• 농약과학회지
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• 제11권3호
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• pp.131-137
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• 2007

상이한 정렬조건에서 imidaclopid 유도체 중, imidazol 고리상 N-치환체(X)들의 벼멸구(Nilaparvata lugens)에 대한 살충활성에 관하여 CoMFA 및 CoMSIA 모델을 유도하고 정량적으로 검토하였다. 두 최적 모델의 예측성($q^2$ 또는 $r_{cv.}^2$)과 상관성($r_{ncv.}^2$)은 field fit (FF) 정렬보다 atom based fit (AF) 정렬조건의 모델이 좋았으며 CoMFA (A5) 모델보다 CoMSIA (A10) 모델이 더 좋았다. 최적의 CoMSIA (A10) 모델로부터 N-치환체(X)들에 의한 살충활성은 주로 정전기장과 수소결합 받게장에 의존적이었다. 그러므로 CoMSIA (A10) 모델의 등고도로부터 benzoyl 고리(X)상 ortho- 위치에는 양전하, carbonyl기의 산소원자 부분에는 음전하가 큰 작용기일수록 그리고 ortho- 및 meta- 위치의 수소결합 받게가 살충활성을 개선하는데 크게 기여할 것으로 예측되었다.

• Bulletin of the Korean Chemical Society
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• 제27권11호
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• pp.1741-1746
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• 2006

3D-QSARs on the neuroblocking activities by 1-(6-chloro-3-pyridylmethyl)-2-nitroiminoimidazolidine analogues as agonist at the nicotinic acetylcholine receptor (nAChR) were studied quantitatively using CoMFA and CoMSIA methodologies. The statistical results of CoMFA (A5: $r^2\;_{cv.}\;=\;0.707\;&\;r^2\;_{ncv.}$= 0.986) and CoMSIA model (A3: $r^2\;_{cv.}$ = 0.715 & $r^2\;_{ncv.}$ = 0.961) showed the best predictability and fitness for neuroblocking activity based on the cross-validated value and non-cross validated value. The steric and H-bond acceptor nature of a compound were essential for high activity. The study on 3D-QSARs between substrate molecules and their neuroblocking activities appears to be an useful approach for designing better neuroblocking drug development.

• Mass Spectrometry Letters
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• 제8권3호
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• pp.65-68
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• 2017

Thiamethoxam is one of the main suspect in honeybee colony collapse disorder (CCD). Due to this reason, thiamethoxam including imidacloprid and clothianidin has been banned for two years in some Europe countries. The CCD phenomenon has also been reported in Korea. Regarding this issue and needs, a new project has started to develop the method for the quatitation of thiamethoxam using isotope dilution mass spectrometry (IDMS). In the process of optimization for the IDMS method with thiamethoxam and $thiamethoxam-d_3$, we observed that the fragment peaks did not correspond to the fragmentation pathway as published elsewhere. Here, we proposed a candidate fragmentation pathway. To validate the proposed fragmentation pathway, another isotope analogue, $thiamethoxam-d_4$, was introduced and the MS/MS spectra of both isotope analogues were compared. In addition, the MS/MS/MS spectra of thiamethoxam were inspected for more evidence of the candidate pathway. Those spectra indicated that the proposed fragmentation pathway could be used to assign the fragment peaks of thiamethoxam.