Krabbe psychosine continued, KD subtypes, Pipeline of KD, MOA for PD, Monthly Report (AC Inhibitor), Safety / Target validation
Krabbe psychosine continued
뇌의 전영역에서 (late-onset KD 도 WM, Caudate 에선 증가로 매우 evident).
In vivo
- Infantile onset
- the late infantile/juvenile (1-16 years) and adult (>16 years)
The latter type includes a spectrum of late infantile-onset (7 months to 2 years), juvenile-onset (3-8 years) and adult onset (>9 years) onset KD (Xu, Sakai, Tanike, Inui, & Ozono, 2006)
usually die before the age of 2-3 years.
a slower rate than infantile patients with some adults living until the sixth decade with mild symptoms.
The disease is generally fatal 2-7 years after the symptoms
Pipeline of KD
https://www.businesswire.com/news/home/20230117005486/en
MOA for PD
↓ GALC activity → ↑ psychosine → ↑ aSyn
| post mortem (Marshall, 2018 #2200) | |
|---|---|
| GALC activity | fig 1 (M, N, O, P) WM 에서만 ↑ |
| ↑ psychosine | (Marshall, 2018 #2200) fig 1 (e, f, g, h, Q) GM 에서만 증가 |
| severe GALC mutation PD patient 에서 psychosine 더 높음 | |
| Niigata: ↑ psychosine | Amygdala: d=0.72 (76% of control would be below average person in PD group), Occipital: d=0.01 |
(Marshall, 2018 #2200) correlation between psychosine and GALC activity is small (r²=0.13)
isoluble truncated aSyn and oligomer were observed after GalSph treatment (in-house data). aSyn truncation may be caused by abnormality of lysosomal proteases (J. Biol. Chem. (2020) 295(30) 10224-10244)
(Marshall, 2018 #2200) In vitro, psychosine accelerates aggregation of a-syn [8] by direct binding to the carboxy-terminus and facilitation of an aggregation-prone protein conformation (Abdelkarim, …)
In house) GALC KD or AC OE → ↑ aSyn (insoluble) oligomer; severe GALC mutation PD patient 에서 psychosine 더 높음 (d=0.53)
(Smith, 2014 #2199), (Abdelkarim, 2018 #2201) genetic correction of GALC deficiency completely prevents a-syn aggregation. Genetic KO of a-syn reduces, but does not completely prevent, neurological signs in a mouse model of KD.
Monthly Report (AC Inhibitor) 202101
GlcSph reduction in iPSC-DaNs (L444P/L444P), 14 days treatment.
Concentration (nM) ratio (n=) groups visible:
- Sanofi GCSi
- Takeda ACi
- rhGBA
- Venglustat
- T-4343016
- T-4178815
- T-4889033 (BT GA4 LAMA4/ALP)
- T-1xxx0C8
- Cerezyme (U/mL)
p-α-Syn (induced by PFF) reduction in mouse primary neurons:
- Y-axis: Normalized Phospho-α-Syn DxA by Nuclei number
- Series: DMSO, 10 μM T-4378886, 10 μM T-3269966
- X-axis: mPFF concentration (ng/mL) 0.1 to 100
Ceramide, GlcCer and Sph levels was not changed by ACi.
202102 Pipeline preclinical
(Caputo, 2020 #1196) (Di Martino, 2020 #1197) — SH-SY5Y compound: 4d (their lead compound, IC50 = 166 nM, Figure 2 and Table S1) as a lead compound with good oral bioavailability, excellent brain penetration, and target engagement in two animal models of neuropathic GD and KD.
Safety
- carmofur has been known to induce leukoencephalopathy, characterized by progressive damage to white matter in the brain with stroke-like symptoms. [8],[9],[10]
- Carmofur: A clinical trial for small hepatocellular carcinoma was stopped prematurely because 56% of the treated patients had unacceptable side effects.
- genetic loss of ACDase activity → Farber disease: Systemic nodules and inflammation, neurologic deterioration, and hepatosplenomegaly with ceramide accumulation
- Spinal muscular atrophy with progressive myoclonic epilepsy (SMA-PME) (1)
- SMA-PME: Epileptic disorder with lower motor neuron dysfunction related to ceramide metabolism (2)
Safety BM
- Carmofur: A clinical trial for small hepatocellular carcinoma was stopped prematurely because 56% of the treated patients had unacceptable side effects.
- genetic loss of ACDase activity → Farber disease: Systemic nodules and inflammation, neurologic deterioration, and hepatosplenomegaly with ceramide accumulation
- → SMA-PME: Epileptic disorder with lower motor neuron dysfunction related to ceramide metabolism (2)
- Monitor ceramide level in vitro / in vivo
- Representative inhibitors did not show effect on ceramide level in GBA KO HAP1 cells
- TSR suggested liver pathology would be sensitive indicator of ACi on target toxicity
- Safety margin will be estimated with front-loaded schedule
- aSyn leading to the slowing of disease progression. AC inhibition might lead to ceramide increase.
- We need to assess safety in the increase of GalCer and Ceramide, although current data does not indicate a ceramide increase as there are multiple pathways to process.
Target validation and correction
Where? (Kim, #1185) carmofur GBA KO cells (HEK293-FT cells)
| Pre-Tx | Post-Tx | |
|---|---|---|
| ↑ (~20%) Protein levels of acid ceramidase | ||
| ↓ GlcSph | ||
| ↑ Cer | ||
| ↑ GlcCer | ||
| C14-GluCer | A → No effect | B |
| GluSph | 15-… | C16-Cer C18-Cer |
Figure 7. Carmofur treatment reverts reduced ceramide levels and increases GluSph levels in GCase-deficient cells. Wild-type and GCase-deficient cells were treated with either DMSO or carmofur for ~20 h. After drug treatments, total lipids were extracted and measured as described in the Materials and Methods section. Lipid analysis results were expressed as lipid levels of picomoles (pmol)/three million cells. Levels of GluSph, GluCer species and dihydroceramide (A), and ceramide species (B) are shown. For each group, three independent samples were analyzed. Data represent mean ± SEM. Two-tailed unpaired t-test, *p<0.001, **p<0.01,
↓ GalCer (AC적으니 당연), ↑ mature (50 kDa) GalCer 중 C18:1 만 증가시킴
↑ AC activity, ↑ Cer, ↑ sphingosine, = SM, ↑ HexCer
Uncertain Spans
| location | transcription | uncertainty |
|---|---|---|
| Monthly Report compound list | T-1xxx0C8 | reads as written; the partially-clipped compound code is preserved verbatim. |