PARKIN GT Expression Timeline And Parkin Delivery Evidence
Parkin Gene/Protein Delivery In Vivo Continuation
| Model / row label | Study / citation | Intervention / timing | Result notes |
|---|---|---|---|
MPTP mice | (Paterna et al. 2007, PMID 17299411) | mice treated transiently with MPTP; preventive, Parkin overexpression; AAV2-Parkin into unilateral SN; after 21-26 days; MPTP Injection (ip, 4 consecutive); 7 days after MPTP, killing -> analysis | prevented DA cell loss; But no effect on striatal DA, DOPAC, HVA (fig 2b,c,d); possible explanation that surviving TH neurons may be compromised in ability to synthesize dopamine |
MPTP mice | (Yasuda et al. 2011, PMID 21760537) | chronic MPTP-Minipump mouse; preventive, Parkin overexpression; AAV-Parkin into unilateral SN; after 14 days; MPTP pump implantation; At 7 or 28 days after implantation of the minipumps, killing -> analysis | prevented motor deficits & DA cell loss; But no effect on striatal DA, DOPAC, HVA (fig 4a,b,c); discrepancy may be related to enhanced dopamine release of surviving DA neurons that overexpress parkin |
6OHDA Rat | (Vercammen et al. 2006, PMID 16914382) | Lentiviral vectors encoding human WT parkin were stereotactically injected into the SN 2 weeks prior to a striatal 6-OHDA lesion; preventive | no report on DA, DOPAC, HVA |
6OHDA Mice | (Chung et al. 2020, PMID 32494688) Cellivery | iCP-Parkin (iCP=intracellular delivery of CPP-Parkin protein); (iv delivery) in 6OHDA mice/Rat or AAV-aSyn mice model; pff 용어는 미사용 |
Chung / Cellivery note:
Takeshi) To overcome solubility issue (otherwise precipitate) -> they added solubilization domain
to produce iCP-Parkin. Even though they adopt this strategy, they couldn't produce soluble
protein in E.coli. Although they refold insoluble iCP-Parkin from the inclusion body, iCP-Parkin
has not a correct structure, resulting in constitutive active protein (?).iCP-Parkin Model Notes
Parkin-KO Mouse 아니니 parkin level 안 봄!
1. Mouse: (fig5A), 6OHDA unilateral lesioning -> 4일후 ICP-PARKIN (for 3 days)
(icp-parkin 직전에) apomorphine rotation test로 확인했으니 (FIG5E, DA loss 도 봤고)
Symptomatic 이네 (이 시점에 ↓ DA일것) therapeutic!
-> 6ohda lesioning으로부터 12일 후 kill -> TH level을 아예 No Tx group의 90%수준으로 만들었네,
(figS6d) restored COX4 & VDAC1, pole test에서 slowing progression 아니라
치료첫날부터 호전시켰고, 시간이 지나면서 vehicle 군은 거의 불변인데, 치료군은 BL보다 improved. (fig5c)
2. Rat: (fig5G), 6OHDA unilateral lesioning -> 2w후 ICP-PARKIN (for 4 w)
(icp-parkin 직전에) apomorphine rotation test로 확인했으니 (FIG5j,k, DA loss 도 봤고)
Symptomatic 이네 therapeutic! (이 시점에 ↓ DA일것)
-> 7주후 kill -> TH level을 No Tx group의 80-90%수준으로 만들었네
normalized DA loss, rotarod 에서 slowing progression 아니라 치료첫날부터 호전시켰고,
시간이 지나면서 vehicle 군은 거의 불변인데 치료군은 BL보다 improved. (fig5h)
3. Mouse: (fig s7) MPTP lesioning -> 4d후 ICP-PARKIN (for 4d) -> 8d 후 kill
-> ↑ rotarod 에서 치료첫날부터 호전시켰음., TH not quantified
4. Mouse: (fig6a), AAV-(human WT) aSyn administration -> 8주후 ICP-PARKIN (30 mg/kg)
was intravenously injected three times per week for 4 weeks
(icp-parkin 직전에) apomorphine rotation test로 확인했으니 (FIG5j,k, DA loss 도 봤고)
Symptomatic 이네 therapeutic! -> normalized preventive아니라 therapeutic!
-> 12주후 kill -> restored DA loss (fig 6c, no quantification), ↓ aSy (fig 6d,e),
rotarod에서 vehicle군은 시간에 따른 변화 무, 치료군은 BL보다 호전
5. Mouse: (fig6f), AAV-aSyn administration -> 8주후 ICP-PARKIN (10 mg/kg)
was intravenously injected three times per week for 4 weeks
(icp-parkin 직전에) apomorphine rotation test로 확인했으니 preventive아니라 therapeutic!
-> TH level을 No Tx group의 90%수준으로 만들었네 (fig 6h),
↓ aSy (fig 6h,j), Pole test에서 vehicle군은 악화되고 치료군은 BL 대비 불면Summary:
종평: 대체로 Sx reversal 을 보였고, TH level 도 (vehicle treated 군의 80-90%를 달성했으니)
reversal 을 보인 듯 함, author's argument on mechanism: TH level are neuronal loss are separate process.
Parkin -> TH expression (measured by IHC) -> DABian MPTP Mouse And p62/SQSTM1 Notes
Bian row:
| Model / row label | Study / citation | Intervention / model | Result notes |
|---|---|---|---|
MPTP mice | (Bian et al. 2012, PMID 22792139) | Parkin (preventive Parkin overexpressing) TG mouse model in which expression of WT parkin was driven by neuron specific enolase (NSE) promoter. | ↑ parkin mRNA by 2x (fig 1c), ↑ parkin protein by 1.5x (fig 1d), ↑ TH-positive cells (fig2), ↓ damaged mt (fig 3, only ~20%), ↓ aSyn (fig6), no report on DA, DOPAC, HVA |
p62/SQSTM1 note:
p62/SQSTM1
- a multi-signaling adaptor molecule
- can directly interact with ubiquitin and LC3, promoting autophagic degradation of ubiquitinated aggregated proteinSymptomatic row:
| Section | Study / row | Model | Result |
|---|---|---|---|
Symptomatic | (Manfredsson, 2007 #1763) | 6OHDA rat + AAV Parkin | 미저장으로 인해, 추후 작성) =TH+ neurons, =striatal TH, ↑NIGral TH, ↑(DOPAC, HVA 등), ↓Amphetamine-induced rotation |
PARKIN GT Executive Summary And Expression Timeline
Milestone headers and fragments:
| Column / milestone | Text |
|---|---|
PARKIN GT | Expression cassette test (plasmid): 12 tested -> 9 identified & nominated as candidates of lead cassette for LGE |
LGE | 2020 Oct; To select Expression cassette (여전히 cassette임) in AAV tools |
PE | 2021 /12 |
CN | 2023 10 (on manufacturing of xx) |
CS | 2024/06 ->; EDE: ? ->; IND 2025/86 ->; P1 start ? |
In Vitro Expression
Text:
iPSC-DA neurons (WT & Parkin KO), Cell lines (HEK293 at GGTR,
Glial cell type: U87 > 1-fold expression compared to endogenous, WT Parkin
-> 9 cassettes were selected (rAAV9-PK031, rAAV9-PK022, rAAV9-PK030,
rAAV9-PK012, rAAV9-PK013, rAAV9-PK023, rAAV9-PK024, rAAV9-PK025, rAAV9-PK026)Continuation in LGE/expression column:
iPSC-DA neurons (WT & Parkin KO), Cell lines:
9 cassettes (근데 cassette대신에 계속 vector prioritization이라 칭하네?)
to be tested in two AAV tools (AAV5 & 9) -> ~5 exp cassette will be selected
for in vivo expression test (Parkin KO mice, ICM).
20210202 & 20210315:
AAV9-Parkin ->
1) ↑ (매우많이) transgene expression
2) ↑ PHOSPHO-UBIQUITIN
3) ↑ mitophagy (reversed 증가되었던 TOM20)CS column in-vitro note:
iPSC-DA neurons (KO, R275W): -> phospho-poly Ubiquitin,
>50% neuroprotection 이 실험이 decision tree에는 xIn Vivo Mouse Expression
Text:
In vivo expression:
(Parkin KO mouse, 4 m old (젊은쥐)
20210617) 6 exp cassette with AAV9 were tested
): ICM rAAV9 administration of (1x10**) vg/10 uL injection, single injection,
(n=7 per cassette)
) -> dissection 1.5 m post-injection -> analysis (ELISA, IHC):
> 1-fold expression compared to endogenous WT Parkin,Later POC columns:
[in vivo POC: 6ohda + Parkin KO]
Necropsy was finished on June 1st. Flash report will be available in early July.
in vivo POC: MPTP + Parkin KO
-> dose finding study (final product), May-Nov2023Uncertain Spans
nav_path: lower half clearly startsPARKIN GT (Takeshi Hioki, PFR-4249-100), but the upper half is a continuation of Parkin PD / Parkin GT in-vivo evidence from20240722_182007.- Manfredsson row was apparently added later after an unsaved state (
미저장으로 인해, 추후 작성); treat the entire result row as provisional. - The vector dose in the in-vivo expression row appears as
(1x10**) vg/10 uL; the exponent is not safely readable. 2025/86may be2025/8?,2025/6?, or another date-like notation; leave unresolved.