM cells
  • Role(s) of lymphatics in LAM
  • VEGF-D as therapy target (blocking abnormal
    lymphatic growth, and LAM cell circulation)
  • Cellular metabolic regulation in LAM
  • Roles(s) of estrogen in LAM
  • Combination therapies
  • Optimal clinical studies organization,
    coordination

22
More information access
  • www.thelamfoundation.org
  • Facebook page
  • Lammies page
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