20240722_183255

	Possible reason
Low SB on 6OHDA in both ARG and homogenate	Low NLRP3 expression? (but well-detected in NLRP3 GoF homogenate) NLRP3 instability - eg. freeze/thaw NLRP3 instability - homogenization
Low NSB on 6OHDA in ARG	Toxin-induced morphology change

Summary

Bmax	Invicro	Date	Study type	Sample	Tracer	Competitor	Stimulation	Results	Next study
		202104	PET SC 발표
		202104 ARG	PET SC 발표	6OHDA rat (40 ug), striatum	3H]MCC 950	(~5 cc... )	mouse and rat NLRP3 insect cell lysates	High (NLRP3) probe injected unilaterally to one of LPS-induced rat brain hemisphere across each of the analysed regions; 의외 NSB (i.e SB이 거의 없음)	Yamatake-san @TBOSS-Imaging will set up homogenate study to test out-of-house probes basic problems in vivo, vs vehicle, vs LPS NLRP3 GoF mice
		1st	Optimization ARG	6OHDA rat (n=1)	[3H]candidate 1 ([3H]TR06616126)	10 / 100 nM		High (~10X) SB was observed in both the 1 site and 4 site 6 OHDA lesioned rat brains. There was a slight increase in SB signal on the lesioned hemisphere in relation to the sham lesioned hemisphere across each of the analysed regions
		2nd	Optimization ARG	the same dose of 6 OHDA spread across 4 sites	3 H]MCC 950	6 nM		necrotic pockets, Binding was notably lower around the 6 OHDA lesion site in 'lesioned hemisphere across each of the analysed regions'
		20220118	both Sec on 1 site and 4 site (40 ug)		3 HPBR 28	10 nM		SB window was poor (<3X SB) in all regions. Little to no differences in SB observed between the sham and 6 OHDA lesioned hemispheres. Increased SB by ~5X with low doses (~50nM) at the 4 binding distribution of the binding resembled that seen with 3 H]Candidate 1; (lower 의외 NSB ~5 (의기), morphology 때문)
		202203	Ad hoc 미팅	1st site (n=1?)	3 HJPBR 28	1µL/4 site (rat)	various, Ashley CW	lesioned side / un-lesioned side: Very low NSB & Total at 100nM un-treated rat 70 ↑↑ p+ & Aconita, Ibotia c't qua & comita 시간 따라 binding range very low SB1, ?? / bonota ?? quat 2J쯤 ㅁ가
			Ad hoc 미팅 autopsy 인 human SC section		3 H]MCC 950	2cc 30 ng / various PBR / 10 ug, 30 ug	MCC 950	total 6m AD vs HCL n/sb / 92% reduction of [3H]PBR28 / 6m AD vs HC, n=10 each / [3H]PBR28 total signal in AD frozen 4-5x higher than that observed using 3 H]MCC 950 / HC brain: very low SB, ND brain: 60% and 75% reduction observed at 30nM / Binding of increasing concentrations of 3HMCC950 / SB window ranges from 20% to 55% with greatest displacement at 100nM (sub-nM 'future' 후 concentrations to reduce NSB)
Postmortem PD samples	i) Using the PD brain samples from NBB, the ARG study will be initiated. It will take ~2 months for the first Feasibility study including optimization and the results with NBB PD brain will be generated by the end of Apr. Tritiated MCC950 and TR126 will be used. ii) Further PD brain tissue from UK biobank will be obtained by the seasoned PD brain. The feasibility of PD brain will be evaluated in Jun.
Paul Rolzin	Homogenate: confirming Invicro's study, with 6OHDA RATs homogenates. Bmax, J our codern, MCC950 Joshua Bliesath for homogenate Date Sample Tracer Result 20220203 Ad hoc 미팅 6OHDA mouse striatum 3H-TR06616126 Fold change increase in Total & NSB, BUT very little SB 6OHDA rat striatum 3H-TR06616126 Dose-dependent increase difference between 6OHDA rat striatum vs naive tissue, (although 5-fold increase in NSB with all of these samples (satellite confirmed by WB.).

Triaging compounds

Team: Anne Kanta (DMPK)-6OHDA rodent

Hi Yamatake-san, Sorry for my delayed response. I had a shot chat with Masato and Mitsuhiro, and came up with some experimental condition to be conducted as a very first attempt. I will be summarizing that within this week and will discuss it with Jaewon first. In brief, we propose to focus on the rat sub-chronic LPS systemic injection model (4 times with 0.4 mg/kg i.p. as rereported) and my add another arm with increase of LPS dose. So the design would be ▢ Normal rat (because Tcal has a good ability of reuptake, not but not to mice) with low/high dose probe (0.3 & 3 mpk) compound i.v. (reference Kp, self-block), 2 time point after ▢ Low dose LPS (0.5 mpk)-treated rats with low/high dose probe compound i.v. (expected enhanced NLRP3 from literature 1.5 fold, change in Kp (>0.05?) and evaluate self-block), 2 time point after ▢ High dose LPS (2 mpk)-treated rats with low/high dose probe compound i.v. (expected enhanced NLRP3 higher than the avobe, change in Kp and evaluate self-block), 2 time point after ▢ Total 12 arms, if N=3 total experimental rat is 36 We have to check if the current animal experiment protocol can cover the LPS injection. The dosing and sampling can be done by the Rabbics colleagues and PK evaluation will be organized by Mitsuhiro. • One missing capability in TSHO is ?? blot. So hope TSD team can support of NLRP3 protein expression change by the western blot. The challenges of the assay is that the NLRP3 protein appeared to be unstable in the extraction with lyse buffer. Wei has the proper experimental conditions for the WB. Now immediate next actions are 1) to confirm if the experimental protocol is covered by the currently approved one (Yoshiro, Masato), 2) determine the dose of probe compound started i.v. by referring to the LLOQ (Mitsuhiro), 3) confirm if TSD can support the WB experiment (Marianthi?), 4) Where NSTM discussion to finalize the protocol (Masato, Yoshiro, Jaewon)

Dosing regimen

TR06647850	Time point	WT rat	LPS (0.5 mg/kg) rat	LPS (2 mg/kg) rat
0.3 mg	1 h	3	3	3
	2 h	3	3	3
3 mg	1 h	3	3	3
	2 h	3	3	3

Habituation/dosing schedule cartoon (SD rat 7-8 week, Day1 Habituation, Days 2-5 LPS (i.p.) arrows, Day 5 TR06647850 (i.v.) and Sampling marker — kept as evidence in body_r05_c01.jpg / body_r05_c02.jpg).

Footer: Private and confidential. For internal use only.

- readouts planned: i) brain penetration (Kp), ii) Bmax difference (PD vs WT), iii) regional distribution (SN, striatum?) of the probe (850) by LCMS? lii) block 한다고 안한다고

왼쪽에 대하여:

• Purpose?
• TO: (drug candidate 안 쓰니) 못 볼 것,
• SB?: i) KO 쓰면 NLRP3 protein-specific SB 볼 수 있을 텐데, 이걸 하진 않는 거고 ii) self-block? 그럼 competing agent (TR06647850)의 conc?

Next study: Triaging, Multiple tracer?, Competition assay (blocking)
TSHO PET-G (Yamatake) In vivo blocking study: 6-OHDA rat model @TCAL
Led by TSHO DMPK-G or TCAL DMPK
Overall control: NSTM (Yoshirou-san)
Candidate compounds: 1st: TR06673219 (TCAL series 3), 2nd: TR06647850 (Novartis Pat.)

Precursor: Synthesis by TSHO PET chemistry-G

Imaging (cold) / hot timeline:

• 202303: synthesis of precursor of 18F]TR06762852 ongoing
• 202304: ship [18F]TR06762852 precursor (5-10mg) and standard (25mg) to Tbos
• 202305: Paul Rolzin to surgery (4-level 6OHDA)
• 202306: Paul Rolzin ship 3-4 rats to Tbos
• 202306: label at Dana Farber → PET Study (baseline and blocking?)

Uncertain Spans

location	transcription	uncertainty
Summary tracer table / column placement	the wide multi-column tracer-experiment table has 9-10 columns including Bmax / Invicro / date / study type / sample / Tracer / Competitor / Stimulation / Results / Next study; per-row column placement is partly inferred from cell width visible in body_r01_c01.jpg.	low confidence on column-by-row placement.
Summary tracer table / 202203 / Ad hoc 미팅 row	the result cell reads lesioned side / un-lesioned side: Very low NSB & Total at 100nM un-treated rat 70 ↑↑ p+ & Aconita, Ibotia c't qua & comita 시간 따라 binding range very low SB1, ?? / bonota ?? quat 2J쯤 ㅁ가; multiple Korean tokens are partly clipped.	low confidence on Aconita, Ibotia c't qua & comita token cluster.
Triaging compounds / Now immediate next actions	the action items reference (Marianthi?) for WB experiment confirmation; preserved verbatim.	low confidence on whether Marianthi is the assignee or a question.
Dosing regimen / TR06647850 row label	reads TR06647850 with strikethrough/cell-clip variation; preserved verbatim.	source typography preserved.
Body bottom / Imaging timeline	reads 202303, 202304, 202305, 202306, 202306 (last entry duplicated); preserved verbatim.	low confidence on whether one of the 202306 entries should be 202307.